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5. Author Correction: Biallelic mutations in SORD cause a common and potentially treatable hereditary neuropathy with implications for diabetes (Nature Genetics, (2020), 52, 5, (473-481), 10.1038/s41588-020-0615-4)

Author

Cortese A., Zhu Y., Rebelo A. P., Negri S., Courel S., Abreu L., Bacon C. J., Bai Y., Bis-Brewer D. M., Bugiardini E., Buglo E., Danzi M. C., Feely S. M. E., Athanasiou-Fragkouli A., Haridy N. A., Rodriguez A., Bacha A., Kosikowski A., Wood B., McCray B., Blume B., Siskind C., Sumner C., Calabrese D., Walk D., Vujovic D., Park E., Muntoni F., Donlevy G., Acsadi G., Day J., Burns J., Li J., Krajewski K., Eichinger K., Cornett K., Mullen K., Laura P. Q., Gutmann L., Barrett M., Saporta M., Skorupinska M., Grant N., Bray P., Seyedsadjadi R., Zuccarino R., Finkel R., Lewis R., Yum S., Hilbert S., Thomas S., Behrens-Spraggins S., Jones T., Lloyd T., Grider T., Estilow T., Fridman V., Isasi R., Khan A., Laura M., Magri S., Pipis M., Pisciotta C., Powell E., Rossor A. M., Saveri P., Sowden J. E., Tozza S., Vandrovcova J., Dallman J., Grignani E., Marchioni E., Scherer S. S., Tang B., Lin Z., Al-Ajmi A., Schule R., Synofzik M., Maisonobe T., Stojkovic T., Auer-Grumbach M., Abdelhamed M. A., Hamed S. A., Zhang R., Manganelli F., Santoro L., Taroni F., Pareyson D., Houlden H., Herrmann D. N., Reilly M. M., Shy M. E., Zhai R. G., Zuchner S., Cortese, A., Zhu, Y., Rebelo, A. P., Negri, S., Courel, S., Abreu, L., Bacon, C. J., Bai, Y., Bis-Brewer, D. M., Bugiardini, E., Buglo, E., Danzi, M. C., Feely, S. M. E., Athanasiou-Fragkouli, A., Haridy, N. A., Rodriguez, A., Bacha, A., Kosikowski, A., Wood, B., Mccray, B., Blume, B., Siskind, C., Sumner, C., Calabrese, D., Walk, D., Vujovic, D., Park, E., Muntoni, F., Donlevy, G., Acsadi, G., Day, J., Burns, J., Li, J., Krajewski, K., Eichinger, K., Cornett, K., Mullen, K., Laura, P. Q., Gutmann, L., Barrett, M., Saporta, M., Skorupinska, M., Grant, N., Bray, P., Seyedsadjadi, R., Zuccarino, R., Finkel, R., Lewis, R., Yum, S., Hilbert, S., Thomas, S., Behrens-Spraggins, S., Jones, T., Lloyd, T., Grider, T., Estilow, T., Fridman, V., Isasi, R., Khan, A., Laura, M., Magri, S., Pipis, M., Pisciotta, C., Powell, E., Rossor, A. M., Saveri, P., Sowden, J. E., Tozza, S., Vandrovcova, J., Dallman, J., Grignani, E., Marchioni, E., Scherer, S. S., Tang, B., Lin, Z., Al-Ajmi, A., Schule, R., Synofzik, M., Maisonobe, T., Stojkovic, T., Auer-Grumbach, M., Abdelhamed, M. A., Hamed, S. A., Zhang, R., Manganelli, F., Santoro, L., Taroni, F., Pareyson, D., Houlden, H., Herrmann, D. N., Reilly, M. M., Shy, M. E., Zhai, R. G., and Zuchner, S.

Abstract

An amendment to this paper has been published and can be accessed via a link at the top of the paper.

