Descriptor: "myoglobinuria" - Searchworks@Jio Institute Digital Library Search Results

251. Genotype-phenotype correlations in a large series of patients with muscle type CPT II deficiency.

Author: Anichini, Angelica, Fanin, Marina, Vianey-Saban, Christine, Cassandrini, Denise, Fiorillo, Chiara, Bruno, Claudio, and Angelini, Corrado
Abstract: Objectives: The adult or 'muscular' form of carnitine-palmitoyl-transferase II (CPT II) deficiency presents with recurrent rhabdomyolytic episodes and myoglobinuria, usually triggered by prolonged exercise. The aim of this study was to investigate a large series of patients in order to provide genotype-phenotype correlations. Methods: Our muscle tissue bank was surveyed for patients showing attacks of rhabdomyolysis with myoglobinuria. After exclusion of cases affected with toxic myoglobinuria, McArdle's disease and Becker muscular dystrophy, over 100 patients were selected for isotope-exchange radioenzymatic assay of CPT enzyme activity in muscle, and 25 cases resulted to be defective. Acylcarnitine profile was performed in five patients using tandem mass spectrometry. Mutations in the CPT2 gene were identified using DNA sequencing. Results: Although the clinical features were rather homogeneous, some patients presented life-threatening events (acute renal failure) and muscle weakness, and low levels of residual CPT activity. The typical acylcarnitine profile found in mutant patients confirmed its value as a screening method for further diagnostic investigations. We found a high frequency of the common p.Ser113Leu mutation, the recurrence of the rare p.Arg631Cys mutation in a genetic isolate in Southern Italy, and identified four novel mutations. In some affected patients only one mutant allele was found, suggesting either incomplete mutation detection or the possibility they are symptomatic carriers. Discussion: Null mutations and homozygous mutations were frequently associated with a more severe phenotype and biochemical defect. The identification of symptomatic obligate heterozygous carriers might suggest that additional epigenetic or environmental factors may contribute to determine the phenotype. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2011</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1179/016164110X12767786356390">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__53734031" data-document-counter="252" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-252"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 252. </span> <a data-context-href="/articles/asx__53734031/track?counter=252&document_id=asx__53734031&search_id=50609420" href="/articles/asx__53734031">Exercise induced cramps and myoglobinuria in dystrophinopathy -- a report of three Malaysian patients.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__53734031" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__53734031" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="OpKEVL1zUYiy2ADW35tWaU8yY2GqHdDizLePIU4AFYSdn7EU8keWTH99GSHhQ76X8SvX3vmD+QNl75maQSO8fQ==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__53734031" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Annuar, Azlina Ahmad, Kum Thong Wong, Ai Sze Ching, Meow Keong Thong, Sau Wei Wong, Alsiddiq, Feizel, Lai Choo Ong, and Khean Jin Goh</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22MUSCLE+cramps%22">MUSCLE cramps</searchLink>, *<searchLink fieldCode="DE" term="%22DYSTROPHIN%22">DYSTROPHIN</searchLink>, *<searchLink fieldCode="DE" term="%22IMMUNOHISTOCHEMISTRY%22">IMMUNOHISTOCHEMISTRY</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22MUSCLE+diseases%22">MUSCLE diseases</searchLink>, *<searchLink fieldCode="DE" term="%22MALAYSIANS%22">MALAYSIANS</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Dystrophinopathies commonly present as Duchenne or Becker muscular dystrophy but rare, unusual phenotypes have also been described. We have identified three Malaysian boys with an unusual form of dystrophinopathy, presenting with exercise-induced cramps and myoglobinuria, but with no apparent muscle weakness. Immunohistochemistry for dystrophin and genetic analysis confirmed the diagnosis. The frequency of this phenotype is unknown but there have been several case reports. Consistent with these reports, we also found that two of our patients had deletions in the rod domain of dystrophin, which has been suggested to be associated with this unusual manifestation. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2010</dd> </dl> </article><article data-document-id="asx__55113149" data-document-counter="253" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-253"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 253. </span> <a data-context-href="/articles/asx__55113149/track?counter=253&document_id=asx__55113149&search_id=50609420" href="/articles/asx__55113149">A genome-wide scan for tying-up syndrome in Japanese Thoroughbreds Tozaki et al. A genome-wide scan for tying-up syndrome.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__55113149" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__55113149" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="iiE2wgD/+P7d5t2BrDzn1pBuYRr+200lAxhe27ouSLnuF2FIc17sfxIvWnGBJCOisbPyY8In5Vjyf82s7K9Hfg==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__55113149" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Tozaki, T., Hirota, K., Sugita, S., Ishida, N., Miyake, T., Oki, H., and Hasegawa, T.</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22THOROUGHBRED+horse%22">THOROUGHBRED horse</searchLink>, *<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22GENOMES%22">GENOMES</searchLink>, *<searchLink fieldCode="DE" term="%22ANIMAL+genetics%22">ANIMAL genetics</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Tying-up syndrome, also known as recurrent exertional rhabdomyolysis in Thoroughbreds, is a common muscle disorder for racehorses. In this study, we performed a multipoint linkage analysis using LOKI based on the Bayesian Markov chain Monte Carlo method using 5 half-sib families (51 affected and 277 nonaffected horses in total), and a genome-wide association study (GWAS) using microsatellites (144 affected and 144 nonaffected horses) to map candidate regions for tying-up syndrome in Japanese Thoroughbreds. The linkage analysis identified one strong L-score (82.45) between the loci UCDEQ411 and COR058 (24.9-27.9 Mb) on ECA12. The GWAS identified two suggestive genomic regions on ECA12 (24.9-27.8 Mb) and ECA20 (29.3-33.5 Mb). Based on both results, the genomic region between UCDEQ411 and TKY499 (24.9-27.8 Mb) on ECA12 was the most significant and was considered as a candidate region for tying-up syndrome in Japanese Thoroughbreds. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2010</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1111/j.1365-2052.2010.02112.x">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__54845687" data-document-counter="254" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-254"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 254. </span> <a data-context-href="/articles/asx__54845687/track?counter=254&document_id=asx__54845687&search_id=50609420" href="/articles/asx__54845687">McArdle disease: a clinical review.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__54845687" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__54845687" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="0mfNg4CmN0sp1tooSBNA/9BJGQ69P4xK7W63Mn9Be/fmmiIfe7XYB4+2QlqSm6qsCsd5kDHq2UDqFjkYcriphQ==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__54845687" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> R Quinlivan</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22PATIENTS%22">PATIENTS</searchLink>, *<searchLink fieldCode="DE" term="%22GENETICS%22">GENETICS</searchLink>, *<searchLink fieldCode="DE" term="%22EXERCISE%22">EXERCISE</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22CHRONIC+kidney+failure%22">CHRONIC kidney failure</searchLink>, *<searchLink fieldCode="DE" term="%22PREGNANCY%22">PREGNANCY</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> METHODS: The clinical phenotype of 45 genetically confirmed McArdle patients is described. RESULTS: In the majority of patients (84%), the onset of symptoms was from early childhood but diagnosis was frequently delayed until after 30 years of age. Not all patients could recognise a second wind although it was always seen with exercise assessment. A history of myoglobinuria was not universal and episodes of acute renal failure had occurred in a minority (11%). The condition does not appear to adversely affect pregnancy and childbirth. Clinical examination was normal in most patients, muscle hypertrophy was present in 24% and mild muscle wasting and weakness were seen only in patients over 40 years of age and was limited to shoulder girdle and axial muscles. The serum creatine kinase was elevated in all but one pregnant patient. Screening for the mutations pArg50X (R50X) and pGly205Ser (G205S) showed at least one mutated allele in 96% of Caucasian British patients, with an allele frequency of 77% for pArg50X in this population. A 12 min walking test to evaluate patients is described. CONCLUSION: The results demonstrated a wide spectrum of severity with the range of distance walked (195–1980 m); the mean distance walked was 512 m, suggesting significant functional impairment in most patients. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2010</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1136/jnnp.2009.195040">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__54478147" data-document-counter="255" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-255"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 255. </span> <a data-context-href="/articles/asx__54478147/track?counter=255&document_id=asx__54478147&search_id=50609420" href="/articles/asx__54478147">European outbreak of atypical myopathy in the autumn 2009 G. van Galen et al. European outbreak of atypical myopathy.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__54478147" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__54478147" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="1VCp3BSbS1Nzm2bxc+H3BbklMFY8q5xd59VIeNtzb0lj7TVJvHdsD5Ui0+RzHvjM7BgC9/zhR6DIddHH9YABfw==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__54478147" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Van Galen, Gaby, Amory, Helene, Busschers, Evita, Cassart, Dominique, De Bruijn, Marco, Gerber, Vincent, Keen, John, Lefere, Laurence, Pitel, Christel Marcillaud, Marr, Celia, Müller, Jessica-M. V., Pineau, Xavier, Saegerman, Claude, Sandersen, Charlotte, Serteyn, Didier, Torfs, Sara, Unger, Lucia, Verwilghen, Denis, and Votion, Dominique-Marie</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22DIAGNOSIS+of+muscle+diseases%22">DIAGNOSIS of muscle diseases</searchLink>, *<searchLink fieldCode="DE" term="%22VETERINARY+diagnosis%22">VETERINARY diagnosis</searchLink>, *<searchLink fieldCode="DE" term="%22DISEASE+prevalence%22">DISEASE prevalence</searchLink>, *<searchLink fieldCode="DE" term="%22DIAGNOSIS%22">DIAGNOSIS</searchLink>, *<searchLink fieldCode="DE" term="%22HORSE+diseases%22">HORSE diseases</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Atypical myopathy is an acute, severe rhabdomyolysis occurring in grazing horses. In the beginning of October 2009, a new outbreak occurred in several European countries. Geographic, demographic and clinical data of the reported cases in the month October 2009 are described. The survival rate in this outbreak was 25%. The most frequently observed clinical signs were congested mucous membranes, dyspnea, tachycardia, depression, weakness, stiffness, recumbency, trembling, sweating, and myoglobinuria. Nonsurvivors were significantly more likely to be recumbent than survivors. Prognostic factors, symptomatic treatment, and preventive measures are discussed. Differences were encountered during the described outbreak of atypical myopathy in October 2009 compared with previous outbreaks reported. Equine practitioners should be aware that previous epidemiological studies have shown that after a high prevalence in the autumn, new cases are likely to occur in the following spring. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2010</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1111/j.1476-4431.2010.00574.x">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__54478148" data-document-counter="256" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-256"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 256. </span> <a data-context-href="/articles/asx__54478148/track?counter=256&document_id=asx__54478148&search_id=50609420" href="/articles/asx__54478148">Comparative stability of canine and feline hemostatic proteins in freeze-thaw-cycled fresh frozen plasma P.E. Yaxley et al. Comparative stability of FTC FFP in dogs and cats.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__54478148" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__54478148" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="+PCAdZ3jf32c1EMPWHqKioD+3i7an8vXzkB8cNpGc9oxiGuiH2mR8HXZicgiFSa/YIGrsr5nnfgcbhwHNge7lg==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__54478148" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Yaxley, Page E., Beal, Matthew W., Jutkowitz, L. Ari, Hauptman, Joe G., Brooks, Marjory B., Hale, Anne S., and Parr, Alice</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22DIAGNOSIS+of+dog+diseases%22">DIAGNOSIS of dog diseases</searchLink>, *<searchLink fieldCode="DE" term="%22CAT+diseases%22">CAT diseases</searchLink>, *<searchLink fieldCode="DE" term="%22HEMOSTATICS%22">HEMOSTATICS</searchLink>, *<searchLink fieldCode="DE" term="%22BLOOD+plasma%22">BLOOD plasma</searchLink>, *<searchLink fieldCode="DE" term="%22VETERINARY+diagnosis%22">VETERINARY diagnosis</searchLink>, *<searchLink fieldCode="DE" term="%22BLOOD+coagulation+factors%22">BLOOD coagulation factors</searchLink>, *<searchLink fieldCode="DE" term="%22LONGITUDINAL+method%22">LONGITUDINAL method</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> To evaluate the stability of canine and feline hemostatic proteins in freeze-thaw-cycled (FTC) fresh frozen plasma (FFP). Prospective study. Veterinary Teaching Hospital. Nine blood donor dogs and 10 blood donor cats. Whole blood was collected and separated into packed RBC and plasma units according to standard methods. Each unit of plasma was divided into 2 equal aliquots and frozen (−41°C). One aliquot from each donor (FTC) was then thawed and then refrozen (−41°C) until time of analysis. The second aliquot (nonfreeze-thaw-cycled; NFTC) remained frozen until time of analysis. The hemostatic proteins assessed included coagulation factors, anticoagulant factors (antithrombin and Protein C), and adhesive proteins (fibrinogen and von Willebrand Factor). The coagulant activities of factors II, VII, VIII, IX, X, XI, and XII were measured in modified one-stage activated partial thromboplastin time or prothrombin time assays. Antithrombin and Protein C activities were measured in chromogenic substrate assays. Clottable fibrinogen was measured via the Clauss method, and von Willebrand Factor concentration (vWF:Ag) was measured in an ELISA. A paired t-test was utilized to identify differences in factor activity or concentration between FTC FFP and NFTC FFP. No clinically or statistically significant differences (all P>0.05) were identified between FTC FFP and NFTC FFP. Refreezing FFP within 1 hour of initial thawing appeared to have no deleterious effects on the hemostatic protein activity or content of that unit. Transfusion of FTC FFP is expected to provide the recipient with comparable replacement of hemostatic proteins as FFP that has remained frozen. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2010</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1111/j.1476-4431.2010.00563.x">View/download PDF</a></dd> </dl> </article><article data-document-id="edo__54311537" data-document-counter="257" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-257"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 257. </span> <a data-context-href="/articles/edo__54311537/track?counter=257&document_id=edo__54311537&search_id=50609420" href="/articles/edo__54311537">Acute renal failure due to multiple stings by Africanized bees. Report on 43 cases.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="edo__54311537" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/edo__54311537" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="fawd7+Ebm7cgJQTjVKe+TZ/9YvR6NWXwobk5GG6lL8Dm0IrXy0VPXrNucAKpupR8xDSxqnMefPctG6khyjVHJA==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_edo__54311537" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Mejía-Vélez, G.</p></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> <i>Copyright of Nefrologia is the property of Revista Nefrologia and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract.</i> (Copyright applies to all Abstracts.) </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2010</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.3265/Nefrologia.pre2010.May.10269">View/download PDF</a></dd> </dl> </article><article data-document-id="edo__83695664" data-document-counter="258" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-258"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 258. </span> <a data-context-href="/articles/edo__83695664/track?counter=258&document_id=edo__83695664&search_id=50609420" href="/articles/edo__83695664">Rabdomiolisis y falla renal aguda en un paciente con trastorno depresivo recurrente tratado con escitalopram y quetiapina.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="edo__83695664" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/edo__83695664" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="bn459SeRUDBFrayQbSnZ7oCWteZo08OzrnptClWEfTbIg72TJvjHFTJxC2aTe8KRsKp+3seSnRRuSw6WJf16LA==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_edo__83695664" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Orozco-Cabal, Luis, Gómez-Restrepo, Carlos, and Rodríguez-Sánchez, Martha Patricia</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors"><searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, <searchLink fieldCode="DE" term="%22STRIATED+muscle+necrosis%22">STRIATED muscle necrosis</searchLink>, <searchLink fieldCode="DE" term="%22ANTIDEPRESSANTS%22">ANTIDEPRESSANTS</searchLink>, <searchLink fieldCode="DE" term="%22ESCITALOPRAM+oxalate%22">ESCITALOPRAM oxalate</searchLink>, <searchLink fieldCode="DE" term="%22SEROTONIN%22">SEROTONIN</searchLink>, <searchLink fieldCode="DE" term="%22NEUROTRANSMITTERS%22">NEUROTRANSMITTERS</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> <i>Copyright of Revista Colombiana de Psiquiatria is the property of Asociacion Colombiana de Psiquiatria and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract.