Your search keyword '"Herranz E"' showing total 31 results

1. The use of 7T MRI in multiple sclerosis: review and consensus statement from the North American Imaging in Multiple Sclerosis Cooperative.

Author

Harrison, Daniel M, Sati, Pascal, Klawiter, Eric C, Narayanan, Sridar, Bagnato, Francesca, Beck, Erin S, Barker, Peter, Calvi, Alberto, Cagol, Alessandro, Donadieu, Maxime, Duyn, Jeff, Granziera, Cristina, Henry, Roland G, Huang, Susie Y, Hoff, Michael N, Mainero, Caterina, Ontaneda, Daniel, Reich, Daniel S, Rudko, David A, and Smith, Seth A

Published

2024

2. Hypereosinophilia and acute lymphocytic leukemia.

Author

Rios-Herranz, E., Fores-Cachon, R., Diez-Martin, S. L., and Fernandez, M. N.

Published

1991

3. Early blood neurofilament light chain and myelin oligodendrocyte glycoprotein antibody levels associate with different disease courses of myelin oligodendrocyte glycoproteinassociated disease in children.

Author

Horellou, Philippe, Flet-Berliac, Lorraine, Leroy, Carole, Giorgi, Laetitia, Joly, Candie, Desjardins, Delphine, Chrétien, Pascale, Hacein-Bey-Abina, Salima, Le Grand, Roger, and Deiva, Kumaran

Published

2023

4. Linking lesions in sensorimotor cortex to contralateral hand function in multiple sclerosis: a 7 T MRI study.

Author

Madsen, Mads A J, Wiggermann, Vanessa, Marques, Marta F M, Lundell, Henrik, Cerri, Stefano, Puonti, Oula, Blinkenberg, Morten, Christensen, Jeppe Romme, Sellebjerg, Finn, Siebner, Hartwig R, and Romme Christensen, Jeppe

Abstract

Cortical lesions constitute a key manifestation of multiple sclerosis and contribute to clinical disability and cognitive impairment. Yet it is unknown whether local cortical lesions and cortical lesion subtypes contribute to domain-specific impairments attributable to the function of the lesioned cortex. In this cross-sectional study, we assessed how cortical lesions in the primary sensorimotor hand area relate to corticomotor physiology and sensorimotor function of the contralateral hand. Fifty relapse-free patients with relapsing-remitting or secondary-progressive multiple sclerosis and 28 healthy age- and sex-matched participants underwent whole-brain 7 T MRI to map cortical lesions. Brain scans were also used to estimate normalized brain volume, pericentral cortical thickness, white matter lesion fraction of the corticospinal tract, infratentorial lesion volume and the cross-sectional area of the upper cervical spinal cord. We tested sensorimotor hand function and calculated a motor and sensory composite score for each hand. In 37 patients and 20 healthy controls, we measured maximal motor-evoked potential amplitude, resting motor threshold and corticomotor conduction time with transcranial magnetic stimulation and the N20 latency from somatosensory-evoked potentials. Patients showed at least one cortical lesion in the primary sensorimotor hand area in 47 of 100 hemispheres. The presence of a lesion was associated with worse contralateral sensory (P = 0.014) and motor (P = 0.009) composite scores. Transcranial magnetic stimulation of a lesion-positive primary sensorimotor hand area revealed a decreased maximal motor-evoked potential amplitude (P < 0.001) and delayed corticomotor conduction (P = 0.002) relative to a lesion-negative primary sensorimotor hand area. Stepwise mixed linear regressions showed that the presence of a primary sensorimotor hand area lesion, higher white-matter lesion fraction of the corticospinal tract, reduced spinal cord cross-sectional area and higher infratentorial lesion volume were associated with reduced contralateral motor hand function. Cortical lesions in the primary sensorimotor hand area, spinal cord cross-sectional area and normalized brain volume were also associated with smaller maximal motor-evoked potential amplitude and longer corticomotor conduction times. The effect of cortical lesions on sensory function was no longer significant when controlling for MRI-based covariates. Lastly, we found that intracortical and subpial lesions had the largest effect on reduced motor hand function, intracortical lesions on reduced motor-evoked potential amplitude and leucocortical lesions on delayed corticomotor conduction. Together, this comprehensive multilevel assessment of sensorimotor brain damage shows that the presence of a cortical lesion in the primary sensorimotor hand area is associated with impaired corticomotor function of the hand, after accounting for damage at the subcortical level. The results also provide preliminary evidence that cortical lesion types may affect the various facets of corticomotor function differentially. [ABSTRACT FROM AUTHOR]

Published

2022

5. In vivo quantitative imaging of hippocampal inflammation in autoimmune neuroinflammatory conditions: a systematic review.