Published
2020

6. Biallelic variants in HPDL cause pure and complicated hereditary spastic paraplegia

Author

Wiessner, M., Maroofian, R., Ni, M.Y., Pedroni, A., Müller, J.S., Stucka, R., Beetz, C., Efthymiou, S., Santorelli, F.M., Alfares, A.A., Zhu, C., Meszarosova, A. Uhrova, Alehabib, E., Bakhtiari, S., Janecke, A.R., Otero, M.G., Chen, J.Y., Peterson, J.T., Strom, T.M., Jonghe, P. De, Deconinck, T., Ridder, W. De, Winter, J., Pasquariello, R., Ricca, I., Alfadhel, M., Warrenburg, B.P.C. van de, Portier, R., Bergmann, C., Firouzabadi, S. Ghasemi, Jin, S.C., Bilguvar, K., Hamed, S., Abdelhameed, M., Haridy, N.A., Maqbool, S., Rahman, F., Anwar, N., Carmichael, J., Pagnamenta, A., Wood, N.W., Mau-Them, F. Tran, Haack, T., Rocco, M. Di, Ceccherini, I., Iacomino, M., Zara, F., Salpietro, V., Scala, M., Rusmini, M., Xu, Y., Wang, Y., Suzuki, Y., Koh, K., Nan, H., Ishiura, H., Tsuji, S., Lambert, L., Schmitt, E., Lacaze, E., Küpper, H., Dredge, D., Skraban, C., Goldstein, A., Willis, M.J.H., Grand, K., Graham, J.M., Lewis, R.A., Millan, F., Duman, Ö., Dündar, N., Uyanik, G., Schöls, L., Nürnberg, P., Nürnberg, G., Bordes, A. Catala, Seeman, P., Kuchar, M., Darvish, H., Rebelo, A., Bouçanova, F., Medard, J.J., Chrast, R., Auer-Grumbach, M., Alkuraya, F.S., Shamseldin, H., Tala, S. Al, Varaghchi, J. Rezazadeh, Najafi, Maryam, Deschner, S., Gläser, D., Hüttel, W., Kruer, M.C., Kamsteeg, E.J., Takiyama, Y., Züchner, S., Baets, J., Synofzik, M., Schüle, R., Horvath, R., Pierson, T.M., Senderek, J., Wiessner, M., Maroofian, R., Ni, M.Y., Pedroni, A., Müller, J.S., Stucka, R., Beetz, C., Efthymiou, S., Santorelli, F.M., Alfares, A.A., Zhu, C., Meszarosova, A. Uhrova, Alehabib, E., Bakhtiari, S., Janecke, A.R., Otero, M.G., Chen, J.Y., Peterson, J.T., Strom, T.M., Jonghe, P. De, Deconinck, T., Ridder, W. De, Winter, J., Pasquariello, R., Ricca, I., Alfadhel, M., Warrenburg, B.P.C. van de, Portier, R., Bergmann, C., Firouzabadi, S. Ghasemi, Jin, S.C., Bilguvar, K., Hamed, S., Abdelhameed, M., Haridy, N.A., Maqbool, S., Rahman, F., Anwar, N., Carmichael, J., Pagnamenta, A., Wood, N.W., Mau-Them, F. Tran, Haack, T., Rocco, M. Di, Ceccherini, I., Iacomino, M., Zara, F., Salpietro, V., Scala, M., Rusmini, M., Xu, Y., Wang, Y., Suzuki, Y., Koh, K., Nan, H., Ishiura, H., Tsuji, S., Lambert, L., Schmitt, E., Lacaze, E., Küpper, H., Dredge, D., Skraban, C., Goldstein, A., Willis, M.J.H., Grand, K., Graham, J.M., Lewis, R.A., Millan, F., Duman, Ö., Dündar, N., Uyanik, G., Schöls, L., Nürnberg, P., Nürnberg, G., Bordes, A. Catala, Seeman, P., Kuchar, M., Darvish, H., Rebelo, A., Bouçanova, F., Medard, J.J., Chrast, R., Auer-Grumbach, M., Alkuraya, F.S., Shamseldin, H., Tala, S. Al, Varaghchi, J. Rezazadeh, Najafi, Maryam, Deschner, S., Gläser, D., Hüttel, W., Kruer, M.C., Kamsteeg, E.J., Takiyama, Y., Züchner, S., Baets, J., Synofzik, M., Schüle, R., Horvath, R., Pierson, T.M., and Senderek, J.