</i> (Copyright applies to all Abstracts.) </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2010</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1016/S0034-7450(14)60231-6">View/download PDF</a></dd> </dl> </article><article data-document-id="edb__53322756" data-document-counter="259" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-259"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 259. </span> <a data-context-href="/articles/edb__53322756/track?counter=259&document_id=edb__53322756&search_id=50609420" href="/articles/edb__53322756">Routine and specialized laboratory testing for the diagnosis of neuromuscular diseases in dogs and cats.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="edb__53322756" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/edb__53322756" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="ln1ODMaYs9/KDrW2Cs/ZA+QOq2KFkkKnSkXqshUsHLCJL/qfjxwsSuxizj8Sa3FH0gMjGncsMsegQCp8+JMSYg==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_edb__53322756" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Shelton, G. Diane</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors"><searchLink fieldCode="DE" term="%22CREATINE+kinase%22">CREATINE kinase</searchLink>, <searchLink fieldCode="DE" term="%22NEUROMUSCULAR+disease+diagnosis%22">NEUROMUSCULAR disease diagnosis</searchLink>, <searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, <searchLink fieldCode="DE" term="%22MYASTHENIA+gravis%22">MYASTHENIA gravis</searchLink>, <searchLink fieldCode="DE" term="%22CHOLINERGIC+receptors%22">CHOLINERGIC receptors</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> The diagnosis of neuromuscular diseases can be challenging. The first step is recognition that the disease involves the neuromuscular system (muscle, neuromuscular junction, peripheral nerve, and ventral horn cells of the spinal cord). Many neuromuscular diseases share clinical signs and cannot be distinguished based on clinical examination. Routine laboratory screening, including a CBC, biochemical profile, and urinalysis, can identify some of the most common systemic abnormalities that cause muscle weakness and myalgia, such as hypo- and hyperglycemia, electrolyte disorders, or thyroid abnormalities, and may suggest a specific diagnosis, such as diabetes mellitus, hypo- or hyperadrenocorticism, renal failure, or hypothyroidism. Increased creatine kinase activity, increased cardiac troponin I concentration, and myoglobinuria are useful in detecting skeletal and cardiac muscle damage. Identification of acetylcholine receptor antibodies is diagnostic for acquired myasthenia gravis. For primary muscle or peripheral nerve diseases, tissue biopsy is the most direct way to determine specific pathology, correctly classify the disease, and determine the course of additional laboratory testing. For example, inflammatory, necrotizing, dystrophic, metabolic, or congenital myopathies require different laboratory testing procedures for further characterization. Many neuromuscular diseases are inherited or breed-associated, and DNA-based tests may already be established or may be feasible to develop after the disorder has been accurately characterized. This review focuses on both routine and specialized laboratory testing necessary to reach a definitive diagnosis and determine an accurate prognosis for neuromuscular diseases. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2010</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1111/j.1939-165X.2010.00244.x">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__77526590" data-document-counter="260" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-260"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 260. </span> <a data-context-href="/articles/asx__77526590/track?counter=260&document_id=asx__77526590&search_id=50609420" href="/articles/asx__77526590">The synthetic polyphenol tert-butyl-bisphenol inhibits myoglobin-induced dysfunction in cultured kidney epithelial cells.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__77526590" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__77526590" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="bbbSLkBwK0Ei3LWny03RVF0ELVpisbQJc8R3hN/QBWehuWxPEC8TfyS/R9wqIHbn7gD2k+PFUuBDz5JepvXsEw==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__77526590" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Shanu, Anu, Parry, Sarah N., Wood, Sarah, Rodas, Elicia, and Witting, Paul K.</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22POLYPHENOLS%22">POLYPHENOLS</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBIN%22">MYOGLOBIN</searchLink>, *<searchLink fieldCode="DE" term="%22EPITHELIAL+cells%22">EPITHELIAL cells</searchLink>, *<searchLink fieldCode="DE" term="%22ACUTE+kidney+failure%22">ACUTE kidney failure</searchLink>, *<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22ETIOLOGY+of+diseases%22">ETIOLOGY of diseases</searchLink>, *<searchLink fieldCode="DE" term="%22ENZYME+inhibitors%22">ENZYME inhibitors</searchLink>, *<searchLink fieldCode="DE" term="%22URINALYSIS%22">URINALYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22TUMOR+necrosis+factors%22">TUMOR necrosis factors</searchLink>, *<searchLink fieldCode="DE" term="%22OXIDATIVE+stress%22">OXIDATIVE stress</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Rhabdomyolysis caused by severe burn releases extracellular myoglobin (Mb) that accumulates in the kidney and urine (maximum [Mb] ∼ 50 μM) (termed myoglobinuria). Extracellular Mb can be a pro-oxidant. This study cultured Madin-Darby-canine-kidney-Type-II (MDCK II) cells in the presence of Mb and tested whether supplementation with a synthetic tert-butyl-polyphenol ( tert-butyl-bisphenol; t-BP) protects these renal cells from dysfunction. In the absence of t-BP, cells exposed to 0-100 μM Mb for 24 h showed a dose-dependent decrease in ATP and the total thiol (TSH) redox status without loss of viability. Gene expression of superoxide dismutases-1/2, haemoxygenase-1 and tumour necrosis factor increased and receptor-mediated endocytosis of transferrin and monolayer permeability decreased significantly. Supplementation with t-BP before Mb-insult maintained ATP and the TSH redox status, diminished antioxidant/pro-inflammatory gene responses, enhanced monolayer permissiveness and restored transferrin uptake. Overall, bolstering the total antioxidant capacity of the kidney may protect against oxidative stress induced by experimental myoglobinuria. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2010</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.3109/10715762.2010.485993">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__52533869" data-document-counter="261" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-261"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 261. </span> <a data-context-href="/articles/asx__52533869/track?counter=261&document_id=asx__52533869&search_id=50609420" href="/articles/asx__52533869">Clinical and biochemical improvement of very long-chain acyl-CoA dehydrogenase deficiency in pregnancy.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__52533869" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__52533869" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="zqa+JD8pJ/owpY8ifMXO07GInTNrwyb+h9+zlSFAbMrXVCK5RNnaMqtzh6VXQ1E1eXQRm076L43C11rBYmCNcQ==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__52533869" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Mendez-Figueroa, H., Shchelochkov, O. A., Shaibani, A., Aagaard-Tillery, K., and Shinawi, M. S.</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22DEHYDROGENASES%22">DEHYDROGENASES</searchLink>, *<searchLink fieldCode="DE" term="%22FATTY+acids%22">FATTY acids</searchLink>, *<searchLink fieldCode="DE" term="%22BIOCHEMIC+medicine%22">BIOCHEMIC medicine</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Very long-chain acyl-CoA dehydrogenase (VLCAD) deficiency is an enzymatic defect of the fatty acid (FA) beta oxidation pathway. In catabolic states, such as labor and early postpartum period, patients are potentially prone to metabolic decompensation and subsequent rhabdomyolysis with increased risk for myoglobinuria and renal insufficiency. We report a 21-year-old primigravida with a previously characterized VLCAD deficiency, who experienced frequent and unprovoked episodes of rhabdomyolysis before pregnancy. As there was no published experience to guide her management, a detailed multidisciplinary care plan was established to minimize the potential morbidity. Although there is little known about the antenatal course of gravidae affected by VLCAD, we predicted that placental and fetal β-oxidation in an unaffected pregnancy may temporize or even improve maternal FA β-oxidation. Consistent with our prediction, we observed a significant clinical and biochemical improvement throughout her pregnancy, and she delivered vaginally with an uncomplicated postpartum course. We conclude that although VLCAD deficiency can present a therapeutic challenge during pregnancy, the beneficial placento-maternal metabolic interactions and the implementation of a proper peripartum management reassure a successful antenatal and perinatal outcome. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2010</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1038/jp.2009.198">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__52428063" data-document-counter="262" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-262"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 262. </span> <a data-context-href="/articles/asx__52428063/track?counter=262&document_id=asx__52428063&search_id=50609420" href="/articles/asx__52428063">A Cardiac Rhabdomyoma in a Guinea Pig.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__52428063" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__52428063" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="eyiIod9cloc8FmXwkhnpXcHit7GDIUjLFQ16NrdHi8pGKbZiARoR7V5t9FoKg0zFEwjmpvCvWGo52VfO5FweAA==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__52428063" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Kobayashi, Tatsuya, Kobayashi, Yoshihiko, Fukuda, Uina, Ozeki, Yukiko, Takahashi, Maki, Fujioka, Shigeru, and Fuchikami, Jun-ichi</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22GUINEA+pigs+as+laboratory+animals%22">GUINEA pigs as laboratory animals</searchLink>, *<searchLink fieldCode="DE" term="%22HEART+histopathology%22">HEART histopathology</searchLink>, *<searchLink fieldCode="DE" term="%22HISTOPATHOLOGY%22">HISTOPATHOLOGY</searchLink>, *<searchLink fieldCode="DE" term="%22HEART+disease+diagnosis%22">HEART disease diagnosis</searchLink>, *<searchLink fieldCode="DE" term="%22CARDIOMYOPATHIES%22">CARDIOMYOPATHIES</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22TRICUSPID+valve+diseases%22">TRICUSPID valve diseases</searchLink>, *<searchLink fieldCode="DE" term="%22IMMUNOHISTOCHEMISTRY%22">IMMUNOHISTOCHEMISTRY</searchLink>, *<searchLink fieldCode="DE" term="%22GLYCOGEN+storage+disease%22">GLYCOGEN storage disease</searchLink>, *<searchLink fieldCode="DE" term="%22DIAGNOSIS%22">DIAGNOSIS</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> A guinea pig (9-week-old) that had been placed in a control group for a pharmacological test was found to have a single nodule on the surface of the right ventricular wall. In a transverse section of the heart after fixation, a whitish mass was found that extended from the subendocardium to the subepicardium of the right ventricular wall. Histopathological examination revealed a spongy network consisting of vacuolated spaces in the myocardium of the right ventricle extending to the myocardium and subepicardium of the right atrium. The vacuolated space was PAS-positive. Immunohistochemical examinations revealed that the lesions contained striated fibers that were positive for anti-desmin and anti-myoglobin. Electron micrographs revealed the lesions resulting in affected striated muscle fibers and accumulations of many glycogen granules. Based on the findings, the lesions were diagnosed as a cardiac rhabdomyoma. This is the first report of application of immunohistochemical examinations to diagnosis of cardiac rhabdomyoma in the guinea pig. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2010</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1293/tox.23.107">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__51422031" data-document-counter="263" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-263"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 263. </span> <a data-context-href="/articles/asx__51422031/track?counter=263&document_id=asx__51422031&search_id=50609420" href="/articles/asx__51422031">Le syndrome de perfusion du propofol</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__51422031" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__51422031" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="HDUnigQWA42TwtkgDO9IhD1yj3nEX/af5l7WhOmSPl1L6qG+W3/BQob2BBxPlqDib+aBPpNnVPv03W5L+a46jg==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__51422031" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Laquay, N., Prieur, S., Greff, B., Meyer, P., and Orliaguet, G.</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22PROPOFOL%22">PROPOFOL</searchLink>, *<searchLink fieldCode="DE" term="%22SIDE+effects+of+anesthetics%22">SIDE effects of anesthetics</searchLink>, *<searchLink fieldCode="DE" term="%22INTENSIVE+care+units%22">INTENSIVE care units</searchLink>, *<searchLink fieldCode="DE" term="%22BENZODIAZEPINES%22">BENZODIAZEPINES</searchLink>, *<searchLink fieldCode="DE" term="%22ARRHYTHMIA%22">ARRHYTHMIA</searchLink>, *<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22CONSCIOUS+sedation%22">CONSCIOUS sedation</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Abstract: Objective: Propofol is commonly used for sedation of children or adult patients in intensive care unit as an alternative to benzodiazepines for the long-term sedation of mechanically ventiled patient. However, the life-threatening complication of propofol-infusion syndrome (PRIS) may in some case occur. The objective of this article is to review the clinical features, physiopathology and management of PRIS. Data sources: A PubMed® database research in English and French languages published until December 2008. Keywords were propofol, propofol infusion syndrome (PRIS), rhabdomyolysis, heart failure, arrhythmias, metabolic acidosis, brain injury, sedation, intensive care. Data synthesis: PRIS is a rare and potentially lethal complication, especially if there''s no early identification of the syndrome. The physiopathology of PRIS mechanism remains unclear, however a dysfunction of mitochondrial respiratory chain could be involved and potential genetic factor may account. Clinical features consist of arrhythmias, metabolic acidosis, lipemia, rhabdomyolisis, myoglobinuria. PRIS has been described classically in children and adults undergoing a long term infusion with propofol (more than 48hours) at doses higher than 4mg/kg per hour. However, it can be observed with lower doses and after shorter duration of sedation. Steroids, vasopressors and low carbohydrate intake act as triggering factors. Early recognition of the syndrome improve patient''s outcome. Propofol infusion must be avoided in susceptible patients and another sedative agent should be considered. When using prolonged sedation with propofol, arrhythmia and serum triglyceridemia level should be monitored. [Copyright &y& Elsevier] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2010</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1016/j.annfar.2010.02.030">View/download PDF</a></dd> </dl> </article><article data-document-id="edo__50337933" data-document-counter="264" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-264"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 264. </span> <a data-context-href="/articles/edo__50337933/track?counter=264&document_id=edo__50337933&search_id=50609420" href="/articles/edo__50337933">Rhabdomyolysis: When Exercising Becomes a Risk.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="edo__50337933" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/edo__50337933" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="71VSY8q7OvT2FCKBWQtHrBBtvliLJIImAxMUKYz7mIEDo+rPnchTv+hnXRsQgI5goWN6tLnN2Nd3AhYOAKM/Og==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_edo__50337933" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Thoenes, Melanie</p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2010</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1016/j.pedhc.2009.08.009">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__48493831" data-document-counter="265" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-265"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 265. </span> <a data-context-href="/articles/asx__48493831/track?counter=265&document_id=asx__48493831&search_id=50609420" href="/articles/asx__48493831">Myoglobinuria after laparoscopic radiofrequency ablation of liver tumors.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__48493831" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__48493831" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="jdqknyK8UbbGx67TtbuRH4w65P7Lfrc2YaU1/EP/BmzlhQQL28+T5uRU9FYF2nXxW9C2A+WZkP6dZHTyLIddfw==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__48493831" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Rodriguez, John, Tellioglu, Gurkan, Siperstein, Allan, and Berber, Eren</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22RADIO+frequency%22">RADIO frequency</searchLink>, *<searchLink fieldCode="DE" term="%22CATHETER+ablation%22">CATHETER ablation</searchLink>, *<searchLink fieldCode="DE" term="%22LIVER+tumors%22">LIVER tumors</searchLink>, *<searchLink fieldCode="DE" term="%22MUSCLE+diseases%22">MUSCLE diseases</searchLink>, *<searchLink fieldCode="DE" term="%22CHI-squared+test%22">CHI-squared test</searchLink>, *<searchLink fieldCode="DE" term="%22CREATINE+kinase%22">CREATINE kinase</searchLink>, *<searchLink fieldCode="DE" term="%22CREATININE%22">CREATININE</searchLink>, *<searchLink fieldCode="DE" term="%22LAPAROSCOPY%22">LAPAROSCOPY</searchLink>, *<searchLink fieldCode="DE" term="%22LONGITUDINAL+method%22">LONGITUDINAL method</searchLink>, *<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22SURGICAL+complications%22">SURGICAL complications</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> <bold>Background: </bold>There are scant data in the literature about myoglobinuria after radiofrequency ablation (RFA) of liver tumors. The aim of this study is to analyze the incidence and identify the risk factors involved in this complication after RFA.