Author

Nwaubani, P, Cercignani, M, and Colasanti, A

Subjects

POSITRON emission tomography, SYSTEMIC lupus erythematosus, LIMBIC system, HIPPOCAMPUS (Brain), MAGNETIC resonance imaging, BRAIN diseases

Abstract

The hippocampus is a morphologically complex region of the brain limbic system centrally involved in important cognitive, affective, and behavioural regulatory roles. It has exquisite vulnerability to neuroinflammatory processes, with some of its subregions found to be specific sites of neuroinflammatory pathology in ex-vivo studies. Optimizing neuroimaging correlates of hippocampal neuroinflammation would enable the direct study of functional consequences of hippocampal neuroinflammatory pathology, as well as the definition of therapeutic end-points for treatments targeting neuroinflammation, and their related affective or cognitive sequelae. However, in vivo traditional imaging of the hippocampus and its subregions is fraught with difficulties, due to methodological challenges deriving from its unique anatomical characteristics. The main objective of this review is to provide a current update on the characterization of quantitative neuroimaging correlates of hippocampal neuroinflammation by focusing on three prototypical autoimmune neuro-inflammatory conditions [multiple sclerosis (MS), systemic lupus erythematosus (SLE), and autoimmune encephalitis (AE)]. We focused on studies employing TSPO-targeting positron emission tomography (PET), quantitative magnetic resonance imaging (MRI), and spectroscopy techniques assumed to be sensitive to neuroinflammatory tissue changes. We found 18 eligible studies (14, 2, and 2 studies in MS, AE, and SLE, respectively). Across conditions, the largest effect was seen in TSPO PET and diffusion-weighted MRI studies. No study examined neuroinflammation-related changes at the hippocampal subfield level. Overall, results were largely inconsistent due to heterogeneous imaging methods, small sample sizes, and different population studies. We discuss how these data could inform future study design and conclude by suggesting further methodological directions aimed at improving the precision and sensitivity of neuroimaging techniques to characterize hippocampal neuroinflammatory pathology in the human brain. The hippocampus is a complex brain region crucially involved in neuroinflammation. We systematically reviewed quantitative imaging studies focusing on hippocampal pathology in autoimmune neuroinflammatory conditions and identified unmet research needs and future methodological directions. [ABSTRACT FROM AUTHOR]

Published

2022

6. Identification and Quantification of Bu Shen Yi Sui Capsule by UPLC-LTQ-Orbitrap-MSn and UPLC-QTOF-MS/MS.

Author

Liu, Haolong, Zhao, Yiyi, Zheng, Qi, Yang, Tao, Zhao, Hui, Zou, Haiyan, Fan, Yongping, Guo, Hongzhu, and Wang, Lei

Subjects

QUADRUPOLE ion trap mass spectrometry, TIME-of-flight mass spectrometry, HIGH performance liquid chromatography, CHINESE medicine, INDUSTRIAL safety, MASS spectrometers

Abstract

Traditional Chinese medicines (TCMs) have been considered as important alternative therapeutics because of their significant medicinal benefits in specific diseases. Chinese herb formula is characterized by a vast molecule that differs in routine medicines. Due to TCMs chemical complexity, proper quality control has been a great challenge. Choosing the appropriate method to identify and qualify these compounds is an important work to ensure its safety, efficacy and quality control. Thus, this study aimed at providing novel information on high-resolution LTQ-Orbitrap mass spectrometer (UPLC-LTQ-Orbitrap-MSn) based identification of Bu Shen Yi Sui capsule (BSYSC), which is used in treating multiple sclerosis as a kind of TCMs. Under the proposed chromatographic conditions, 80 chemical components classified as anthraquinone, phenolic acid and phenylethanoid glycosides were separated and identified from BSYSC. Coupled with the high-performance liquid chromatography quadrupole time-of-flight mass spectrometry (UPLC-QTOF-MS/MS) method, eight of them were regarded as marker compounds for the quantitative evaluation of BSYSC. The identification and quantification with precision of UPLC-LTQ-Orbitrap-MSn and UPLC-QTOF-MS/MS could facilitate essential data for further pharmacokinetic studies of BSYSC. [ABSTRACT FROM AUTHOR]