Abstract

Item does not contain fulltext, Human 4-hydroxyphenylpyruvate dioxygenase-like (HPDL) is a putative iron-containing non-heme oxygenase of unknown specificity and biological significance. We report 25 families containing 34 individuals with neurological disease associated with biallelic HPDL variants. Phenotypes ranged from juvenile-onset pure hereditary spastic paraplegia to infantile-onset spasticity and global developmental delays, sometimes complicated by episodes of neurological and respiratory decompensation. Variants included bona fide pathogenic truncating changes, although most were missense substitutions. Functionality of variants could not be determined directly as the enzymatic specificity of HPDL is unknown; however, when HPDL missense substitutions were introduced into 4-hydroxyphenylpyruvate dioxygenase (HPPD, an HPDL orthologue), they impaired the ability of HPPD to convert 4-hydroxyphenylpyruvate into homogentisate. Moreover, three additional sets of experiments provided evidence for a role of HPDL in the nervous system and further supported its link to neurological disease: (i) HPDL was expressed in the nervous system and expression increased during neural differentiation; (ii) knockdown of zebrafish hpdl led to abnormal motor behaviour, replicating aspects of the human disease; and (iii) HPDL localized to mitochondria, consistent with mitochondrial disease that is often associated with neurological manifestations. Our findings suggest that biallelic HPDL variants cause a syndrome varying from juvenile-onset pure hereditary spastic paraplegia to infantile-onset spastic tetraplegia associated with global developmental delays.

Published
2021

7. SPG10 is a rare cause of spastic paraplegia in European families

Author

Schule, R., Kremer, B.P.H., Kassubek, J., Auer-Grumbach, M., Kostic, V., Klopstock, T., Klimpe, S., Otto, S., Boesch, S., van de Warrenburg, B.P., and Schols, L.

Subjects
Paralysis, Spastic -- Causes of, Paralysis, Spastic -- Demographic aspects, Paralysis, Spastic -- Genetic aspects, Gene mutations -- Research, Gene mutations -- Physiological aspects, Health, Psychology and mental health
Published
2008

9. Demyelinating Charcot–Marie–Tooth neuropathy associated with FBLN5 mutations

Author

Safka Brozkova, D., primary, Stojkovic, T., additional, Haberlová, J., additional, Mazanec, R., additional, Windhager, R., additional, Fernandes Rosenegger, P., additional, Hacker, S., additional, Züchner, S., additional, Kochański, A., additional, Leonard‐Louis, S., additional, Francou, B., additional, Latour, P., additional, Senderek, J., additional, Seeman, P., additional, and Auer‐Grumbach, M., additional

Published
2020
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10. Multi-system neurological disease is common in patients with OPA1 mutations

Author

Yu-Wai-Man, P., Griffiths, P.G., Gorman, G.S., Lourenco, C.M., Wright, A.F., Auer-Grumbach, M., Toscano, A., Musumeci, O., Valentino, M.L., Caporali, L., Lamperti, C., Tallaksen, C.M., Duffey, P., Miller, J., Whittaker, R.G., Baker, M.R., Jackson, M.J., Clarke, M.P., Dhillon, B., Czermin, B., Stewart, J.D., Hudson, G., Reynier, P., Bonneau, D., Marques, W., Jr, Lenaers, G., McFarland, R., Taylor, R.W., Turnbull, D.M., Votruba, M., Zeviani, M., Carelli, V., Bindoff, L.A., Horvath, R., Amati-Bonneau, P., and Chinnery, P.F.

Published
2010
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13. Inverted formin 2-related Charcot-Marie-Tooth disease: extension of the mutational spectrum and pathological findings in Schwann cells and axons

Author

Roos, A, Weis, J, Korinthenberg, R, Auer-Grumbach, M, and Senderek, J

Subjects
congenital, hereditary, and neonatal diseases and abnormalities, ddc: 610, urogenital system, macromolecular substances, 610 Medical sciences, Medicine, urologic and male genital diseases, female genital diseases and pregnancy complications
Abstract

Question: Mutations in the gene encoding inverted formin FH2 and WH2 domain containing protein (INF2), a Cdc42 effector involved in the regulation of actin dynamics, cause focal segmental glomerulosclerosis (FSGS) and intermediate Charcot-Marie-Tooth neuropathy combined with FSGS (FSGS-CMT). Here, we[for full text, please go to the a.m. URL], 60th Annual Meeting of the German Society for Neuropathology and Neuroanatomy (DGNN)