<bold>Patients and Methods: </bold>An initial case of myoglobinuria and acute kidney injury (AKI) during laparoscopic liver RFA after 10 years of the liver ablation program led to the design of this study. Prospective data were collected on 41 consecutive patients undergoing laparoscopic RFA at our institution over a 9-month period. Urine myoglobin, serum creatinine kinase, and serum creatinine levels were obtained preablation and postablation. Variables were compared between patients to identify possible risk factors that might be related to this rare complication. Data are expressed as mean +/- standard error of the mean.<bold>Results: </bold>Two patients were excluded from the study due to preoperative myoglobinuria of unknown etiology. Of the remaining 39 patients, three developed dark urine with significant myoglobinuria on postoperative day 1. Two of these patients had carcinoid liver metastases; the remaining patient had a metastatic colorectal lesion. The number of tumors ablated in these patients was 14, 11, and 3 vs. 2.4 +/- 0.4 in the rest of the patients. Cumulative tumor volume was larger in the group of patients that developed the complication vs. those who did not (127.9 +/- 59.5 vs. 48 +/- 3 cm(3)). Two grounding pads were used in the three patients that had a complication vs. four pads in the rest of the patients. Dark urine was identified promptly intraoperatively and treated aggressively. All of these patients required intensive care unit (ICU) admission and had a prolonged hospital stay. Marked elevation of transaminases and creatinine kinase as well as a drop in hematocrit and platelet count was observed in patients with myoglobinuria. In our retrospective review of 706 patients that underwent liver RFA in the past 10 years, we detected 27 patients (3.8%) with ten or more lesions (11.9 +/- 0.4). None of these patients had significant elevation of serum creatinine postoperatively. In the whole series of 706 patients, 22 (3.2%) were found to have elevated creatinine after liver RFA, with return to baseline in all but seven patients in follow-up.<bold>Conclusion: </bold>Myoglobinuria after liver RFA is a rare but potentially devastating complication that may lead to AKI with significant morbidity and prolonged hospital stay. Patients with large tumor volumes requiring longer ablation times need to be monitored closely for the development of this complication. The fact that this was not observed in other patients with similar tumor characteristics suggests that individual patient-related factors might play an important role. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2010</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1007/s11605-009-1118-x">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__49719354" data-document-counter="266" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-266"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 266. </span> <a data-context-href="/articles/asx__49719354/track?counter=266&document_id=asx__49719354&search_id=50609420" href="/articles/asx__49719354">PROTEIN SYNTHESIS CHANGES IN BRAIN SUBCELLULAR PARTICLES DURING THE CRUSH SYNDROME. THE INFLUENCE OF HYPOTHALAMIC CYTOKINE PROLINE-RICH PEPTIDE (PRP).</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__49719354" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__49719354" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="5Dtn51wlBU0SuwhO6Xt/FHnpu8WVG/X3h3NTMd1q34r7X5HGrpy0b7hUytCYGIFmnNkIBwsRwXUNNDUkC3ZsIA==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__49719354" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Kevorkian, G. A., Kanayan, A. S., Guevorkian, A. G., Hayrapetyan, H. L., Khachatryan, H. F., and Mkrtchyan, A.</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22PROTEIN+synthesis%22">PROTEIN synthesis</searchLink>, *<searchLink fieldCode="DE" term="%22CRUSH+syndrome%22">CRUSH syndrome</searchLink>, *<searchLink fieldCode="DE" term="%22SOFT+tissue+injuries%22">SOFT tissue injuries</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22PROTEOLYSIS%22">PROTEOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22ACUTE+kidney+failure%22">ACUTE kidney failure</searchLink>, *<searchLink fieldCode="DE" term="%22HYPOTHALAMIC+hormones%22">HYPOTHALAMIC hormones</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Crush of soft tissues is followed by acute hemodynamic shock, myoglobinuria, acute renal insufficiency, and lethal endotoxicity. Research on the pathogenesis of crush syndrome has shown that the largest changes in crush occur during decompression and are accompanied by acute alteration of brain protein synthesis and strong morphological changes of brain structures. The investigations have shown that a "proline rich peptide", originating from proteolysis of C-terminal glycoprotein a neurophysin II and along with vasopressin and oxytocin, is transferred from the hypothalamus to the neurohypophysis by axonal transport. During 2-hour compression protein synthesis decreased in cytosol (32.7%) and mitochondria (49%), after 5-h compression non-significant changes occurred in the level of protein synthesis. In 2, 4, 24, and 48 h of decompression after 2-h compression, and in 2- and 48-h decompression after 5-h compression; the level of protein synthesis in brain subcellular particles decreased. After intraperitoneal administration of proline-rich peptide (10 g per 100 g weight of white rats) activation of the protein synthesis occurs in all studied particles and the soluble fraction of brain cells. The positive effect of the peptide is conditioned, most probably, on activation of the immune system and adaptation mechanisms, including mobilization of endogen-protective mechanisms of the organism itself. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2010</dd> </dl> </article><article data-document-id="asx__119465863" data-document-counter="267" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-267"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 267. </span> <a data-context-href="/articles/asx__119465863/track?counter=267&document_id=asx__119465863&search_id=50609420" href="/articles/asx__119465863">White collar rhabdomyolysis with acute kidney injury.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__119465863" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__119465863" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="mWbufzbEz3vSU6X9rZ3dxfKCtNlx+cz1Pa/P7YWPo51C5jkD8KVqucxXVK/8+IHC0+1BIaW1emY1SsxKuk5CcA==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__119465863" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Bhakthavatsalam, R. K., Venu, G., Raju, P. Krishnam, and Madhusudan, H. C.</p></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Rhabdomyolysis is a clinical syndrome resulting from the disintegration of muscle cell and spillage of toxic intracellular contents into circulation. Strenuous, unaccustomed exercise leads to exertional rhabdomyolysis and cause AKI. We report a 26-year-old female who developed white collar rhabdomyolysis with AKI after performing sit-ups (Super Yoga Brain) for 108 times in temple. She was managed with hemodialysis and supporting therapy. She made a full recovery after 4 weeks. Awareness of this condition and early diagnosis is highlighted. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2016</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.4103/0971-4065.177209">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__118422356" data-document-counter="268" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-268"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 268. </span> <a data-context-href="/articles/asx__118422356/track?counter=268&document_id=asx__118422356&search_id=50609420" href="/articles/asx__118422356">Phosphoglycerate mutase deficiency (glycogen storage disease X) caused by a novel variant in PGAM-M.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__118422356" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__118422356" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="H+q2+KnKnxURqIW+velvjpAbF7OjkP6QQ9bz7PL0icBBVZdMb+lm099H3nimP0AF/TaBgy/fRNLxvYq4yFn8rA==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__118422356" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Koo, Benjamin and Oskarsson, Bjorn</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22GLYCOGEN+storage+disease%22">GLYCOGEN storage disease</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22PHOSPHOGLYCERATE+kinase%22">PHOSPHOGLYCERATE kinase</searchLink>, *<searchLink fieldCode="DE" term="%22GLYCOGENOLYSIS%22">GLYCOGENOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Phosphoglycerate mutase enzyme deficiency in muscle causes a metabolic myopathy (glycogen storage disease X) characterized by exertional muscle contractures, weakness, hyperCKemia, and myoglobinuria. Six different autosomal recessive variants in PGAM-M have been described thus far (Salameh et al., 2013). In this case report, we report a novel disease-causing variant. A 52-year-old African-American woman presented with exertional muscle contractures, myalgias, and weakness since childhood including an episode of rhabdomyolysis. Neurologic examination and EMG were normal. CK was mildly elevated at rest and over 20,000 U/L during her episode of rhabdomyolysis. Muscle biopsy revealed subsarcolemmal collections suggestive of tubular aggregates. Phosphoglycerate mutase activity was 8% of the reference value. PGAM-M sequencing showed compound heterozygous variants: c.233G>A, which has been found only in African-Americans with this disease, and a novel variant, c.278G>A. This case expands the genetic spectrum of phosphoglycerate mutase deficiency. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2016</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1016/j.nmd.2016.08.002">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__118001916" data-document-counter="269" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-269"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 269. </span> <a data-context-href="/articles/asx__118001916/track?counter=269&document_id=asx__118001916&search_id=50609420" href="/articles/asx__118001916">Serum myoglobin immunoassays: obsolete or still clinically useful?</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__118001916" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__118001916" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="zRuOXzIy1jLDMwBYrzPT3hExk8a/zpBWLyI81m4pT2zMESuokaNbyK9CIOe+4xt0vgTWvbuP8oX0/fhbWNLWHw==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__118001916" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Lippi, Giuseppe and Plebani, Mario</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22STRIATED+muscle+necrosis%22">STRIATED muscle necrosis</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22INTENSIVE+care+units%22">INTENSIVE care units</searchLink>, *<searchLink fieldCode="DE" term="%22MEDICAL+care%22">MEDICAL care</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> The article presents an editorial on diagnosis of rhabdomyolysis. It is stated that the most frequent and severe complication of rhabdomyolysis is acute kidney injury (AKI), the presence of which enhance the overall mortality up to 30%, approximating 60% in intensive care unit (ICU) patients. It is also noted that rhabdomyolysis has been based on the assessment of the enzymatic activity of creatine kinase. </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2016</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1515/cclm-2016-0472">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__115296014" data-document-counter="270" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-270"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 270. </span> <a data-context-href="/articles/asx__115296014/track?counter=270&document_id=asx__115296014&search_id=50609420" href="/articles/asx__115296014">Brauner Urin : Myoglobininduziertes Nierenversagen nach gleichzeitiger Gabe von Simvastatin und Amiodaron.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__115296014" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__115296014" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="Coqo3fDhjaLWqWVPW3n4PmxHSey8SFwj+UH54n9mwv4y/j1fY9Gt94/gqGu3D/Rv005jE/LLlIyQiXhJOmuz4w==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__115296014" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Pietsch, U., Müller-Höcker, C., Filipovic, M., and Müller-Höcker, C</p></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Rhabdomyolysis is a rare but well-known complication of statin therapy. The risk is considerably increased when concomitant drugs are administered that inhibit metabolism and breakdown via the cytochrome CYP3A4. We report a case of myoglobin-induced acute renal failure secondary to the concomitant use of simvastatin and amiodarone. The risk of rhabdomyolysis is mainly determined by the statin dose; in the case of the concomitant use of CYP3A4 inhibitors, a maximal daily dose of 20 mg is recommended to avoid harmful drug interactions. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2016</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1007/s00101-016-0171-6">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__45071764" data-document-counter="271" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-271"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 271. </span> <a data-context-href="/articles/asx__45071764/track?counter=271&document_id=asx__45071764&search_id=50609420" href="/articles/asx__45071764">A fatal case of myocardial damage due to misuse of the “designer drug” MDMA</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__45071764" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__45071764" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="WtsI5+QITjAVEVvc+iU+c48zY6GkEXrg/vOlEchL7T9DebiCNExVmCibAZ5bvZoVtR8l9dvDLpQNYrao9f4vOQ==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__45071764" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Sano, Rie, Hasuike, Toshikazu, Nakano, Minoru, Kominato, Yoshihiko, and Itoh, Hideaki</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22DESIGNER+drugs%22">DESIGNER drugs</searchLink>, *<searchLink fieldCode="DE" term="%22ECSTASY+%28Drug%29%22">ECSTASY (Drug)</searchLink>, *<searchLink fieldCode="DE" term="%22LOSS+of+consciousness%22">LOSS of consciousness</searchLink>, *<searchLink fieldCode="DE" term="%22CAUSES+of+death%22">CAUSES of death</searchLink>, *<searchLink fieldCode="DE" term="%22AUTOPSY%22">AUTOPSY</searchLink>, *<searchLink fieldCode="DE" term="%22HEART+diseases%22">HEART diseases</searchLink>, *<searchLink fieldCode="DE" term="%22DRUG+side+effects%22">DRUG side effects</searchLink>, *<searchLink fieldCode="DE" term="%22INFLAMMATION%22">INFLAMMATION</searchLink>, *<searchLink fieldCode="DE" term="%22IMMUNOHISTOCHEMISTRY%22">IMMUNOHISTOCHEMISTRY</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Abstract: A 39-year-old woman collapsed after oral intake of 3,4-methylenedioxymethyl-amphetamine (MDMA, “ecstasy”). After ingestion of the drug, she had felt persistent discomfort in her anterior chest area, and lost consciousness for a few minutes on the following morning. She was transported to a hospital and died seven days after collapse. A serum sample obtained on admission revealed an MDMA concentration of 1.2mg/L, but no evidence of any other drug including amphetamine, methamphetamine, or other ring-substituted amphetamines. Microscopic examination at autopsy revealed striking changes in the heart, including small foci of myocyte necrosis with a surrounding macrophage inflammatory response, foci of fibrosis, and calcification accompanied by myocyte necrosis, these changes being predominant in the right ventricle. In the liver, hepatic necrosis was observed with fatty degeneration accompanied by inflammation. Myoglobinuria was demonstrated in the kidney by immunohistochemistry. Degeneration of neurons throughout the whole brain was also evident, in addition to haemorrhagic foci in the pons and medulla. Serious bronchopneumonia was also found in the right lung. These findings provide evidence that oral intake of MDMA can result in cardiotoxicity, inducing cardiac arrhythmia and cardiovascular collapse. As a consequence of the compromised blood supply, brain necrosis may occur, followed by severe bronchopneumonia. Ingestion of MDMA could also lead to liver damage as well as myoglobinuria resulting from rhabdomyolysis. These data suggest that death in this case had been caused largely by MDMA intoxication. [Copyright &y& Elsevier] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2009</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1016/j.legalmed.2009.09.003">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__43273471" data-document-counter="272" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-272"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 272. </span> <a data-context-href="/articles/asx__43273471/track?counter=272&document_id=asx__43273471&search_id=50609420" href="/articles/asx__43273471">RHABDOMYOLYSIS IN A COLLEGIATE FOOTBALL PLAYER.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__43273471" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__43273471" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="AeD5m+VD7TZz9othnQeA1Xi3acUzC1bKjrlCxCDE9+6UdGX3TPIfwaaEXvCTAbmt/ucrZmyJNXTSz2+0/P1nnA==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__43273471" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> MOECKEL-COLE, STEPHANIE A. and CLARKSON, PRISCILLA M.