Published

2022

7. Multifaceted involvement of microglia in gray matter pathology in multiple sclerosis.

Author

Tsouki, Foteini and Williams, Anna

Subjects

MICROGLIA, GRAY matter (Nerve tissue), MULTIPLE sclerosis, CENTRAL nervous system, NEURODEGENERATION

Abstract

In the inflammatory demyelinating neurodegenerative disease multiple sclerosis (MS), there is increasing interest in gray matter pathology, as neuronal loss and cortical atrophy correlate with disability and disease progression, and MS therapeutics fail to significantly slow or stop neurodegeneration. Microglia, the central nervous system (CNS)‐resident macrophages, are extensively involved in white matter MS pathology, but are also implicated in gray matter pathology, similar to other neurodegenerative diseases, for which there is synaptic, axonal, and neuronal degeneration. Microglia display regional heterogeneity within the CNS, which reflects their highly plastic nature and their ability to deliver context‐dependent responses tailored to the demands of their microenvironment. Therefore, microglial roles in the MS gray matter in part reflect and in part diverge from those in the white matter. The present review summarizes current knowledge of microglial involvement in gray matter changes in MS, in demyelination, synaptic damage, and neurodegeneration, with evidence implicating microglia in pathology, neuroprotection, and repair. As our understanding of microglial physiology and pathophysiology increases, we describe how we are moving toward potential therapeutic applications in MS, harnessing microglia to protect and regenerate the CNS. [ABSTRACT FROM AUTHOR]

Published

2021

8. Cortical and phase rim lesions on 7 T MRI as markers of multiple sclerosis disease progression.

Author

Treaba, Constantina A., Conti, Allegra, Klawiter, Eric C., Barletta, Valeria T., Herranz, Elena, Mehndiratta, Ambica, Russo, Andrew W., Sloane, Jacob A., Kinkel, Revere P., Toschi, Nicola, and Mainero, Caterina

Published

2021

9. Effects of Trigger Point Dry Needling for Nontraumatic Shoulder Pain of Musculoskeletal Origin: A Systematic Review and Meta-Analysis.

Author

Navarro-Santana, Marcos J, Gómez-Chiguano, Guido F, Cleland, Joshua A, Arias-Buría, Jose L, Fernández-de-las-Peñas, César, and Plaza-Manzano, Gustavo

Subjects

SHOULDER pain treatment, CINAHL database, ONLINE information services, META-analysis, CONFIDENCE intervals, MEDICAL information storage & retrieval systems, INFORMATION storage & retrieval systems, MEDICAL databases, SYSTEMATIC reviews, PHYSICAL therapy, MUSCULOSKELETAL system, MYOFASCIAL pain syndromes, TREATMENT effectiveness, DESCRIPTIVE statistics, MEDLINE, MYOFASCIAL pain syndrome treatment, AMED (Information retrieval system)

Abstract

Objective The purpose of this study was to evaluate the effects of trigger point (TrP) dry needling alone or as an adjunct to other interventions on pain intensity and related disability in nontraumatic shoulder pain. Methods Ten databases were searched from inception to January 2020 for randomized clinical trials in which at least 1 group received TrP dry needling for shoulder pain of musculoskeletal origin with outcomes collected on pain intensity and related disability. Data extraction including participant and therapist details, interventions, blinding strategy, blinding assessment outcomes, and results were extracted by 2 reviewers. The risk of bias (Cochrane Risk of Bias, Cochrane Guidelines), methodological quality (Physiotherapy Evidence Database score), and evidence level (Grading of Recommendations Assessment, Development, and Evaluation approach) were assessed. The search identified 551 publications with 6 trials eligible for inclusion. Results There was moderate-quality evidence that TrP dry needling reduces shoulder pain intensity with a small effect (mean difference = −0.49 points, 95% CI = −0.84 to −0.13; standardized mean difference = −0.25, 95% CI = −0.42 to −0.09) and low-quality evidence that TrP dry needling improves related disability with a large effect (mean difference = −9.99 points, 95% CI −15.97 to −4.01; standardized mean difference = −1.14, 95% CI −1.81 to −0.47) compared with a comparison group. The effects on pain were only found at short term. The Cochrane Risk of Bias was generally low, but the heterogenicity of the results downgraded the evidence level. Conclusion Moderate- to low-quality evidence suggests positive effects of TrP dry needling for pain intensity (small effect) and pain-related disability (large effect) in nontraumatic shoulder pain of musculoskeletal origin, mostly at short term. Future clinical trials investigating long-term effects are needed. Impact Dry needling is commonly used for the management of musculoskeletal pain. This is the first meta-analysis to examine the effects of dry needling on nontraumatic shoulder pain. [ABSTRACT FROM AUTHOR]