Published
2015
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19. Classification and diagnostic guidelines for Charcot-Marie-Tooth type 2 (CMT2-HMSN II) and distal hereditary motor neuropathy (distal HMN - spinal CMT)

Author

Jonghe, P. de, Timmermans, V., Visser, M. de, Brice, A., Broeckhoven, C. van, Auer-Grumbach, M., Berciano, J., Beuten, J., Braathen, G.J., Christodoulou, K., Chanchetti, C., Dubourg-LeGuern, O., Engelen, B.G.M. van, Ericson, U., and Gabreëls-Festen, A.A.W.M.

Subjects
Hereditary motor and sensory neuropathies, Hereditaire motore en sensore neuropathieën
Abstract

Item does not contain fulltext

Published
1998

20. Exome sequencing identifies a REEP1 mutation involved in distal hereditary motor neuropathy type V

Author

Beetz, C., Pieber, T.R., Hertel, N., Schabhüttl, M., Fischer, C., Trajanoski, S., Graf, E., Keiner, S., Kurth, I., Wieland, T., Varga, R.-E., Timmerman, V., Reilly, M.M., Strom, T.M., and Auer-Grumbach, M.

Subjects
Male, Report, Mutation, Humans, Membrane Transport Proteins, Peripheral Nervous System Diseases, Exome, Female, Sequence Analysis, DNA, Cell Line, Pedigree
Abstract

The distal hereditary motor neuropathies (dHMNs) are a heterogeneous group of neurodegenerative disorders affecting the lower motoneuron. In a family with both autosomal-dominant dHMN and dHMN type V (dHMN/dHMN-V) present in three generations, we excluded mutations in all genes known to be associated with a dHMN phenotype through Sanger sequencing and defined three potential loci through linkage analysis. Whole-exome sequencing of two affected individuals revealed a single candidate variant within the linking regions, i.e., a splice-site alteration in REEP1 (c.304-2A>G). A minigene assay confirmed complete loss of splice-acceptor functionality and skipping of the in-frame exon 5. The resulting mRNA is predicted to be expressed at normal levels and to encode an internally shortened protein (p.102_139del). Loss-of-function REEP1 mutations have previously been identified in dominant hereditary spastic paraplegia (HSP), a disease associated with upper-motoneuron pathology. Consistent with our clinical-genetic data, we show that REEP1 is strongly expressed in the lower motoneurons as well. Upon exogeneous overexpression in cell lines we observe a subcellular localization defect for p.102_139del that differs from that observed for the known HSP-associated missense mutation c.59C>A (p.Ala20Glu). Moreover, we show that p.102_139del, but not p.Ala20Glu, recruits atlastin-1, i.e., one of the REEP1 binding partners, to the altered sites of localization. These data corroborate the loss-of-function nature of REEP1 mutations in HSP and suggest that a different mechanism applies in REEP1-associated dHMN.

Published
2012

22. Genetic spectrum of hereditary neuropathies with onset in the first year of life

Author

Baets, J. Deconinck, T. De Vriendt, E. Zimoń, M. Yperzeele, L. Van Hoorenbeeck, K. Peeters, K. Spiegel, R. Parman, Y. Ceulemans, B. Van Bogaert, P. Pou-Serradell, A. Bernert, G. Dinopoulos, A. Auer-Grumbach, M. Sallinen, S.-L. Fabrizi, G.M. Pauly, F. Van Den Bergh, P. Bilir, B. Battaloglu, E. Madrid, R.E. Kabzińska, D. Kochanski, A. Topaloglu, H. Miller, G. Jordanova, A. Timmerman, V. De Jonghe, P.