</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22SPORTS+injuries%22">SPORTS injuries</searchLink>, *<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22STRIATED+muscle+necrosis%22">STRIATED muscle necrosis</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22MUSCLE+injuries%22">MUSCLE injuries</searchLink>, *<searchLink fieldCode="DE" term="%22PATIENTS%22">PATIENTS</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> The article presents an overview of rhabdomyolysis, which is a serious potentially life threatening condition seen during athletic training where striated muscle tissue breaks down, releasing the cellular constituents into the extracellular fluid and circulation. The case of an 18-year-old place kicker who developed rhabdomyolysis following a supervised practice session led by the team's strength and conditioning coach is discussed. </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2009</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1519/JSC.0b013e3181ad316b">View/download PDF</a></dd> </dl> </article><article data-document-id="edo__41587631" data-document-counter="273" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-273"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 273. </span> <a data-context-href="/articles/edo__41587631/track?counter=273&document_id=edo__41587631&search_id=50609420" href="/articles/edo__41587631">Gluteal Compartment Syndrome After Prolonged Immobilisation.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="edo__41587631" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/edo__41587631" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="4QjSkLpJOC+S9PP7qV/55LjxtivF6h3JhwAFtBtecbLeq7RtIdIbUGPggh71mv3qEtP3otdNdMTuZGMd5h5L7A==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_edo__41587631" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Liu, H.L. and Wong, David S.Y.</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors"><searchLink fieldCode="DE" term="%22BUTTOCKS%22">BUTTOCKS</searchLink>, <searchLink fieldCode="DE" term="%22COMPARTMENT+syndrome%22">COMPARTMENT syndrome</searchLink>, <searchLink fieldCode="DE" term="%22MUSCLE+diseases%22">MUSCLE diseases</searchLink>, <searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Muscles in the gluteal region are confined by distinct fascial attachments which can potentially result in compartment syndrome. A 74-year-old chronic drinker was admitted to the medical ward after being found drunk on the street. He noticed acute painful swelling of the right side of his buttock the following morning and recalled a slip and fall prior to his blackout. The whole right half of the buttock was tense with erythematous overlying skin. Examination revealed sciatic nerve palsy and myoglobinuria. Emergency fasciotomy and debridement were performed. Intra-operative pressure measurement confirmed a grossly elevated intra-compartmental pressure. Gluteal compartment syndrome is an extremely rare condition and has only been scantily documented previously in case reports. Early diagnosis is crucial but delay recognition is common from lack of knowledge of the condition and readily results in permanent sciatic nerve injury and acute renal shutdown from myoglobinuria. Awareness of the condition, early diagnosis and prompt exploration provide the only chance of avoiding these devastating consequences. Acute swelling diffusely affecting the whole or one side of the buttock, a history of trauma and prolonged local pressure impingement associated with pain out of proportion to the clinical signs should raise a suspicion of this rare condition. [Copyright &y& Elsevier] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2009</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1016/S1015-9584(09)60023-3">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__36970344" data-document-counter="274" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-274"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 274. </span> <a data-context-href="/articles/asx__36970344/track?counter=274&document_id=asx__36970344&search_id=50609420" href="/articles/asx__36970344">Myopathic form of phosphoglycerate kinase (PGK) deficiency: A new case and pathogenic considerations</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__36970344" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__36970344" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="l7ZXV5Q5BZr712J+q3jHq/2FfTOmW/f6OHxW2S6VrcVOOqYN3v5wFJpNq/fpJYUvGZNHSVm9xqFTdVfrbM1n9Q==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__36970344" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Spiegel, Ronen, Gomez, Estela Area, Akman, Hasan O., Krishna, Sindu, Horovitz, Yoseph, and DiMauro, Salvatore</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22MUSCLE+diseases%22">MUSCLE diseases</searchLink>, *<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22HEMOLYTIC+anemia%22">HEMOLYTIC anemia</searchLink>, *<searchLink fieldCode="DE" term="%22HEMOLYSIS+%26+hemolysins%22">HEMOLYSIS & hemolysins</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Abstract: We describe an 18-year-old man with muscle cramps and recurrent exertional myoglobinuria, without hemolytic anemia or brain dysfunction. Phosphoglycerate kinase (PGK) deficiency was documented in muscle and erythrocytes and molecular analysis of the PGK1 gene identified a novel mutation, T378P. This is the ninth case presenting with isolated myopathy, whereas most other patients show hereditary non-spherocytic hemolytic anemia alone or associated with brain dysfunction, and a few patients have myopathy plus brain involvement. Although the diverse tissue involvement in PGK deficiency remains unclear, all mutations in myopathic patients tend to cluster in the C terminal domain, adjacent to the substrate-binding pocket. This may lead to a failure in the closure of the N terminal and C terminal domains and loss of stability due to lack of inter-domain communication during the catalytic process. [Copyright &y& Elsevier] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2009</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1016/j.nmd.2008.12.004">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__34999055" data-document-counter="275" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-275"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 275. </span> <a data-context-href="/articles/asx__34999055/track?counter=275&document_id=asx__34999055&search_id=50609420" href="/articles/asx__34999055">Mutations in LPIN1 Cause Recurrent Acute Myoglobinuria in Childhood.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__34999055" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__34999055" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="lKFntmQodte0QbDAPShiX4MJ0np6RwQpu1worhR0LVi94eW3jjujQbREhHqp8MnP/OFrw3WUorCwv6Yim7SsHQ==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__34999055" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Zeharia, Avraham, Shaag, Avraham, Houtkooper, Riekelt H., Hindi, Tareq, De Lonlay, Pascale, Erez, Gilli, Hubert, Laurence, Saada, Ann, De Keyzer, Yves, Eshel, Gideon, Vaz, Frédéric M., Pines, Ophry, and Elpeleg, Orly</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22GLYCOGENOLYSIS%22">GLYCOGENOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22MICROBIAL+mutation%22">MICROBIAL mutation</searchLink>, *<searchLink fieldCode="DE" term="%22FATTY+acids%22">FATTY acids</searchLink>, *<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22GENE+mapping%22">GENE mapping</searchLink>, *<searchLink fieldCode="DE" term="%22PATIENTS%22">PATIENTS</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Recurrent episodes of life-threatening myoglobinuria in childhood are caused by inborn errors of glycogenolysis, mitochondrial fatty acid beta-oxidation, and oxidative phosphorylation. Nonetheless, approximately half of the patients do not suffer from a defect in any of these pathways. Using homozygosity mapping, we identified six deleterious mutations in the LPIN1 gene in patients who presented at 2-7 years of age with recurrent, massive rhabdomyolysis. The LPIN1 gene encodes the muscle-specific phosphatidic acid phosphatase, a key enzyme in triglyceride and membrane phospholipid biosynthesis. Of six individuals who developed statin-induced myopathy, one was a carrier for Glu769Gly, a pathogenic mutation in the LPIN1 gene. Analysis of phospholipid content disclosed accumulation of phosphatidic acid and lysophospholipids in muscle tissue of the more severe genotype. Mutations in the LPIN1 gene cause recurrent rhabdomyolysis in childhood, and a carrier state may predispose for statin-induced myopathy. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2008</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1016/j.ajhg.2008.09.002">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__34926862" data-document-counter="276" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-276"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 276. </span> <a data-context-href="/articles/asx__34926862/track?counter=276&document_id=asx__34926862&search_id=50609420" href="/articles/asx__34926862">McArdle disease: what do neurologists need to know?</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__34926862" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__34926862" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="SRKty+FOsl0RRobSrS0l5SY+1GENZMQlcJa+g+8r82Gt16h3uvC0M5AW4Ed2Ap1Vd+9f9cOR/NM3UIdVjuiAdg==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__34926862" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Lucia, Alejandro, Nogales-Gadea, Gisela, Pérez, Margarita, Martín, Miguel A., Andreu, Antoni L., and Arenas, Joaquín</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22GLYCOGEN+storage+disease%22">GLYCOGEN storage disease</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22PHYSICAL+fitness%22">PHYSICAL fitness</searchLink>, *<searchLink fieldCode="DE" term="%22NEUROLOGISTS%22">NEUROLOGISTS</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> McArdle disease (also known as glycogen storage disease type V) is a pure myopathy caused by an inherited deficit of myophosphorylase, the skeletal muscle isoform of the enzyme glycogen phosphorylase. The disease exhibits clinical heterogeneity, but patients typically experience exercise intolerance, that is, reversible, acute crises (early fatigue and contractures, sometimes with rhabdomyolysis and myoglobinuria) triggered by static muscle contractions (e.g. lifting weights) or dynamic exercise (e.g. climbing stairs or running). In this Review, we discuss the main features of McArdle disease, with the aim of providing neurologists with up-to-date, useful information to assist their patients. The topics covered include diagnostic tools—for example, molecular genetic diagnosis, the classic ischemic forearm test and the so-called 'second wind' phenomenon—and current therapeutic options—for example, a carbohydrate-rich diet and carbohydrate ingestion shortly before strenuous exercise, in combination with medically supervised aerobic training of low to moderate intensity. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2008</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1038/ncpneuro0913">View/download PDF</a></dd> </dl> </article><article data-document-id="edb__34651644" data-document-counter="277" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-277"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 277. </span> <a data-context-href="/articles/edb__34651644/track?counter=277&document_id=edb__34651644&search_id=50609420" href="/articles/edb__34651644">Therapeutic Options in Other Metabolic Myopathies</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="edb__34651644" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/edb__34651644" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="orNcpoUUpmz8BeTWiufbUa63jwiwQga+GYcSf80INFbMpuxG4b3E6FocJyCI2ttfDQZF1NIIqoPS7H6bYoPEvw==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_edb__34651644" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Vorgerd, Matthias</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors"><searchLink fieldCode="DE" term="%22MUSCLE+disease+treatment%22">MUSCLE disease treatment</searchLink>, <searchLink fieldCode="DE" term="%22METABOLIC+disorder+treatment%22">METABOLIC disorder treatment</searchLink>, <searchLink fieldCode="DE" term="%22MUSCLE+cramps%22">MUSCLE cramps</searchLink>, <searchLink fieldCode="DE" term="%22FATIGUE+%28Physiology%29%22">FATIGUE (Physiology)</searchLink>, <searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, <searchLink fieldCode="DE" term="%22GLYCOGEN+storage+disease%22">GLYCOGEN storage disease</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Summary: Adult patients with metabolic myopathies typically present with exercise-induced pain, cramps, fatigue, and myoglobinuria. The current therapeutic options of glycogen and lipid storage myopathies include dietary treatments, excersise training, and pharmacological supplementations. Herein is a review of evidence from randomized controlled trials in McArdle disease (glycogen storage disease type V, muscle phosphorylase deficiency) and carnitine palmitoyltransferase (CPT) 2 deficiency. A brief overview on current treatment options in rhabdomyolysis is also included because patients with McArdle disease and CPT 2 often experience such potentially life-threatening complications. [Copyright &y& Elsevier] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2008</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1016/j.nurt.2008.08.006">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__33136011" data-document-counter="278" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-278"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 278. </span> <a data-context-href="/articles/asx__33136011/track?counter=278&document_id=asx__33136011&search_id=50609420" href="/articles/asx__33136011">Caveolinopathy – New mutations and additional symptoms</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__33136011" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__33136011" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="lBXGSjOeXMd7OgwiugtFacGKkt8J/7tJKHPfZG141eQft9jgLA90Y7xpZfvs3mVjwEzoZ9AkB3B2YEkmXm5Sfw==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__33136011" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Aboumousa, Ahmed, Hoogendijk, Jessica, Charlton, Richard, Barresi, Rita, Herrmann, Ralf, Voit, Thomas, Hudson, Judith, Roberts, Mark, Hilton-Jones, David, Eagle, Michelle, Bushby, Kate, and Straub, Volker</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22GENETIC+mutation%22">GENETIC mutation</searchLink>, *<searchLink fieldCode="DE" term="%22GENES%22">GENES</searchLink>, *<searchLink fieldCode="DE" term="%22PHENOTYPES%22">PHENOTYPES</searchLink>, *<searchLink fieldCode="DE" term="%22MUSCULAR+dystrophy%22">MUSCULAR dystrophy</searchLink>, *<searchLink fieldCode="DE" term="%22MUSCLE+diseases%22">MUSCLE diseases</searchLink>, *<searchLink fieldCode="DE" term="%22MYALGIA%22">MYALGIA</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Abstract: Mutations in the caveolin-3 gene (CAV3) can lead to a broad spectrum of clinical phenotypes. Phenotypes that have so far been associated with primary caveolin-3 deficiency include limb girdle muscular dystrophy, rippling muscle disease, distal myopathy and hyperCKaemia. This is the first report describing the clinical, pathological and genetic features of patients with caveolinopathy from the UK. Ten patients (six families) were identified via the National Commissioning Group (NCG) service for patients with limb girdle muscle dystrophy in Newcastle. Myalgia was the most prominent symptom in our cohort of patients and for 50% it was the reason for referral. Muscle weakness was only found in 60% of the patients, whereas rippling muscle movement was present in 80%. One of the patients reported episodes of myoglobinuria and another one episodes of hypoglycaemia. Five different mutations were identified, two of which were novel and three that had previously been described. Caveolinopathy needs to be considered as a differential diagnosis in a range of clinical situations, including in patients who do not have any weakness. Indeed, rippling muscles are a more frequent symptom than weakness, and can be detected in childhood. Presentation with myalgia is common and management of it as well as of myoglobinuria and hypoglycaemia may have a major impact on the patients’ quality of life. [Copyright &y& Elsevier] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2008</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1016/j.nmd.2008.05.003">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__67344530" data-document-counter="279" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-279"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 279. </span> <a data-context-href="/articles/asx__67344530/track?counter=279&document_id=asx__67344530&search_id=50609420" href="/articles/asx__67344530">Clinical role of urinary low molecular weight proteins: Their diagnostic and prognostic implications.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__67344530" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__67344530" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="CED4afj4szs5GjaMzV7oYermzen58zstrTpgIiciH5NhSmDVHqez2lo4+eEjHXp83VYdT5S84ETpy5HE7n/e+Q==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__67344530" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Guder, Walter G. and Hofmann, Walter</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22URINARY+organs%22">URINARY organs</searchLink>, *<searchLink fieldCode="DE" term="%22MOLECULAR+weights%22">MOLECULAR weights</searchLink>, *<searchLink fieldCode="DE" term="%22ENZYMES%22">ENZYMES</searchLink>, *<searchLink fieldCode="DE" term="%22PROTEINS%22">PROTEINS</searchLink>, *<searchLink fieldCode="DE" term="%22URINE%22">URINE</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBIN%22">MYOGLOBIN</searchLink>, *<searchLink fieldCode="DE" term="%22BLADDER%22">BLADDER</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> In traditional urinalysis, casts in the urinary sediment are the only specific signs of renal tubular injury. When tubulo-interstitial fibrosis became the most predictive sign of renal outcome, tubular enzymes derived from proximal tubular brush border or lysosomes were used as early markers of nephrotoxicity and other tubular dysfunctions. More recently, the increase in low molecular weight proteins in urine, assumed to be freely filtered, was reported to reflect tubular dysfunction. This can have pre-renal, renal and post-renal causes. Among the pre-renal causes, Bence Jones protein (immunoglobulin light chains), myoglobin and haemoglobin are signs of extra-renal diseases. On the other hand, β2-microglobulin, α1-microglobulin, retinol binding protein and lysozyme were recommended as tubular markers. Because of its lower pre-renal variability and higher stability in urine during storage in the bladder and urinary vessel, α1-microglobulin proved to be the most valuable in early detection, renal outcome prediction and easy inclusion in routine analytical programmes. In addition, other markers of intra-renal inflammatory processes may help to mirror histological changes occurring in the kidney. Future guidelines should therefore include low molecular protein as a tubular marker. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2008</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1080/00365510802150174">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__32201614" data-document-counter="280" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-280"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 280. </span> <a data-context-href="/articles/asx__32201614/track?counter=280&document_id=asx__32201614&search_id=50609420" href="/articles/asx__32201614">Macrophagic Myofasciitis in Children Is a Localized Reaction to Vaccination.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__32201614" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__32201614" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="ftOSica6ORyje2V2lfcObL9do7B4MbHZsib8i5ahlkjQjOwO6u3z3XsLccvO5Faddo5HjaFuSpIoax0OAtCYoA==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__32201614" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Lach, Boleslaw and Cupler, Edward J.</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22MUSCLE+diseases%22">MUSCLE diseases</searchLink>, *<searchLink fieldCode="DE" term="%22FASCIITIS%22">FASCIITIS</searchLink>, *<searchLink fieldCode="DE" term="%22BIOPSY%22">BIOPSY</searchLink>, *<searchLink fieldCode="DE" term="%22MUSCULAR+atrophy+in+children%22">MUSCULAR atrophy in children</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22CYTOCHROME+c%22">CYTOCHROME c</searchLink>, *<searchLink fieldCode="DE" term="%22SPINAL+muscular+atrophy%22">SPINAL muscular atrophy</searchLink>, *<searchLink fieldCode="DE" term="%22DUCHENNE+muscular+dystrophy%22">DUCHENNE muscular dystrophy</searchLink>, *<searchLink fieldCode="DE" term="%22PEDIATRIC+neurology%22">PEDIATRIC neurology</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Macrophagic myofasciitis is a novel, "inflammatory myopathy" described after a variety of vaccinations, almost exclusively in adults. We examined the relevance of histological findings of this myopathy to the clinical presentation in pediatric patients. Muscle biopsies from 8 children (7 months to 6 years old) with histological features of macrophagic myofasciitis were reviewed and correlated with the clinical manifestations. Patients underwent quadriceps muscle biopsy for suspected mitochondrial disease (4 patients), spinal muscular atrophy (2 patients), myoglobinuria (1 patient), and hypotonia with motor delay (1 patient). All biopsies showed identical granulomas composed of periodic acid-Schiff-positive and CD68-positive macrophages. Characteristic aluminum hydroxide crystals were identified by electron microscopy in 2 cases. The biopsy established diagnoses other than macrophagic myofasciitis in 5 patients: spinal muscular atrophy (2), Duchenne muscular dystrophy (1), phospho-glycerate kinase deficiency (1), and cytochrome c oxidase deficiency (1). Three children with manifestations and/or a family history of mitochondrial disease had otherwise morphologically normal muscle. All children had routine vaccinations between 2 months and 1 year before the biopsy, with up to 11 intramuscular injections, including the biopsy sites. There was no correlation between histological findings of macrophagic myofasciitis in biopsies and the clinical symptoms. We believe that macrophagic myofasciitis represents a localized histological hallmark of previous immunization with the aluminum hydroxide adjuvants contained in vaccines, rather than a primary or distinct inflammatory muscle disease. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2008</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1177/0883073807312370">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__31275073" data-document-counter="281" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-281"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 281. </span> <a data-context-href="/articles/asx__31275073/track?counter=281&document_id=asx__31275073&search_id=50609420" href="/articles/asx__31275073">Splice Mutation in the Iron-Sulfur Cluster Scaffold Protein ISCU Causes Myopathy with Exercise Intolerance.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__31275073" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__31275073" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="tE4jsifPEcHn7LiGH44GsY3CiiLbzJhFSiADnfcEctdwOLa+Y43wZQL8HUZACP3wDSkQdi1nRgY/sdslucqTcg==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__31275073" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Mochel, Fanny, Knight, Melanie A., Wing-Hang Tong, Hernandez, Dena, Ayyad, Karen, Taivassalo, Tanja, Andersen, Peter M., Singleton, Andrew, Rouault, Tracey A., Fischbeck, Kenneth H., and Haller, Ronald G.</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22GENETIC+mutation%22">GENETIC mutation</searchLink>, *<searchLink fieldCode="DE" term="%22MUSCLE+diseases%22">MUSCLE diseases</searchLink>, *<searchLink fieldCode="DE" term="%22EXERCISE%22">EXERCISE</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22SUCCINATE+dehydrogenase%22">SUCCINATE dehydrogenase</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> A myopathy with severe exercise intolerance and myoglobinuria has been described in patients from northern Sweden, with associated deficiencies of succinate dehydrogenase and aconitase in skeletal muscle. We identified the gene for the iron-sulfur cluster scaffold protein ISCU as a candidate within a region of shared homozygosity among patients with this disease. We found a single mutation in ISCU that likely strengthens a weak splice acceptor site, with consequent exon retention. A marked reduction of ISCU mRNA and mitochondrial ISCU protein in patient muscle was associated with a decrease in the iron regulatory protein IRP1 and intracellular iron overload in skeletal muscle, consistent with a muscle-specific alteration of iron homeostasis in this disease. ISCU interacts with the Friedreich ataxia gene product frataxin in iron-sulfur cluster biosynthesis. Our results therefore extend the range of known human diseases that are caused by defects in iron-sulfur cluster biogenesis. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2008</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1016/j.ajhg.2007.12.012">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__30068449" data-document-counter="282" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-282"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 282. </span> <a data-context-href="/articles/asx__30068449/track?counter=282&document_id=asx__30068449&search_id=50609420" href="/articles/asx__30068449">Myoglobin Induces Oxidative Stress and Decreases Endocytosis and Monolayer Permissiveness in Cultured Kidney Epithelial Cells without Affecting Viability.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__30068449" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__30068449" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="w3FIWB1ozC37I6CQKIUUU236714cEfnE/s570Kby1nBtXM4QQmQCq8QW+BXm3QPI+/UTaGWEl0MJlymcj9vRIQ==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__30068449" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Parry, Sarah N., Ellis, Natasha, Zhe Li, Maitz, Peter, and Witting, Paul K.</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22MYOGLOBIN%22">MYOGLOBIN</searchLink>, *<searchLink fieldCode="DE" term="%22BLOOD+proteins%22">BLOOD proteins</searchLink>, *<searchLink fieldCode="DE" term="%22OXIDATIVE+stress%22">OXIDATIVE stress</searchLink>, *<searchLink fieldCode="DE" term="%22OXIDATION-reduction+reaction%22">OXIDATION-reduction reaction</searchLink>, *<searchLink fieldCode="DE" term="%22ENDOCYTOSIS%22">ENDOCYTOSIS</searchLink>, *<searchLink fieldCode="DE" term="%22EPITHELIAL+cells%22">EPITHELIAL cells</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Background: Muscle degradation caused by severe burn releases myoglobin (Mb), which accumulates in the kidney (termed myoglobinuria). Mb is a pro-oxidant. Aim: To demonstrate that Mb promotes oxidative stress and dysfunction in cultured Madin-Darby canine kidney type II (MDCK II) cells. Methods: The glutathione redox ratio was used to monitor oxidative stress. Regulation of antioxidant response genes was determined with RT-PCR. Propidium iodide and annexin V staining were markers of necrosis and apoptosis, respectively. Mitochondrial function was assessed by monitoring mitochondrial depolarisation. Endocytosis was determined with immune fluorescence microscopy, and monolayer permeability was monitored with labelled inulin. Results: Kidney epithelial cells exposed to (0–100 μM) Mb showed a dose-dependent decrease in the glutathione redox ratio indicative of enhanced oxidative stress. In parallel, the expression of antioxidant genes for superoxide dismutase (SOD)-1/2, inducible haemoxygenase (HO-1) and catalase (CAT) increased in MDCK II cells, coupled with increases in corresponding activity. Notably, apoptosis and necrosis remained unaffected. However, transferrin endocytosis and monolayer permeability decreased significantly, while clathrin distribution and mitochondrial function were unaffected. Conclusion: Low concentrations of Mb promote oxidative stress in kidney epithelial cells that manifest as subtle changes to function without decreasing viability. Whether this impairs kidney function in burns patients is not clear. Copyright © 2008 S. Karger AG, Basel [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2008</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1159/000112921">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__35683129" data-document-counter="283" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-283"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 283. </span> <a data-context-href="/articles/asx__35683129/track?counter=283&document_id=asx__35683129&search_id=50609420" href="/articles/asx__35683129">Human CoQ_{10} deficiencies.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__35683129" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__35683129" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="6n+IoTZBWhIfGP3jnH9R/Yn5URo+N+dAHj9QykBP9Pg7+0JDvUNLZ7ZApOvOki6TypRhMNxNajtcSDpQNoS9Pg==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__35683129" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Quinzii, C. M., López, L. C., Naini, A., DiMauro, S., and Hirano, M.</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22UBIQUINONES%22">UBIQUINONES</searchLink>, *<searchLink fieldCode="DE" term="%22CELL+membranes%22">CELL membranes</searchLink>, *<searchLink fieldCode="DE" term="%22MITOCHONDRIA%22">MITOCHONDRIA</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22CEREBELLAR+ataxia%22">CEREBELLAR ataxia</searchLink>, *<searchLink fieldCode="DE" term="%22GENES%22">GENES</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Coenzyme Q_{10} (CoQ_{10} or ubiquinone) is a lipid-soluble component of virtually all cell membranes and has multiple metabolic functions. A major function of CoQ_{10} is to transport electrons from complexes I and II to complex III in the respiratory chain which resides in the mitochondrial inner membrane. Deficiencies of CoQ_{10} (MIM 607426) have been associated with four major clinical phenotypes: 1) encephalomyopathy characterized by a triad of recurrent myoglobinuria, brain involvement, and ragged-red fibers; 2) infantile multisystemic disease typically with prominent nephropathy and encephalopathy; 3) cerebellar ataxia with marked cerebellar atrophy; and 4) pure myopathy. Primary CoQ_{10} deficiencies due to mutations in ubiquinone biosynthetic genes (COQ2, PDSS1, PDSS2, and ADCK3 [CABC1]) have been identified in patients with the infantile multisystemic and cerebellar ataxic phenotypes. In contrast, secondary CoQ_{10} deficiencies, due to mutations in genes not directly related to ubiquinone biosynthesis (APTX, ETFDH, and BRAF), have been identified in patients with cerebellar ataxia, pure myopathy, and cardiofaciocutaneous syndrome. In many patients with CoQ_{10} deficiencies, the causative molecular genetic defects remain unknown; therefore, it is likely that mutations in additional genes will be identified as causes of CoQ_{10} deficiencies. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2008</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1002/biof.5520320113">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__30094323" data-document-counter="284" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-284"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 284. </span> <a data-context-href="/articles/asx__30094323/track?counter=284&document_id=asx__30094323&search_id=50609420" href="/articles/asx__30094323">Genetic determinants of statin intolerance.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__30094323" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__30094323" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="KEjEocImj+cP4l+YUnpMNsCVA2aqjC6hzTXBuoCb3yT0kJGlgcbvigIbySkmumnOvC8IY3+idAvY4glOlrB7dQ==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__30094323" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Jisun Oh, Ban, Matthew R., Miskie, Brooke A., Pollex, Rebecca L., and Hegele, Robert A.</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22STATINS+%28Cardiovascular+agents%29%22">STATINS (Cardiovascular agents)</searchLink>, *<searchLink fieldCode="DE" term="%22MUSCLE+diseases%22">MUSCLE diseases</searchLink>, *<searchLink fieldCode="DE" term="%22MYOSITIS%22">MYOSITIS</searchLink>, *<searchLink fieldCode="DE" term="%22CREATININE%22">CREATININE</searchLink>, *<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22GENETIC+polymorphisms%22">GENETIC polymorphisms</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Background: Statin-related skeletal muscle disorders range from benign myalgias — such as nonspecific muscle aches or joint pains without elevated serum creatinine kinase (CK) concentration — to true myositis with >10-fold elevation of serum CK, to rhabdomyolysis and myoglobinuria. The genetic basis of statin-related muscle disorders is largely unknown. Because mutations in the COQ2 gene are associated with severe inherited myopathy, we hypothesized that common, mild genetic variation in COQ2 would be associated with inter-individual variation in statin intolerance. We studied 133 subjects who developed myopathy on statin monotherapy and 158 matched controls who tolerated statins without incident or complaint. Results: COQ2 genotypes, based on two single nucleotide polymorphisms (SNP1 and SNP2) and a 2-SNP haplotype, all showed significant associations with statin intolerance. Specifically, the odds ratios (with 95% confidence intervals) for increased risk of statin intolerance among homozygotes for the rare alleles were 2.42 (0.99 to 5.89), 2.33 (1.13 to 4.81) and 2.58 (1.26 to 5.28) for SNP1 and SNP2 genotypes, and the 2-SNP haplotype, respectively. Conclusion: These preliminary pharmacogenetic results, if confirmed, are consistent with the idea that statin intolerance which is manifested primarily through muscle symptoms is associated with genomic variation in COQ2 and thus perhaps with the CoQ10 pathway. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2007</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1186/1476-511X-6-7">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__24828455" data-document-counter="285" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-285"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 285. </span> <a data-context-href="/articles/asx__24828455/track?counter=285&document_id=asx__24828455&search_id=50609420" href="/articles/asx__24828455">Rabdomiólisis e insuficiencia renal aguda.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__24828455" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__24828455" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="zGq8D25YN0MGyZzAroU+H6bwIUJHTKsbGRMBUzZyx4ZcM0IZQjRuE80Oqe73oYX1Y79h3eup9wS+Ojm5ExgM5w==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__24828455" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Mote, Jesús Duarte, Meza, Salvador Díaz, and Castro, Víctor Enrique Lee Eng</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22ISCHEMIA%22">ISCHEMIA</searchLink>, *<searchLink fieldCode="DE" term="%22REPERFUSION%22">REPERFUSION</searchLink>, *<searchLink fieldCode="DE" term="%22ALCOHOLISM%22">ALCOHOLISM</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22BLOOD+cells%22">BLOOD cells</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Rhabdomyolysis is the liberation of components of injured skeletal muscle into the circulation. There are many etiologies of rhabdomyolysis. Direct compression of muscle leading to a local crush injury is the most common mechanism of traumatic rhabdomyolysis. Compression causes muscle ischemia, as tissue pressure rises to a level that exceeds capillary perfusion pressure. When the compression is relieved, the muscle tissue is reperfused. Muscle ischemia followed by reperfusion (ischemia—reperfusion—injury) represents the fundamental pathophysiologic mechanism of rhabdomyolysis. Acute alcohol intoxication with subsequent immobility and coma is the most common etiologic factor of direct muscle compression. Other etiologies are infectious, metabolic and genetics. Dark, tea-colored urine that is dipstick positive for blood despite the absence of red blood cells on microscopy is suggestive of myoglobinuria and rhabdomyolysis. The quickest and least expensive screening test for rhabdomyolysis is the serum CK level. Acute renal failure is one of its most serious consequences and occurs in 4 to 33% of cases, carrying with it a mortality rate of 3 to 50%. The vigorous fluid resuscitation is the cornerstone of the treatment. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2007</dd> </dl> </article><article data-document-id="asx__23951935" data-document-counter="286" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-286"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 286. </span> <a data-context-href="/articles/asx__23951935/track?counter=286&document_id=asx__23951935&search_id=50609420" href="/articles/asx__23951935">PGK deficiency.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__23951935" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__23951935" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="gpTztaXB4rMbOgoU/liHNAjTDSqpsbUtFmymZMbrxlbJwLvO0TNvN7Nyl3xDHpfGzrC/uxVuTpFWZkRNTN7t/g==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__23951935" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Beutler, Ernest</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22ENOLASE%22">ENOLASE</searchLink>, *<searchLink fieldCode="DE" term="%22HEMOLYTIC+anemia%22">HEMOLYTIC anemia</searchLink>, *<searchLink fieldCode="DE" term="%22ERYTHROCYTES%22">ERYTHROCYTES</searchLink>, *<searchLink fieldCode="DE" term="%22MUSCLE+diseases%22">MUSCLE diseases</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22INTELLECTUAL+disabilities%22">INTELLECTUAL disabilities</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Phosphoglycerate kinase (PGK) deficiency is one of the relatively uncommon causes of hereditary non-spherocytic haemolytic anaemia (HNSHA). The gene encoding the erythrocyte enzyme PGK1, is X-linked. Mutations of this gene may cause chronic haemolysis with or without mental retardation and they may cause myopathies, often with episodes of myoglobinuria, or a combination of these clinical manifestations. Twenty-six families have been described and in 20 of these the mutations are known. The reason for different clinical manifestations of mutations of the same gene remains unknown. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2007</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1111/j.1365-2141.2006.06351.x">View/download PDF</a></dd> </dl> </article><article data-document-id="edo__142101148" data-document-counter="287" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-287"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 287. </span> <a data-context-href="/articles/edo__142101148/track?counter=287&document_id=edo__142101148&search_id=50609420" href="/articles/edo__142101148">Exertional Rhabdomyolysis in Civilian and Military Populations.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="edo__142101148" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/edo__142101148" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="MtF5j2A6VDWCsWyR2d44QYDYZmTGtCCXLPOFaxbO/1PR/Hy42PHqZmqz9ksTcwKK2Sd8+b1esHiXA/2KTJQP6w==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_edo__142101148" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Eichner, E. Randy</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors"><searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, <searchLink fieldCode="DE" term="%22MILITARY+administration%22">MILITARY administration</searchLink>, <searchLink fieldCode="DE" term="%22CIVILIAN+evacuation%22">CIVILIAN evacuation</searchLink>, <searchLink fieldCode="DE" term="%22EPIDEMIOLOGY%22">EPIDEMIOLOGY</searchLink>, <searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> The article discusses Exertional Rhabdomyolysis in Civilian and Military Populations. Topics include Persons who developed ER in Olmsted County, MN from 2003 to 2015 were identified via the Rochester Epidemiology Project, using ICD-9 codes for rhabdomyolysis or myoglobinuria; and the military calls for greater awareness and preventive actions by commanders, risk of ER can be reduced, the military advises, by taking into account fitness and fatness. </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2020</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1249/JSR.0000000000000690">View/download PDF</a></dd> </dl> </article><article data-document-id="edsair__edsair-doi-dedup-11d9d85a5fd88c6f92182b50d07607b9" data-document-counter="288" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight- document document-position-288"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 288. </span> <a data-context-href="/articles/edsair__edsair.doi.dedup.....11d9d85a5fd88c6f92182b50d07607b9/track?counter=288&document_id=edsair__edsair.doi.dedup.....11d9d85a5fd88c6f92182b50d07607b9&search_id=50609420" href="/articles/edsair__edsair.doi.dedup.....11d9d85a5fd88c6f92182b50d07607b9">Exertional rhabdomyolysis leading to acute kidney injury: when genetic defects are diagnosed in adult life</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="edsair__edsair.doi.dedup.....11d9d85a5fd88c6f92182b50d07607b9" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/edsair__edsair.doi.dedup.....11d9d85a5fd88c6f92182b50d07607b9" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="MBXohYxSYfH4ozUAEaYoyB+Qm9Nk1G51l3SwVh7HxHjIcxaebpuGRQbzjjVb/T5Ojca4j1gcpX16qAa9uN0RlQ==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_edsair__edsair.doi.dedup.....11d9d85a5fd88c6f92182b50d07607b9" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Francesco Reggiani, Irene Faravelli, Irene Colombo, David Cucchiari, Rossella Valentino, Manuel Alfredo Podestà, Salvatore Badalamenti, Silvia Testolin, Maurizio Moggio, and Ottavia Amato</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors"><searchLink fieldCode="DE" term="%22Nephrology%22">Nephrology</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Emedical%5Fspecialty%22">medicine.medical_specialty</searchLink>, <searchLink fieldCode="DE" term="%22Creatinine%22">Creatinine</searchLink>, <searchLink fieldCode="DE" term="%22Urinalysis%22">Urinalysis</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Ediagnostic%5Ftest%22">medicine.diagnostic_test</searchLink>, <searchLink fieldCode="DE" term="%22business%2Eindustry%22">business.industry</searchLink>, <searchLink fieldCode="DE" term="%22Myoglobinuria%22">Myoglobinuria</searchLink>, <searchLink fieldCode="DE" term="%22Acute+kidney+injury%22">Acute kidney injury</searchLink>, <searchLink fieldCode="DE" term="%22Renal+function%22">Renal function</searchLink>, <searchLink fieldCode="DE" term="%22Case+Report%22">Case Report</searchLink>, <searchLink fieldCode="DE" term="%22General+Medicine%22">General Medicine</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Edisease%22">medicine.disease</searchLink>, <searchLink fieldCode="DE" term="%2203+medical+and+health+sciences%22">03 medical and health sciences</searchLink>, <searchLink fieldCode="DE" term="%22chemistry%2Echemical%5Fcompound%22">chemistry.chemical_compound</searchLink>, <searchLink fieldCode="DE" term="%220302+clinical+medicine%22">0302 clinical medicine</searchLink>, <searchLink fieldCode="DE" term="%22chemistry%22">chemistry</searchLink>, <searchLink fieldCode="DE" term="%22Internal+medicine%22">Internal medicine</searchLink>, <searchLink fieldCode="DE" term="%22Exertional+rhabdomyolysis%22">Exertional rhabdomyolysis</searchLink>, <searchLink fieldCode="DE" term="%22Medicine%22">Medicine</searchLink>, <searchLink fieldCode="DE" term="%22030212+general+%26+internal+medicine%22">030212 general & internal medicine</searchLink>, <searchLink fieldCode="DE" term="%22business%22">business</searchLink>, <searchLink fieldCode="DE" term="%22Rhabdomyolysis%22">Rhabdomyolysis</searchLink>, <searchLink fieldCode="DE" term="%22030217+neurology+%26+neurosurgery%22">030217 neurology & neurosurgery</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Rhabdomyolysis is a common cause of acute kidney injury (AKI) that is usually triggered by trauma. However, less common causes of rhabdomyolysis may precipitate AKI as well, possibly representing a diagnostic challenge even for the experienced nephrologist. Genetic defects of muscle metabolism represent one of these causes and can be overlooked in adults, since these diseases usually become apparent in childhood. We present here a case in which an adult patient with severe exertional rhabdomyolysis leading to AKI was finally diagnosed with a genetic defect of lipid metabolism. A 41-year-old patient was brought to our attention because of AKI and pigmenturia after strenuous physical effort. At admission, the patient was over-hydrated with a weight increase of 3 kg in few days. Laboratory examination showed creatinine of 8.7 mg/dl, along with increased myoglobin and CPK. Urinalysis was positive for haemoglobin and proteins, while urinary sediment analysis did not demonstrate any red blood cell but rather “muddy-brown” casts and tubular cells. Urine output was forced and the patient completely recovered renal function. Genetic analysis later demonstrated the presence of a common mutation of Carnitine Palmitoyl-Transferase II (CPTII). When facing rhabdomyolysis of obscure origin, nephrologists must keep in mind the possibility that even adult patients may have a genetic defect of energy metabolism. In these cases, patients usually experience rhabdomyolysis during exertion, fasting, or infection. CPTII deficiency often has a subtle presentation and might be unrecognized until AKI develops. Therefore, it is important to consider a genetic defect of muscle metabolism even in adult patients when a history of rhabdomyolysis of unclear origin is present. </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2017</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1007/s13730-017-0292-z">View/download PDF</a></dd> </dl> </article><article data-document-id="edsair__edsair-doi-a54b9bd6ef0b3ab76af20ae44d25c3c2" data-document-counter="289" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight- document document-position-289"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 289. </span> <a data-context-href="/articles/edsair__edsair.doi...........a54b9bd6ef0b3ab76af20ae44d25c3c2/track?counter=289&document_id=edsair__edsair.doi...........a54b9bd6ef0b3ab76af20ae44d25c3c2&search_id=50609420" href="/articles/edsair__edsair.doi...........a54b9bd6ef0b3ab76af20ae44d25c3c2">Clinics in diagnostic imaging (179)</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="edsair__edsair.doi...........a54b9bd6ef0b3ab76af20ae44d25c3c2" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/edsair__edsair.doi...........a54b9bd6ef0b3ab76af20ae44d25c3c2" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="8JJkJ1f4iZF61Xi6+wy1xeiutBwfSuyeaXeWckz2GYHrX2ysG1fY6U2WEInB55wdZLACVH5l/Cl9Yx3t2zbiFQ==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_edsair__edsair.doi...........a54b9bd6ef0b3ab76af20ae44d25c3c2" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Shi Xian Shawn Kok and Tien Jin Tan</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors"><searchLink fieldCode="DE" term="%22medicine%2Emedical%5Fspecialty%22">medicine.medical_specialty</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Ediagnostic%5Ftest%22">medicine.diagnostic_test</searchLink>, <searchLink fieldCode="DE" term="%22biology%22">biology</searchLink>, <searchLink fieldCode="DE" term="%22business%2Eindustry%22">business.industry</searchLink>, <searchLink fieldCode="DE" term="%22Myoglobinuria%22">Myoglobinuria</searchLink>, <searchLink fieldCode="DE" term="%22Magnetic+resonance+imaging%22">Magnetic resonance imaging</searchLink>, <searchLink fieldCode="DE" term="%22General+Medicine%22">General Medicine</searchLink>, <searchLink fieldCode="DE" term="%22Emergency+department%22">Emergency department</searchLink>, <searchLink fieldCode="DE" term="%22Thigh%22">Thigh</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Edisease%22">medicine.disease</searchLink>, <searchLink fieldCode="DE" term="%22030218+nuclear+medicine+%26+medical+imaging%22">030218 nuclear medicine & medical imaging</searchLink>, <searchLink fieldCode="DE" term="%2203+medical+and+health+sciences%22">03 medical and health sciences</searchLink>, <searchLink fieldCode="DE" term="%220302+clinical+medicine%22">0302 clinical medicine</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Eanatomical%5Fstructure%22">medicine.anatomical_structure</searchLink>, <searchLink fieldCode="DE" term="%22030220+oncology+%26+carcinogenesis%22">030220 oncology & carcinogenesis</searchLink>, <searchLink fieldCode="DE" term="%22medicine%22">medicine</searchLink>, <searchLink fieldCode="DE" term="%22biology%2Eprotein%22">biology.protein</searchLink>, <searchLink fieldCode="DE" term="%22Creatine+kinase%22">Creatine kinase</searchLink>, <searchLink fieldCode="DE" term="%22Radiology%22">Radiology</searchLink>, <searchLink fieldCode="DE" term="%22Gluteal+muscles%22">Gluteal muscles</searchLink>, <searchLink fieldCode="DE" term="%22business%22">business</searchLink>, <searchLink fieldCode="DE" term="%22Rhabdomyolysis%22">Rhabdomyolysis</searchLink>, <searchLink fieldCode="DE" term="%22Myositis%22">Myositis</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> A 32-year-old man presented to the emergency department with severe right lower limb pain and swelling of three days' duration. He had multiple prior admissions for recurrent seizures and suicide attempts. Markedly elevated serum creatine kinase levels and urine myoglobinuria were consistent with a diagnosis of rhabdomyolysis. Initial magnetic resonance imaging of the right lower limb revealed diffuse muscle oedema and features of myositis in the gluteal muscles and the adductor, anterior and posterior compartments of the thigh. Follow-up magnetic resonance imaging performed 11 days later showed interval development of areas of myonecrosis and haemorrhage. The causes, clinical presentation and imaging features of rhabdomyolysis are discussed. </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2017</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.11622/smedj.2017081">View/download PDF</a></dd> </dl> </article><article data-document-id="edsair__edsair-doi-dedup-cf3ad25c7c4f35349e70fa2655c72f9f" data-document-counter="290" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight- document document-position-290"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 290. </span> <a data-context-href="/articles/edsair__edsair.doi.dedup.....cf3ad25c7c4f35349e70fa2655c72f9f/track?counter=290&document_id=edsair__edsair.doi.dedup.....cf3ad25c7c4f35349e70fa2655c72f9f&search_id=50609420" href="/articles/edsair__edsair.doi.dedup.....cf3ad25c7c4f35349e70fa2655c72f9f">Exercise‐induced acute renal failure in a trainee cyclist without hypouricemia: Successful athletic career post‐treatment</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="edsair__edsair.doi.dedup.....cf3ad25c7c4f35349e70fa2655c72f9f" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/edsair__edsair.doi.dedup.....cf3ad25c7c4f35349e70fa2655c72f9f" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="P612p+2LeDo4vVRovDEevHtCZOnKqtaxXsqQaOnzxw+y1ygB29Q9522kB9OSaWhncEqgrS2GuewAVK8mmpIpSw==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_edsair__edsair.doi.dedup.....cf3ad25c7c4f35349e70fa2655c72f9f" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Koji Takaori, Sayako Maeda, and Yoko Shimizu</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors"><searchLink fieldCode="DE" term="%22musculoskeletal+diseases%22">musculoskeletal diseases</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Emedical%5Fspecialty%22">medicine.medical_specialty</searchLink>, <searchLink fieldCode="DE" term="%22030232+urology+%26+nephrology%22">030232 urology & nephrology</searchLink>, <searchLink fieldCode="DE" term="%22Case+Report%22">Case Report</searchLink>, <searchLink fieldCode="DE" term="%22Case+Reports%22">Case Reports</searchLink>, <searchLink fieldCode="DE" term="%22030204+cardiovascular+system+%26+hematology%22">030204 cardiovascular system & hematology</searchLink>, <searchLink fieldCode="DE" term="%22urologic+and+male+genital+diseases%22">urologic and male genital diseases</searchLink>, <searchLink fieldCode="DE" term="%22acute+renal+failure%22">acute renal failure</searchLink>, <searchLink fieldCode="DE" term="%2203+medical+and+health+sciences%22">03 medical and health sciences</searchLink>, <searchLink fieldCode="DE" term="%220302+clinical+medicine%22">0302 clinical medicine</searchLink>, <searchLink fieldCode="DE" term="%22Internal+medicine%22">Internal medicine</searchLink>, <searchLink fieldCode="DE" term="%22Internal+Medicine%22">Internal Medicine</searchLink>, <searchLink fieldCode="DE" term="%22medicine%22">medicine</searchLink>, <searchLink fieldCode="DE" term="%22RENAL+HYPOURICEMIA%22">RENAL HYPOURICEMIA</searchLink>, <searchLink fieldCode="DE" term="%22ALPE%22">ALPE</searchLink>, <searchLink fieldCode="DE" term="%22Hypouricemia%22">Hypouricemia</searchLink>, <searchLink fieldCode="DE" term="%22Renal+ischemia%22">Renal ischemia</searchLink>, <searchLink fieldCode="DE" term="%22exercise%22">exercise</searchLink>, <searchLink fieldCode="DE" term="%22renal+hypouricemia%22">renal hypouricemia</searchLink>, <searchLink fieldCode="DE" term="%22business%2Eindustry%22">business.industry</searchLink>, <searchLink fieldCode="DE" term="%22musculoskeletal%2C+neural%2C+and+ocular+physiology%22">musculoskeletal, neural, and ocular physiology</searchLink>, <searchLink fieldCode="DE" term="%22Myoglobinuria%22">Myoglobinuria</searchLink>, <searchLink fieldCode="DE" term="%22Serum+uric+acid%22">Serum uric acid</searchLink>, <searchLink fieldCode="DE" term="%22Acute+kidney+injury%22">Acute kidney injury</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Edisease%22">medicine.disease</searchLink>, <searchLink fieldCode="DE" term="%22acute+kidney+injury%22">acute kidney injury</searchLink>, <searchLink fieldCode="DE" term="%22Physical+therapy%22">Physical therapy</searchLink>, <searchLink fieldCode="DE" term="%22Geriatrics+and+Gerontology%22">Geriatrics and Gerontology</searchLink>, <searchLink fieldCode="DE" term="%22Post+treatment%22">Post treatment</searchLink>, <searchLink fieldCode="DE" term="%22Family+Practice%22">Family Practice</searchLink>, <searchLink fieldCode="DE" term="%22business%22">business</searchLink>, <searchLink fieldCode="DE" term="%22Anaerobic+exercise%22">Anaerobic exercise</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Acute renal failure with severe loin pain and patchy renal ischemia after anaerobic exercise (ALPE) is exercise‐induced acute renal failure that occurs without myoglobinuria. We describe a typical case involving an 18‐year‐old man. Generally, patients with ALPE are advised to avoid anaerobic exercise due to risk of recurrence, but our patient continued and went on to become a professional cyclist without relapse. About 51% of ALPE cases involve patients with renal hypouricemia. His serum uric acid levels were rather high, at 6.4 mg/dL. He is the first patient with ALPE to succeed as a professional athlete in an anaerobic sport. </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2017</dd> </dl> </article><article data-document-id="asx__22537742" data-document-counter="291" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-291"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 291. </span> <a data-context-href="/articles/asx__22537742/track?counter=291&document_id=asx__22537742&search_id=50609420" href="/articles/asx__22537742">Bortezomib-Induced Rhabdomyolysis in Multiple Myeloma.