Published

2021

10. In vivo gradients of thalamic damage in paediatric multiple sclerosis: a window into pathology.

Author

Meo, Ermelinda De, Storelli, Loredana, Moiola, Lucia, Ghezzi, Angelo, Veggiotti, Pierangelo, Filippi, Massimo, Rocca, Maria A, and De Meo, Ermelinda

Subjects

MULTIPLE sclerosis, WHITE matter (Nerve tissue), NEURODEGENERATION, MAGNETIC resonance, PATHOLOGY

Abstract

The thalamus represents one of the first structures affected by neurodegenerative processes in multiple sclerosis. A greater thalamic volume reduction over time, on its CSF side, has been described in paediatric multiple sclerosis patients. However, its determinants and the underlying pathological changes, likely occurring before this phenomenon becomes measurable, have never been explored. Using a multiparametric magnetic resonance approach, we quantified, in vivo, the different processes that can involve the thalamus in terms of focal lesions, microstructural damage and atrophy in paediatric multiple sclerosis patients and their distribution according to the distance from CSF/thalamus interface and thalamus/white matter interface. In 70 paediatric multiple sclerosis patients and 26 age- and sex-matched healthy controls, we tested for differences in thalamic volume and quantitative MRI metrics-including fractional anisotropy, mean diffusivity and T1/T2-weighted ratio-in the whole thalamus and in thalamic white matter, globally and within concentric bands originating from CSF/thalamus interface. In paediatric multiple sclerosis patients, the relationship of thalamic abnormalities with cortical thickness and white matter lesions was also investigated. Compared to healthy controls, patients had significantly increased fractional anisotropy in whole thalamus (f2 = 0.145; P = 0.03), reduced fractional anisotropy (f2 = 0.219; P = 0.006) and increased mean diffusivity (f2 = 0.178; P = 0.009) in thalamic white matter and a trend towards a reduced thalamic volume (f2 = 0.027; P = 0.058). By segmenting the whole thalamus and thalamic white matter into concentric bands, in paediatric multiple sclerosis we detected significant fractional anisotropy abnormalities in bands nearest to CSF (f2 = 0.208; P = 0.002) and in those closest to white matter (f2 range = 0.183-0.369; P range = 0.010-0.046), while we found significant mean diffusivity (f2 range = 0.101-0.369; P range = 0.018-0.042) and T1/T2-weighted ratio (f2 = 0.773; P = 0.001) abnormalities in thalamic bands closest to CSF. The increase in fractional anisotropy and decrease in mean diffusivity detected at the CSF/thalamus interface correlated with cortical thickness reduction (r range = -0.27-0.34; P range = 0.004-0.028), whereas the increase in fractional anisotropy detected at the thalamus/white matter interface correlated with white matter lesion volumes (r range = 0.24-0.27; P range = 0.006-0.050). Globally, our results support the hypothesis of heterogeneous pathological processes, including retrograde degeneration from white matter lesions and CSF-mediated damage, leading to thalamic microstructural abnormalities, likely preceding macroscopic tissue loss. Assessing thalamic microstructural changes using a multiparametric magnetic resonance approach may represent a target to monitor the efficacy of neuroprotective strategies early in the disease course. [ABSTRACT FROM AUTHOR]

Published

2021

11. 7 T imaging reveals a gradient in spinal cord lesion distribution in multiple sclerosis.

Author

Ouellette, Russell, Treaba, Constantina A, Granberg, Tobias, Herranz, Elena, Barletta, Valeria, Mehndiratta, Ambica, Leener, Benjamin De, Tauhid, Shahamat, Yousuf, Fawad, Dupont, Sarah M, Klawiter, Eric C, Sloane, Jacob A, Bakshi, Rohit, Cohen-Adad, Julien, Mainero, Caterina, and De Leener, Benjamin

Subjects

SPINAL cord, MULTIPLE sclerosis, CERVICAL cord, BRAIN diseases, DISABILITIES, RESEARCH, RESEARCH methodology, MAGNETIC resonance imaging, EVALUATION research, MEDICAL cooperation, COMPARATIVE studies, RESEARCH funding