Abstract

Early onset hereditary motor and sensory neuropathies are rare disorders encompassing congenital hypomyelinating neuropathy with disease onset in the direct post-natal period and Dejerine-Sottas neuropathy starting in infancy. The clinical spectrum, however, reaches beyond the boundaries of these two historically defined disease entities. De novo dominant mutations in PMP22, MPZ and EGR2 are known to be a typical cause of very early onset hereditary neuropathies. In addition, mutations in several other dominant and recessive genes for Charcot-Marie-Tooth disease may lead to similar phenotypes. To estimate mutation frequencies and to gain detailed insights into the genetic and phenotypic heterogeneity of early onset hereditary neuropathies, we selected a heterogeneous cohort of 77 unrelated patients who presented with symptoms of peripheral neuropathy within the first year of life. The majority of these patients were isolated in their family. We performed systematic mutation screening by means of direct sequencing of the coding regions of 11 genes: MFN2, PMP22, MPZ, EGR2, GDAP1, NEFL, FGD4, MTMR2, PRX, SBF2 and SH3TC2. In addition, screening for the Charcot-Marie-Tooth type 1A duplication on chromosome 17p11.2-12 was performed. In 35 patients (45), mutations were identified. Mutations in MPZ, PMP22 and EGR2 were found most frequently in patients presenting with early hypotonia and breathing difficulties. The recessive genes FGD4, PRX, MTMR2, SBF2, SH3TC2 and GDAP1 were mutated in patients presenting with early foot deformities and variable delay in motor milestones after an uneventful neonatal period. Several patients displaying congenital foot deformities but an otherwise normal early development carried the Charcot-Marie-Tooth type 1A duplication. This study clearly illustrates the genetic heterogeneity underlying hereditary neuropathies with infantile onset. © 2011 The Author.

Published
2011

25. Extended phenotypic spectrum of KIF5A mutations: From spastic paraplegia to axonal neuropathy

Author

Liu, Y.-T., primary, Laura, M., additional, Hersheson, J., additional, Horga, A., additional, Jaunmuktane, Z., additional, Brandner, S., additional, Pittman, A., additional, Hughes, D., additional, Polke, J. M., additional, Sweeney, M. G., additional, Proukakis, C., additional, Janssen, J. C., additional, Auer-Grumbach, M., additional, Zuchner, S., additional, Shields, K. G., additional, Reilly, M. M., additional, and Houlden, H., additional

Published
2014
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28. Alterations in the ankyrin domain of TRPV4 cause congenital distal SMA, scapuloperoneal SMA and HMSN2C.

Author

Auer-Grumbach, M., Olschewski, A., Papic, L., Kremer, J.M.J., McEntagart, M.E., Uhrig, S., Fischer, C., Frohlich, E., Balint, Z., Tang, B., Strohmaier, H., Lochmuller, H., Schlotter-Weigel, B., Senderek, J., Krebs, A., Dick, K.J., Petty, R., Longman, C., Anderson, N.E., Padberg, G.W.A.M., Schelhaas, H.J., Ravenswaaij-Arts, C.M.A. van, Pieber, T.R., Crosby, A.H., Guelly, C., Auer-Grumbach, M., Olschewski, A., Papic, L., Kremer, J.M.J., McEntagart, M.E., Uhrig, S., Fischer, C., Frohlich, E., Balint, Z., Tang, B., Strohmaier, H., Lochmuller, H., Schlotter-Weigel, B., Senderek, J., Krebs, A., Dick, K.J., Petty, R., Longman, C., Anderson, N.E., Padberg, G.W.A.M., Schelhaas, H.J., Ravenswaaij-Arts, C.M.A. van, Pieber, T.R., Crosby, A.H., and Guelly, C.

Abstract

1 februari 2010, Contains fulltext : 88054_2.pdf (publisher's version ) (Closed access) Contains fulltext : 88054.pdf (author's version ) (Open Access), Spinal muscular atrophies (SMA, also known as hereditary motor neuropathies) and hereditary motor and sensory neuropathies (HMSN) are clinically and genetically heterogeneous disorders of the peripheral nervous system. Here we report that mutations in the TRPV4 gene cause congenital distal SMA, scapuloperoneal SMA, HMSN 2C. We identified three missense substitutions (R269H, R315W and R316C) affecting the intracellular N-terminal ankyrin domain of the TRPV4 ion channel in five families. Expression of mutant TRPV4 constructs in cells from the HeLa line revealed diminished surface localization of mutant proteins. In addition, TRPV4-regulated Ca(2+) influx was substantially reduced even after stimulation with 4alphaPDD, a TRPV4 channel-specific agonist, and with hypo-osmotic solution. In summary, we describe a new hereditary channelopathy caused by mutations in TRPV4 and present evidence that the resulting substitutions in the N-terminal ankyrin domain affect channel maturation, leading to reduced surface expression of functional TRPV4 channels.