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__22537742" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__22537742" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="Wz4lo9/neo3oX6SXOiBtQk7/nsNg+erouH+6WbO9/rxNp+1ussHkHhU+t8oo6Aofd3a59KM1JhFNrMhPCH7Bew==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__22537742" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Cibeira, M. Teresa, Mercadal, Santiago, Arenillas, Leonor, Muntañola, Anna, Salamero, Olga, and Bladé, Joan</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22DRUG+side+effects%22">DRUG side effects</searchLink>, *<searchLink fieldCode="DE" term="%22STRIATED+muscle+necrosis%22">STRIATED muscle necrosis</searchLink>, *<searchLink fieldCode="DE" term="%22MULTIPLE+myeloma%22">MULTIPLE myeloma</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Although multiple myeloma (MM) remains an incurable disease, its treatment has improved over the past decade. This improvement has been at least in part due to the introduction of novel antimyeloma agents with new mechanisms of action, including those that target both myeloma cells and the tumor microenvironment, with antiangiogenic and immunomodulatory properties. Among these drugs, bortezomib (Velcade®), a selective proteasome inhibitor, has been approved for the treatment of relapsed and refractory MM patients after one line of therapy. The toxicity profile of bortezomib includes gastrointestinal symptoms, fatigue, thrombocytopenia, peripheral neuropathy, postural hypotension, as well as some uncommon events. A patient with relapsed MM who developed recurrent bortezomib-induced rhabdomyolysis is reported. To our knowledge, this adverse event has not been previously described is this context. Copyright © 2006 S. Karger AG, Basel [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2006</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1159/000094682">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__21880592" data-document-counter="292" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-292"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 292. </span> <a data-context-href="/articles/asx__21880592/track?counter=292&document_id=asx__21880592&search_id=50609420" href="/articles/asx__21880592">The effect of myoglobin concentration on aerobic dive limit in a Weddell seal.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__21880592" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__21880592" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="vlHnW7pgz2Gp2nQBnQryg56ceMtWJHzDrCGdZNviIsK+2VoOqCz+pIqRQxnNWslL3eAf4r5B8SObJnnfTbpj+A==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__21880592" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Wright, T. J. and Davis, R. W.</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22WEDDELL+seal%22">WEDDELL seal</searchLink>, *<searchLink fieldCode="DE" term="%22LEPTONYCHOTES%22">LEPTONYCHOTES</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBIN%22">MYOGLOBIN</searchLink>, *<searchLink fieldCode="DE" term="%22BLOOD+proteins%22">BLOOD proteins</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22MUSCLE+proteins%22">MUSCLE proteins</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> One physiological adaptation for prolonged dive duration in marine mammals is an elevated myoglobin (Mb) concentration in skeletal muscle. To determine the influence of Mb concentration on the aerobic dive limit (ADL), we modified a previously published model that simulated aerobic dives in a Weddell seal (Leptonychotes weddellii) and ran it for four Mb concentrations: 5, 27, 54 and 108 g Mb kg-1 muscle representing 7%, 50%, 100% and 200%, respectively, of the normal Mb concentration in Weddell seal skeletal muscle. The model was run at increasing levels of muscular exertion and under postabsorptive and postprandial conditions to determine their effect on ADL. For each set of conditions, the model was also run at different levels of cardiac output (i.e. the dive response was varied) to determine the level of convective oxygen transport that optimized the ADL. In a postabsorptive state at a routine level of muscular exertion for a diving Weddell seal, a decrease in Mb concentration to 7% of normal caused a 39% decrease in the ADL (18 min to 11 min), while doubling the Mb concentration increased the ADL by 30% (18 min to 24 min). Under postprandial conditions at a routine level of muscular exertion, doubling the Mb concentration did not increase the ADL (12 min). The convective oxygen transport needed to meet the metabolic demands (Heat Increment of Feeding, HIF) of the splanchnic organs during digestion and assimilation required a cardiac output that was not optimal for the efficient use of muscle oxygen stores. This resulted in an over perfusion of the muscles and incomplete use of myoglobin-bound oxygen. As a result, the postprandial ADL was limited by the amount of oxygen stored in the blood, and increasing the Mb concentration had no effect on the ADL. We hypothesize that myoglobin concentration is optimized for the type and duration of dives routinely made by Weddell seals, and that a further increase may not increase the ADL for most free-ranging dives. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2006</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1242/jeb.02273">View/download PDF</a></dd> </dl> </article><article data-document-id="edsair__edsair-doi-dedup-7d26d503f8222cb964223da283518e87" data-document-counter="293" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight- document document-position-293"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 293. </span> <a data-context-href="/articles/edsair__edsair.doi.dedup.....7d26d503f8222cb964223da283518e87/track?counter=293&document_id=edsair__edsair.doi.dedup.....7d26d503f8222cb964223da283518e87&search_id=50609420" href="/articles/edsair__edsair.doi.dedup.....7d26d503f8222cb964223da283518e87">McArdle disease: a 'pediatric' disorder presenting in an adult with acute kidney injury</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="edsair__edsair.doi.dedup.....7d26d503f8222cb964223da283518e87" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/edsair__edsair.doi.dedup.....7d26d503f8222cb964223da283518e87" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="wPZ254aqyWgRVT2sLOeBObd/6c+jIHhi9e9rvsxnahOQLo+5dyL4mLR2/Rocw+I/XKB89d4u16Mg+wGLpA4jXw==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_edsair__edsair.doi.dedup.....7d26d503f8222cb964223da283518e87" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Michael Muriello, Angela Li, Xixi Zhao, Madhu Soni, Carolyn Jones, and William L. Whittier</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors"><searchLink fieldCode="DE" term="%22Nephrology%22">Nephrology</searchLink>, <searchLink fieldCode="DE" term="%22Pediatrics%22">Pediatrics</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Emedical%5Fspecialty%22">medicine.medical_specialty</searchLink>, <searchLink fieldCode="DE" term="%22Pathology%22">Pathology</searchLink>, <searchLink fieldCode="DE" term="%22MCARDLE+DISEASE%22">MCARDLE DISEASE</searchLink>, <searchLink fieldCode="DE" term="%22business%2Eindustry%22">business.industry</searchLink>, <searchLink fieldCode="DE" term="%22Myoglobinuria%22">Myoglobinuria</searchLink>, <searchLink fieldCode="DE" term="%22Acute+kidney+injury%22">Acute kidney injury</searchLink>, <searchLink fieldCode="DE" term="%22Case+Report%22">Case Report</searchLink>, <searchLink fieldCode="DE" term="%22General+Medicine%22">General Medicine</searchLink>, <searchLink fieldCode="DE" term="%22Disease%22">Disease</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Edisease%22">medicine.disease</searchLink>, <searchLink fieldCode="DE" term="%2203+medical+and+health+sciences%22">03 medical and health sciences</searchLink>, <searchLink fieldCode="DE" term="%220302+clinical+medicine%22">0302 clinical medicine</searchLink>, <searchLink fieldCode="DE" term="%22Internal+medicine%22">Internal medicine</searchLink>, <searchLink fieldCode="DE" term="%22medicine%22">medicine</searchLink>, <searchLink fieldCode="DE" term="%22Etiology%22">Etiology</searchLink>, <searchLink fieldCode="DE" term="%22030212+general+%26+internal+medicine%22">030212 general & internal medicine</searchLink>, <searchLink fieldCode="DE" term="%22business%22">business</searchLink>, <searchLink fieldCode="DE" term="%22Acute+rhabdomyolysis%22">Acute rhabdomyolysis</searchLink>, <searchLink fieldCode="DE" term="%22Rhabdomyolysis%22">Rhabdomyolysis</searchLink>, <searchLink fieldCode="DE" term="%22030217+neurology+%26+neurosurgery%22">030217 neurology & neurosurgery</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Rhabdomyolysis is characterized by the acute breakdown of skeletal muscle, resulting in the release of muscle cell contents, subsequent myoglobinuria, and in severe cases, acute renal failure. A number of etiologies have been identified in acute rhabdomyolysis, in which drugs and trauma account for the majority of cases. One etiological category that is commonly overlooked in the adult population is an underlying genetic defect. This may be challenging to diagnose due to its rarity in the adult demographic and the marked heterogeneity, often requiring a high level of clinical suspicion before investigation is pursued. Once diagnosed, however, appropriate steps can be taken to reduce future episodes of rhabdomyolysis, further renal injury, and other systemic complications. Here, we report a case of an adult patient presenting with acute rhabdomyolysis secondary to McArdle disease, a genetic disease causing defective glycogenolysis. The case highlights the importance of recognizing the potential of undiagnosed “pediatric” disorders in adulthood and particularly for underlying genetic causes of rhabdomyolysis. </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2017</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1007/s13730-017-0265-2">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__20179847" data-document-counter="294" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-294"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 294. </span> <a data-context-href="/articles/asx__20179847/track?counter=294&document_id=asx__20179847&search_id=50609420" href="/articles/asx__20179847">Myopathy is a prominent feature in Marinesco-Sjögren syndrome.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__20179847" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__20179847" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="boGHj/AKbf6WFHCkMmh8xa/FpL/0bip7C3vhVdw94QlLkYHnYknNxALGwTK/qvQHqpvCp+ba7EcOuwSYEDrBhQ==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__20179847" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Mahjneh, Ibrahim, Anttonen, Anna-Kaisa, Somer, Mirja, Paetau, Anders, Lehesjoki, Anna-Elina, Somer, Hannu, and Udd, Bjarne</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22GENETICS%22">GENETICS</searchLink>, *<searchLink fieldCode="DE" term="%22HETEROGENEITY%22">HETEROGENEITY</searchLink>, *<searchLink fieldCode="DE" term="%22CEREBELLAR+ataxia%22">CEREBELLAR ataxia</searchLink>, *<searchLink fieldCode="DE" term="%22CATARACT%22">CATARACT</searchLink>, *<searchLink fieldCode="DE" term="%22MOVEMENT+disorders%22">MOVEMENT disorders</searchLink>, *<searchLink fieldCode="DE" term="%22INTELLECTUAL+disabilities%22">INTELLECTUAL disabilities</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22NEUROPATHY%22">NEUROPATHY</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Background Marinesco-Sjögren syndrome (MSS) is an autosomal recessive multiorgan disorder showing clinical and genetic heterogeneity. The key features of MSS include cerebellar ataxia, early bilateral cataracts, delayed motor development, and varying degrees of mental retardation. Patients with a subtype of MSS with myoglobinuria and neuropathy have been linked to chromosome 18qter, and recently a locus for classical MSS has been localized on chromosome 5q31. Objective To determine the importance of myopathy in this disorder apart from the CNS based disability and to establish the pattern of muscle involvement and degree of its severity. Methods Muscle computed tomography (CT) investigations were carried out in nine Finnish MSS patients homozygous for markers around the MSS locus on chromosome 5q31. Results Patients with severe clinical disability showed severe and generalized muscle degeneration. Muscle CT findings in patients with relatively severe clinical picture were characterized by severe involvement of the posterior thoracic and pelvic muscles,and almost all thigh muscles. In the legs the peronei and posterior compartment muscles were severely degenerated. The group of patients with moderate severity of disease showed the same pattern of involved muscle, albeit with lower degree of muscle degeneration. Conclusions Patients with MSS linked to chromosome 5q31 have a severe progressive myopathy, the extent of which may remain largely unrecognized because of the CNS involvement. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2006</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1007/s00415-005-0983-9">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__20338358" data-document-counter="295" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-295"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 295. </span> <a data-context-href="/articles/asx__20338358/track?counter=295&document_id=asx__20338358&search_id=50609420" href="/articles/asx__20338358">The use of extracorporeal life support in the treatment of influenza-associated myositis/rhabdomyolysis.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__20338358" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__20338358" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="yenDhH45XBsyfBeA34zfCkUmz4OX6w/wcewvrcM94csoXnxMJ0spj4D9LTj3sVoBM1kQNqvheAvOGwxVqfbCrg==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__20338358" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Augustin, Simon L., Horton, Stephen, Thuys, Clarke, Bennett, Martin, Claessen, Catie, and Brizard, Christian</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22FATIGUE+%28Physiology%29%22">FATIGUE (Physiology)</searchLink>, *<searchLink fieldCode="DE" term="%22HEADACHE%22">HEADACHE</searchLink>, *<searchLink fieldCode="DE" term="%22MUSCLE+diseases%22">MUSCLE diseases</searchLink>, *<searchLink fieldCode="DE" term="%22EDEMA%22">EDEMA</searchLink>, *<searchLink fieldCode="DE" term="%22EXTRACORPOREAL+membrane+oxygenation%22">EXTRACORPOREAL membrane oxygenation</searchLink>, *<searchLink fieldCode="DE" term="%22ACUTE+kidney+failure%22">ACUTE kidney failure</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> A 13-year-old girl presented to the emergency department with fatigue, headaches and muscle stiffness after returning from a family camping trip. Within 24 h, she was transferred to ICU with general oedema and low saturations, where she had a cardio-respiratory arrest and was placed on veno-arterial extracorporeal membrane oxygenation (ECMO). The patient was successfully supported with ECMO for profound myocardial dysfunction and haemofiltration for rhabdomyolysis and acute renal failure. Patients who present with profound myocardial dysfunction and myoglobinuria as a consequence of viral infection can be successfully supported with ECMO. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2006</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1191/0267659106pf850oa">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__20408054" data-document-counter="296" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-296"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 296. </span> <a data-context-href="/articles/asx__20408054/track?counter=296&document_id=asx__20408054&search_id=50609420" href="/articles/asx__20408054">Recurrent Rhabdomyolysis in a Collegiate Athlete: A Case Report.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__20408054" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__20408054" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="8ICZGYCSSE/BQLxM9Kee69kfZBB+S/vBgyNWmwzphsriJt93r1LmDhBlamqwP+k8OQS3eYZL+Xzx6ijHhldW+g==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__20408054" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Krivickas, Lisa S.</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22RHABDOMYOLYSIS%22">RHABDOMYOLYSIS</searchLink>, *<searchLink fieldCode="DE" term="%22STRIATED+muscle+necrosis%22">STRIATED muscle necrosis</searchLink>, *<searchLink fieldCode="DE" term="%22ATHLETES%22">ATHLETES</searchLink>, *<searchLink fieldCode="DE" term="%22METABOLIC+disorders%22">METABOLIC disorders</searchLink>, *<searchLink fieldCode="DE" term="%22DISEASES%22">DISEASES</searchLink>, *<searchLink fieldCode="DE" term="%22CARNITINE%22">CARNITINE</searchLink>, *<searchLink fieldCode="DE" term="%22VITAMIN+B+complex%22">VITAMIN B complex</searchLink>, *<searchLink fieldCode="DE" term="%22PHOSPHORYLASES%22">PHOSPHORYLASES</searchLink>, *<searchLink fieldCode="DE" term="%22GLYCOSYLTRANSFERASES%22">GLYCOSYLTRANSFERASES</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Purpose: Hereditary metabolic disorders can cause rhabdomyolysis in athletes. Team physicians should be aware of the presentation, workup, and management of the most common of these disorders, carnitine palmitoyltransferase (CPT) II deficiency and muscle phosphorylase deficiency. Methods: The case of a collegiate athlete with recurrent bouts of rhabdomyolysis is presented, and the diagnostic workup is discussed. Results: The patient described in this case has CPT II deficiency. The diagnosis and management of CPT II deficiency and muscle phosphorylase deficiency (McArdle's disease) are discussed. Conclusion: Athletes with rhabdomyolysis, in the absence of an obvious cause such as drug toxicity, severe trauma, or excessive exercise, should be evaluated for the presence of a metabolic myopathy. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2006</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1249/01.mss.0000187413.41416.7e">View/download PDF</a></dd> </dl> </article><article data-document-id="asx__19813051" data-document-counter="297" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight-academic-journal document document-position-297"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 297. </span> <a data-context-href="/articles/asx__19813051/track?counter=297&document_id=asx__19813051&search_id=50609420" href="/articles/asx__19813051">PROTEIN SYNTHESIS CHANGE IN BRAIN SUB CELLULAR PARTICLES AND SOLUBLE FRACTION AT THE CRUSH SYNDROME.</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="asx__19813051" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/asx__19813051" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="RMLiW95wmeieqDNyd6ja1+9ThZXjPBnkbJjLcC11DOXxcDL/rc/GHSNYtWMmeXfWhUDT+lHQppdTOBkTHA/MdA==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_asx__19813051" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Kevorkian, G. A., Kanayan, A. S., Guevorkian, A. G., Hayrapetyan, H. L., and Galoyan, A. A.</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors">*<searchLink fieldCode="DE" term="%22CRUSH+syndrome%22">CRUSH syndrome</searchLink>, *<searchLink fieldCode="DE" term="%22PROTEIN+synthesis%22">PROTEIN synthesis</searchLink>, *<searchLink fieldCode="DE" term="%22MYOGLOBINURIA%22">MYOGLOBINURIA</searchLink>, *<searchLink fieldCode="DE" term="%22ACUTE+kidney+failure%22">ACUTE kidney failure</searchLink>, *<searchLink fieldCode="DE" term="%22NEUROPHYSINS%22">NEUROPHYSINS</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Crush of soft tissues is followed by acute hemodynamic shock, myoglobinuria, acute renal insufficiency, and lethal endotoxicity. Research on the pathogenesis of crush syndrome has shown that the largest changes in crush occur during decompression and are accompanied by acute alteration of brain protein synthesis and strong morphological changes of brain structures. The investigations (by Prof. A. Galoyan) have shown that a praline rich peptide originates from proteolysis of C-terminal glycoprotein a neurophysin II and along with vasopressin and oxytocin is transferred from the hypothalamus to the neurohypophysis by axonal transport. During 2-hour compression protein synthesis decreased in cytosol (32.7%) and mitochondria (49%), after 5-h compression non-significant changes occurred in the level of protein synthesis. In 2, 4, 24, and 48 h of decompression after 2-h compression, and in 2- and 48-h decompression after 5-h compression; the level of protein synthesis in brain subcellular particles decreased. After intraperitoneal administration of proline-rich peptide (10mcg per 100g weight of white rats) activation of the protein synthesis occurs in all studied particles and the soluble fraction of brain cells. The positive effect of the peptide is conditioned, most probably, on activation of the immune system and adaptation mechanisms, including mobilization of endogen-protective mechanisms of the organism itself. [ABSTRACT FROM AUTHOR] </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2006</dd> </dl> </article><article data-document-id="edsair__edsair-doi-997393acc49f5c3164c635c191c96f55" data-document-counter="298" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight- document document-position-298"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 298. </span> <a data-context-href="/articles/edsair__edsair.doi...........997393acc49f5c3164c635c191c96f55/track?counter=298&document_id=edsair__edsair.doi...........997393acc49f5c3164c635c191c96f55&search_id=50609420" href="/articles/edsair__edsair.doi...........997393acc49f5c3164c635c191c96f55">Clinical protocol for the management of malignant hyperthermia</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="edsair__edsair.doi...........997393acc49f5c3164c635c191c96f55" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/edsair__edsair.doi...........997393acc49f5c3164c635c191c96f55" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="92QwPqk6fwXDteNIDAKKd+OjnsHINQi+HFcUbjABwhPnigHEEUvX86e814ckq5jf7VmqaHyQGvsD5tMBB6/A/A==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_edsair__edsair.doi...........997393acc49f5c3164c635c191c96f55" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> M.J. Yepes, B. del Blanco, Antonio Domínguez, J. L. Guerrero, Angeles García, A. Kollmann-Camaiora, and E. Alsina</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors"><searchLink fieldCode="DE" term="%22Disseminated+intravascular+coagulation%22">Disseminated intravascular coagulation</searchLink>, <searchLink fieldCode="DE" term="%22Tachycardia%22">Tachycardia</searchLink>, <searchLink fieldCode="DE" term="%22Ryanodine+receptor%22">Ryanodine receptor</searchLink>, <searchLink fieldCode="DE" term="%22business%2Eindustry%22">business.industry</searchLink>, <searchLink fieldCode="DE" term="%22Myoglobinuria%22">Myoglobinuria</searchLink>, <searchLink fieldCode="DE" term="%22Malignant+hyperthermia%22">Malignant hyperthermia</searchLink>, <searchLink fieldCode="DE" term="%22030208+emergency+%26+critical+care+medicine%22">030208 emergency & critical care medicine</searchLink>, <searchLink fieldCode="DE" term="%22General+Medicine%22">General Medicine</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Edisease%22">medicine.disease</searchLink>, <searchLink fieldCode="DE" term="%22Dantrolene+Sodium%22">Dantrolene Sodium</searchLink>, <searchLink fieldCode="DE" term="%2203+medical+and+health+sciences%22">03 medical and health sciences</searchLink>, <searchLink fieldCode="DE" term="%22Respiratory+acidosis%22">Respiratory acidosis</searchLink>, <searchLink fieldCode="DE" term="%220302+clinical+medicine%22">0302 clinical medicine</searchLink>, <searchLink fieldCode="DE" term="%22030202+anesthesiology%22">030202 anesthesiology</searchLink>, <searchLink fieldCode="DE" term="%22Anesthesia%22">Anesthesia</searchLink>, <searchLink fieldCode="DE" term="%22medicine%22">medicine</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Esymptom%22">medicine.symptom</searchLink>, <searchLink fieldCode="DE" term="%22Halothane%22">Halothane</searchLink>, <searchLink fieldCode="DE" term="%22business%22">business</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Edrug%22">medicine.drug</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Malignant hyperthermia is a hypermetabolic syndrome that appears in susceptible patients after exposure to certain anaesthetic drugs (succinylcholine, inhalation anaesthetics). Its incidence in Spain is 1 in 40,000 adults, with a 10% mortality rate. It is induced by an abnormal regulation of the ryanodine receptors, producing a massive release of calcium from the sarcoplasmic reticulum in the striate muscle. Clinical manifestations include: CO2 increase, tachycardia, haemodynamic instability, metabolic and respiratory acidosis, profuse sweating, hyperpyrexia, CPK increase, myoglobinuria, kidney failure, disseminated intravascular coagulation (DIC), and ending in cardiac arrest. Dantrolene sodium is a ryanodine receptor antagonist, and inhibits the release of intracellular calcium. Definitive diagnosis is achieved by the exposure of muscle fibres to caffeine and halothane. Protocols can help guarantee a reliable and secure management when this severe event occurs. </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2017</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.1016/j.redare.2016.11.001">View/download PDF</a></dd> </dl> </article><article data-document-id="edsair__edsair-doi-13aef170a99b8c33d340f871f5e74b5c" data-document-counter="299" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight- document document-position-299"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 299. </span> <a data-context-href="/articles/edsair__edsair.doi...........13aef170a99b8c33d340f871f5e74b5c/track?counter=299&document_id=edsair__edsair.doi...........13aef170a99b8c33d340f871f5e74b5c&search_id=50609420" href="/articles/edsair__edsair.doi...........13aef170a99b8c33d340f871f5e74b5c">A novel PGK1 mutation associated with neurological dysfunction and the absence of episodes of hemolytic anemia or myoglobinuria</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="edsair__edsair.doi...........13aef170a99b8c33d340f871f5e74b5c" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/edsair__edsair.doi...........13aef170a99b8c33d340f871f5e74b5c" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="+p9qovqACg1nyueqflY4F1dCQjewm6X2hxhUCtJAw0T1K3dO1vrdgerybPBTFhpB6uNgRmofrCxi6v5YHrEgKQ==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_edsair__edsair.doi...........13aef170a99b8c33d340f871f5e74b5c" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Keiko Shimojima, Toshiyuki Yamamoto, Hirokazu Oguni, Shigeto Matsumaru, Satoru Nagata, Hitoshi Kanno, and Hiromi Ogura</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors"><searchLink fieldCode="DE" term="%220301+basic+medicine%22">0301 basic medicine</searchLink>, <searchLink fieldCode="DE" term="%22Hemolytic+anemia%22">Hemolytic anemia</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Emedical%5Fspecialty%22">medicine.medical_specialty</searchLink>, <searchLink fieldCode="DE" term="%22Phosphoglycerate+kinase%22">Phosphoglycerate kinase</searchLink>, <searchLink fieldCode="DE" term="%22Mutation%22">Mutation</searchLink>, <searchLink fieldCode="DE" term="%22business%2Eindustry%22">business.industry</searchLink>, <searchLink fieldCode="DE" term="%22Myoglobinuria%22">Myoglobinuria</searchLink>, <searchLink fieldCode="DE" term="%22Central+nervous+system%22">Central nervous system</searchLink>, <searchLink fieldCode="DE" term="%22Muscle+weakness%22">Muscle weakness</searchLink>, <searchLink fieldCode="DE" term="%22General+Medicine%22">General Medicine</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Edisease%5Fcause%22">medicine.disease_cause</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Edisease%22">medicine.disease</searchLink>, <searchLink fieldCode="DE" term="%22Molecular+biology%22">Molecular biology</searchLink>, <searchLink fieldCode="DE" term="%2203+medical+and+health+sciences%22">03 medical and health sciences</searchLink>, <searchLink fieldCode="DE" term="%22030104+developmental+biology%22">030104 developmental biology</searchLink>, <searchLink fieldCode="DE" term="%220302+clinical+medicine%22">0302 clinical medicine</searchLink>, <searchLink fieldCode="DE" term="%22Endocrinology%22">Endocrinology</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Eanatomical%5Fstructure%22">medicine.anatomical_structure</searchLink>, <searchLink fieldCode="DE" term="%22Internal+medicine%22">Internal medicine</searchLink>, <searchLink fieldCode="DE" term="%22Etiology%22">Etiology</searchLink>, <searchLink fieldCode="DE" term="%22Medicine%22">Medicine</searchLink>, <searchLink fieldCode="DE" term="%22Glycolysis%22">Glycolysis</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Esymptom%22">medicine.symptom</searchLink>, <searchLink fieldCode="DE" term="%22business%22">business</searchLink>, <searchLink fieldCode="DE" term="%22030217+neurology+%26+neurosurgery%22">030217 neurology & neurosurgery</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Phosphoglycerate kinase (PGK) deficiency affects three different organs: red blood cells (RBC), the central nervous system, and muscles. Next-generation sequencing identified a hemizygous PGK1 mutation (p.V217I) in a 16-year-old Japanese male patient presenting with intellectual disability and episodes of muscle weakness of unknown etiology. Enzymatic analysis demonstrated slightly lower RBC-PGK activity and compensatory increases of other glycolysis enzymes. This is the first PGK1 mutation found through next-generation sequencing. </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2017</dd> <dt class="blacklight-eds_authors col-md-3"><span class="tags-custom">Full Text</span></dt> <dd class="col-md-9 blacklight-eds_authors"><a class="pdf-blue-icon" target="_blank" href="https://doi.org/10.5582/irdr.2017.01020">View/download PDF</a></dd> </dl> </article><article data-document-id="edsair__edsair-doi-dedup-88eb22878510a1bb6bad26f22af14118" data-document-counter="300" itemscope="itemscope" itemtype="http://schema.org/Thing" class="blacklight- document document-position-300"> <header class="documentHeader row"> <h3 class="index_title document-title-heading col-sm-9 col-lg-10"> <span class="document-counter"> 300. </span> <a data-context-href="/articles/edsair__edsair.doi.dedup.....88eb22878510a1bb6bad26f22af14118/track?counter=300&document_id=edsair__edsair.doi.dedup.....88eb22878510a1bb6bad26f22af14118&search_id=50609420" href="/articles/edsair__edsair.doi.dedup.....88eb22878510a1bb6bad26f22af14118">Severe Fever with Thrombocytopenia Syndrome Presenting with Rhabdomyolysis</a> </h3> <div class="index-document-functions col-sm-3 col-lg-2"> <form class="bookmark-toggle" data-doc-id="edsair__edsair.doi.dedup.....88eb22878510a1bb6bad26f22af14118" data-present="In Bookmarks" data-absent="Bookmark" data-inprogress="Saving..." action="/bookmarks/edsair__edsair.doi.dedup.....88eb22878510a1bb6bad26f22af14118" accept-charset="UTF-8" method="post"><input type="hidden" name="_method" value="put" /><input type="hidden" name="authenticity_token" value="MR/qqtsx/rS+umJttJ2es+IZnClLJP+U9R9HMGFY12ZMh/F17Ee+fxK4gi5qxfYbufW4DRiVBYswll1QKdoweQ==" /> <input type="hidden" name="catalog_type" id="catalog_type" value="articles" /> <input type="submit" name="commit" value="Bookmark" id="bookmark_toggle_edsair__edsair.doi.dedup.....88eb22878510a1bb6bad26f22af14118" class="bookmark-add btn btn-outline-secondary" data-disable-with="Bookmark" /> </form> </div> </header> <dl class="document-metadata dl-invert row"> <dt class="blacklight-eds_authors col-md-3">Author</dt> <dd class="col-md-9 blacklight-eds_authors mb-0"> <p class="truncate-text"> Jiwon Jung, Yang Soo Kim, Sung-Han Kim, Sang-Ho Choi, Jun Hee Woo, Sang-Oh Lee, Sang-Bum Hong, and Min Gu Kim</p></dd> <dt class="blacklight-eds_authors col-md-3">Subjects</dt> <dd class="col-md-9 blacklight-eds_authors"><searchLink fieldCode="DE" term="%220301+basic+medicine%22">0301 basic medicine</searchLink>, <searchLink fieldCode="DE" term="%22myalgia%22">myalgia</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Emedical%5Fspecialty%22">medicine.medical_specialty</searchLink>, <searchLink fieldCode="DE" term="%22030106+microbiology%22">030106 microbiology</searchLink>, <searchLink fieldCode="DE" term="%22Case+Report%22">Case Report</searchLink>, <searchLink fieldCode="DE" term="%22urologic+and+male+genital+diseases%22">urologic and male genital diseases</searchLink>, <searchLink fieldCode="DE" term="%22Severe+fever+with+thrombocytopenia+syndrome%22">Severe fever with thrombocytopenia syndrome</searchLink>, <searchLink fieldCode="DE" term="%22Rhabdomyolysis%22">Rhabdomyolysis</searchLink>, <searchLink fieldCode="DE" term="%2203+medical+and+health+sciences%22">03 medical and health sciences</searchLink>, <searchLink fieldCode="DE" term="%22Acute+renal+failure%22">Acute renal failure</searchLink>, <searchLink fieldCode="DE" term="%220302+clinical+medicine%22">0302 clinical medicine</searchLink>, <searchLink fieldCode="DE" term="%22Internal+medicine%22">Internal medicine</searchLink>, <searchLink fieldCode="DE" term="%22Medicine%22">Medicine</searchLink>, <searchLink fieldCode="DE" term="%22Pharmacology+%28medical%29%22">Pharmacology (medical)</searchLink>, <searchLink fieldCode="DE" term="%22030212+general+%26+internal+medicine%22">030212 general & internal medicine</searchLink>, <searchLink fieldCode="DE" term="%22Leukopenia%22">Leukopenia</searchLink>, <searchLink fieldCode="DE" term="%22business%2Eindustry%22">business.industry</searchLink>, <searchLink fieldCode="DE" term="%22Myoglobinuria%22">Myoglobinuria</searchLink>, <searchLink fieldCode="DE" term="%22Febrile+illness%22">Febrile illness</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Edisease%22">medicine.disease</searchLink>, <searchLink fieldCode="DE" term="%22Infectious+Diseases%22">Infectious Diseases</searchLink>, <searchLink fieldCode="DE" term="%22Elevated+muscle+enzyme%22">Elevated muscle enzyme</searchLink>, <searchLink fieldCode="DE" term="%22Azotemia%22">Azotemia</searchLink>, <searchLink fieldCode="DE" term="%22medicine%2Esymptom%22">medicine.symptom</searchLink>, <searchLink fieldCode="DE" term="%22business%22">business</searchLink></dd> <dt class="blacklight-eds_languages col-md-3">Abstract</dt> <dd class="col-md-9 blacklight-eds_languages"><p class="truncate-text"> Severe fever with thrombocytopenia syndrome (SFTS) is an emerging febrile illness. While many kinds of severe complications including acute renal failure have been reported, rhabdomyolysis is rarely reported in association with SFTS. A 54-year-old female farmer was admitted with fever and diffuse myalgia. Laboratory finding showed thrombocytopenia, leukopenia, azotemia, extremely elevated muscle enzyme levels and myoglobinuria. We describe a fatal case of rhabdomyolysis with acute renal failure complicated by SFTS. </p></dd> <dt class="blacklight-eds_authors col-md-3">Published</dt> <dd class="col-md-9 blacklight-eds_authors">2017</dd> </dl> </article> </div> <div class="row record-padding"> <div class="col-md-12"> <nav class="pagination" role="region" aria-label="pagination links"> <ul class="pagination"> <li class="page-item"> <a rel="prev" class="page-link" aria-label="Go to previous page" href="/?page=5&q=%22myoglobinuria%22&search_field=descriptor">Previous</a> </li> <li class="page-item "> <a class="page-link" aria-label="Go to page 1" href="/?q=%22myoglobinuria%22&search_field=descriptor">1</a> </li> <li class="page-item "> <a class="page-link" aria-label="Go to page 2" href="/?page=2&q=%22myoglobinuria%22&search_field=descriptor">2</a> </li> <li class="page-item "> <a class="page-link" aria-label="Go to page 3" href="/?page=3&q=%22myoglobinuria%22&search_field=descriptor">3</a> </li> <li 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