Published
2010

29. Dominant mutations in the cation channel gene transient receptor potential vanilloid 4 cause an unusual spectrum of neuropathies

Author

Zimoń, M, Baets, J, Auer-Grumbach, M, et al, Boltshauser, E, Zimoń, M, Baets, J, Auer-Grumbach, M, et al, and Boltshauser, E

Abstract

Hereditary neuropathies form a heterogeneous group of disorders for which over 40 causal genes have been identified to date. Recently, dominant mutations in the transient receptor potential vanilloid 4 gene were found to be associated with three distinct neuromuscular phenotypes: hereditary motor and sensory neuropathy 2C, scapuloperoneal spinal muscular atrophy and congenital distal spinal muscular atrophy. Transient receptor potential vanilloid 4 encodes a cation channel previously implicated in several types of dominantly inherited bone dysplasia syndromes. We performed DNA sequencing of the coding regions of transient receptor potential vanilloid 4 in a cohort of 145 patients with various types of hereditary neuropathy and identified five different heterozygous missense mutations in eight unrelated families. One mutation arose de novo in an isolated patient, and the remainder segregated in families. Two of the mutations were recurrent in unrelated families. Four mutations in transient receptor potential vanilloid 4 targeted conserved arginine residues in the ankyrin repeat domain, which is believed to be important in protein-protein interactions. Striking phenotypic variability between and within families was observed. The majority of patients displayed a predominantly, or pure, motor neuropathy with axonal characteristics observed on electrophysiological testing. The age of onset varied widely, ranging from congenital to late adulthood onset. Various combinations of additional features were present in most patients including vocal fold paralysis, scapular weakness, contractures and hearing loss. We identified six asymptomatic mutation carriers, indicating reduced penetrance of the transient receptor potential vanilloid 4 defects. This finding is relatively unusual in the context of hereditary neuropathies and has important implications for diagnostic testing and genetic counselling.

Published
2010

32. O.10 Mutations in a new dynein/dynactin adaptor gene cause Dominant Congenital Spinal Muscular Atrophy (DCSMA) and Hereditary Spastic Paraplegia (HSP)

Author

Oates, E.C., primary, Rosser, A.M., additional, Hafezparast, M., additional, Lek, M., additional, Scoto, M., additional, Greensmith, L., additional, Auer-Grumbach, M., additional, Schule, R., additional, Herrmann, D.N., additional, Clarke, N.F., additional, MacArthur, D.G., additional, Züchner, S., additional, Muntoni, F., additional, Reilly, M.M., additional, and North, K.N., additional

Published
2013
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33. The phenotype of motor neuropathies associated with BSCL2 mutations is broader than Silver syndrome and distal HMN type V

Author

UCL - Cliniques universitaires Saint-Luc, UCL - MD/NOPS - Département de neurologie et de psychiatrie, UCL - (SLuc) Service de neurologie, Irobi, J, Van den Bergh, Peter, Merlini, L, Dumoulin, Christine, Van Maldergem, L., Dierick, I, Verpoorten, N, Jordanova, A., Windpassinger, C, De Vriendt, E, Van Gerwen, V, Auer-Grumbach, M, Wagner, K., Timmerman, V, De Jonghe, P., UCL - Cliniques universitaires Saint-Luc, UCL - MD/NOPS - Département de neurologie et de psychiatrie, UCL - (SLuc) Service de neurologie, Irobi, J, Van den Bergh, Peter, Merlini, L, Dumoulin, Christine, Van Maldergem, L., Dierick, I, Verpoorten, N, Jordanova, A., Windpassinger, C, De Vriendt, E, Van Gerwen, V, Auer-Grumbach, M, Wagner, K., Timmerman, V, and De Jonghe, P.

Abstract

Silver syndrome is a rare autosomal dominant neurodegenerative disorder characterized by marked amyotrophy and weakness of small hand muscles and spasticity in the lower limbs. The locus for Silver syndrome (SPG17) was assigned to a 13 cM region on chromosome 11q12-q14 in a single large pedigree. We recently found heterozygous mutations in the Berardinelli-Seip congenital lipodystrophy (BSCL2, seipin) gene causing SPG17 and distal hereditary motor neuropathy type V (distal HMN V). Here we report the clinical features of two families with heterozygous BSCL2 mutations. Interestingly, both families show a clinical phenotype different from classical Silver syndrome, and in some patients the phenotype is also different from distal HMN V. Patients in the first family had marked spasticity in the lower limbs and very striking distal amyotrophy that always started in the legs. Patients in the second family had distal amyotrophy sometimes starting and predominating in the legs, but no pyramidal tract signs. These observations broaden the clinical phenotype of disorders associated with BSCL2 mutations, having consequences for molecular genetic testing.

Published
2004

34. Heterozygous missense mutations in BSCL2 are associated with distal hereditary motor neuropathy and Silver syndrome

Author

UCL - Cliniques universitaires Saint-Luc, UCL - MD/NOPS - Département de neurologie et de psychiatrie, UCL - (SLuc) Service de neurologie, Windpassinger, C, Van den Bergh, Peter, Auer-Grumbach, M, Irobi, J, Patel, H, Petek, E, Horl, G, Malli, R, Reed, JA, Dierick, I, Verpoorten, N, Warner, TT, Proukakis, C, Dumoulin, Christine, Van Maldergem, L., Merlini, L, De Jonghe, P., Timmerman, V, Crosby, AH, Wagner, K., UCL - Cliniques universitaires Saint-Luc, UCL - MD/NOPS - Département de neurologie et de psychiatrie, UCL - (SLuc) Service de neurologie, Windpassinger, C, Van den Bergh, Peter, Auer-Grumbach, M, Irobi, J, Patel, H, Petek, E, Horl, G, Malli, R, Reed, JA, Dierick, I, Verpoorten, N, Warner, TT, Proukakis, C, Dumoulin, Christine, Van Maldergem, L., Merlini, L, De Jonghe, P., Timmerman, V, Crosby, AH, and Wagner, K.

Abstract

Distal hereditary motor neuropathy (dHMN) or distal spinal muscular atrophy (OMIM #182960) is a heterogeneous group of disorders characterized by an almost exclusive degeneration of motor nerve fibers, predominantly in the distal part of the limbs(1). Silver syndrome (OMIM #270685) is a rare form of hereditary spastic paraparesis mapped to chromosome 11q12q14 (SPG17) in which spasticity of the legs is accompanied by amyotrophy of the hands and occasionally also the lower limbs(2,3). Silver syndrome and most forms of dHMN are autosomal dominantly inherited with incomplete penetrance and a broad variability in clinical expression. A genome-wide scan in an Austrian family with dHMN-V (ref. 4) showed linkage to the locus SPG17, which was confirmed in 16 additional families with a phenotype characteristic of dHMN or Silver syndrome. After refining the critical region to 1 Mb, we sequenced the gene Berardinelli-Seip congenital lipodystrophy (BSCL2) and identified two heterozygous missense mutations resulting in the amino acid substitutions N88S and S90L. Null mutations in BSCL2, which encodes the protein seipin, were previously shown to be associated with autosomal recessive Berardinelli-Seip congenital lipodystrophy 5 (OMIM #269700). We show that seipin is an integral membrane protein of the endoplasmic reticulum (ER). The amino acid substitutions N88S and S90L affect glycosylation of seipin and result in aggregate formation leading to neurodegeneration.

Published
2004

35. Genetic spectrum of hereditary neuropathies with onset in the first year of life

Author

Baets, J., primary, Deconinck, T., additional, De Vriendt, E., additional, Zimon, M., additional, Yperzeele, L., additional, Van Hoorenbeeck, K., additional, Peeters, K., additional, Spiegel, R., additional, Parman, Y., additional, Ceulemans, B., additional, Van Bogaert, P., additional, Pou-Serradell, A., additional, Bernert, G., additional, Dinopoulos, A., additional, Auer-Grumbach, M., additional, Sallinen, S.-L., additional, Fabrizi, G. M., additional, Pauly, F., additional, Van den Bergh, P., additional, Bilir, B., additional, Battaloglu, E., additional, Madrid, R. E., additional, Kabzinska, D., additional, Kochanski, A., additional, Topaloglu, H., additional, Miller, G., additional, Jordanova, A., additional, Timmerman, V., additional, and De Jonghe, P., additional

Published
2011
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36. Dominant GDAP1 mutations cause predominantly mild CMT phenotypes

Author

Zimoń, M., primary, Baets, J., additional, Fabrizi, G.M., additional, Jaakkola, E., additional, Kabzińska, D., additional, Pilch, J., additional, Schindler, A.B., additional, Cornblath, D.R., additional, Fischbeck, K.H., additional, Auer-Grumbach, M., additional, Guelly, C., additional, Huber, N., additional, De Vriendt, E., additional, Timmerman, V., additional, Suter, U., additional, Hausmanowa-Petrusewicz, I., additional, Niemann, A., additional, Kochański, A., additional, De Jonghe, P., additional, and Jordanova, A., additional

Published
2011
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37. SPG15 is the second most common cause of hereditary spastic paraplegia with thin corpus callosum

Author

Goizet, C., primary, Boukhris, A., additional, Maltete, D., additional, Guyant-Marechal, L., additional, Truchetto, J., additional, Mundwiller, E., additional, Hanein, S., additional, Jonveaux, P., additional, Roelens, F., additional, Loureiro, J., additional, Godet, E., additional, Forlani, S., additional, Melki, J., additional, Auer-Grumbach, M., additional, Fernandez, J. C., additional, Martin-Hardy, P., additional, Sibon, I., additional, Sole, G., additional, Orignac, I., additional, Mhiri, C., additional, Coutinho, P., additional, Durr, A., additional, Brice, A., additional, and Stevanin, G., additional

Published
2009
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38. Diagnosis of Polyneuropathies

Author

Heuß, D., primary, Auer-Grumbach, M., additional, Haupt, W., additional, Löscher, W., additional, Neundörfer, B., additional, Rautenstrauß, B., additional, Renaud, S., additional, and Sommer, C., additional

Published
2009
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39. High throughput genotyping: microarray-based resequencing for autosomal-dominant hereditary spastic paraplegia

Author

Schlipf, N, primary, Schüle, R, additional, Dufke, C, additional, Bonin, M, additional, Auer-Grumbach, M, additional, Stevanin, G, additional, Brice, A, additional, Beetz, C, additional, Kassubek, J, additional, Klebe, S, additional, Klimpe, S, additional, Klopstock, T, additional, Otto, S, additional, Poths, S, additional, Seibel, A, additional, Stolze, H, additional, Bauer, P, additional, and Schöls, L, additional

Published
2009
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40. Genes for hereditary sensory and autonomic neuropathies: a genotype-phenotype correlation

Author

Rotthier, A., primary, Baets, J., additional, Vriendt, E. D., additional, Jacobs, A., additional, Auer-Grumbach, M., additional, Levy, N., additional, Bonello-Palot, N., additional, Kilic, S. S., additional, Weis, J., additional, Nascimento, A., additional, Swinkels, M., additional, Kruyt, M. C., additional, Jordanova, A., additional, De Jonghe, P., additional, and Timmerman, V., additional

Published
2009
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41. Relative contribution of mutations in genes for autosomal dominant distal hereditary motor neuropathies: a genotype-phenotype correlation study

Author

Dierick, I., primary, Baets, J., additional, Irobi, J., additional, Jacobs, A., additional, De Vriendt, E., additional, Deconinck, T., additional, Merlini, L., additional, Van den Bergh, P., additional, Rasic, V. M., additional, Robberecht, W., additional, Fischer, D., additional, Morales, R. J., additional, Mitrovic, Z., additional, Seeman, P., additional, Mazanec, R., additional, Kochanski, A., additional, Jordanova, A., additional, Auer-Grumbach, M., additional, Helderman-van den Enden, A. T. J. M., additional, Wokke, J. H. J., additional, Nelis, E., additional, De Jonghe, P., additional, and Timmerman, V., additional

Published
2007
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