Abstract

We used 7 T MRI to: (i) characterize the grey and white matter pathology in the cervical spinal cord of patients with early relapsing-remitting and secondary progressive multiple sclerosis; (ii) assess the spinal cord lesion spatial distribution and the hypothesis of an outside-in pathological process possibly driven by CSF-mediated immune cytotoxic factors; and (iii) evaluate the association of spinal cord pathology with brain burden and its contribution to neurological disability. We prospectively recruited 20 relapsing-remitting, 15 secondary progressive multiple sclerosis participants and 11 age-matched healthy control subjects to undergo 7 T imaging of the cervical spinal cord and brain as well as conventional 3 T brain acquisition. Cervical spinal cord imaging at 7 T was used to segment grey and white matter, including lesions therein. Brain imaging at 7 T was used to segment cortical and white matter lesions and 3 T imaging for cortical thickness estimation. Cervical spinal cord lesions were mapped voxel-wise as a function of distance from the inner central canal CSF pool to the outer subpial surface. Similarly, brain white matter lesions were mapped voxel-wise as a function of distance from the ventricular system. Subjects with relapsing-remitting multiple sclerosis showed a greater predominance of spinal cord lesions nearer the outer subpial surface compared to secondary progressive cases. Inversely, secondary progressive participants presented with more centrally located lesions. Within the brain, there was a strong gradient of lesion formation nearest the ventricular system that was most evident in participants with secondary progressive multiple sclerosis. Lesion fractions within the spinal cord grey and white matter were related to the lesion fraction in cerebral white matter. Cortical thinning was the primary determinant of the Expanded Disability Status Scale, white matter lesion fractions in the spinal cord and brain of the 9-Hole Peg Test and cortical thickness and spinal cord grey matter cross-sectional area of the Timed 25-Foot Walk. Spinal cord lesions were localized nearest the subpial surfaces for those with relapsing-remitting and the central canal CSF surface in progressive disease, possibly implying CSF-mediated pathogenic mechanisms in lesion development that may differ between multiple sclerosis subtypes. These findings show that spinal cord lesions involve both grey and white matter from the early multiple sclerosis stages and occur mostly independent from brain pathology. Despite the prevalence of cervical spinal cord lesions and atrophy, brain pathology seems more strongly related to physical disability as measured by the Expanded Disability Status Scale. [ABSTRACT FROM AUTHOR]

Published

2020

12. Cortical Microstructural Alterations in Mild Cognitive Impairment and Alzheimer's Disease Dementia.

Author

Vogt, Nicholas M, Hunt, Jack F, Adluru, Nagesh, Dean, Douglas C, Johnson, Sterling C, Asthana, Sanjay, Yu, John-Paul J, Alexander, Andrew L, and Bendlin, Barbara B

Published

2020

13. A quantitative neuropathological assessment of translocator protein expression in multiple sclerosis.

Author

Nutma, Erik, Stephenson, Jodie A, Gorter, Rianne P, Bruin, Joy de, Boucherie, Deirdre M, Donat, Cornelius K, Breur, Marjolein, van der Valk, Paul, Matthews, Paul M, Owen, David R, Amor, Sandra, and de Bruin, Joy

Subjects

MULTIPLE sclerosis, PROTEIN expression, MYELITIS, TRANSLOCATOR proteins, LIGAND binding (Biochemistry), ASTROCYTES

Abstract

The 18 kDa translocator protein (TSPO) is increasingly used to study brain and spinal cord inflammation in degenerative diseases of the CNS such as multiple sclerosis. The enhanced TSPO PET signal that arises during disease is widely considered to reflect activated pathogenic microglia, although quantitative neuropathological data to support this interpretation have not been available. With the increasing interest in the role of chronic microglial activation in multiple sclerosis, characterising the cellular neuropathology associated with TSPO expression is of clear importance for understanding the cellular and pathological processes on which TSPO PET imaging is reporting. Here we have studied the cellular expression of TSPO and specific binding of two TSPO targeting radioligands (3H-PK11195 and 3H-PBR28) in tissue sections from 42 multiple sclerosis cases and 12 age-matched controls. Markers of homeostatic and reactive microglia, astrocytes, and lymphocytes were used to investigate the phenotypes of cells expressing TSPO. There was an approximate 20-fold increase in cells double positive for TSPO and HLA-DR in active lesions and in the rim of chronic active lesion, relative to normal appearing white matter. TSPO was uniformly expressed across myeloid cells irrespective of their phenotype, rather than being preferentially associated with pro-inflammatory microglia or macrophages. TSPO+ astrocytes were increased up to 7-fold compared to normal-appearing white matter across all lesion subtypes and accounted for 25% of the TSPO+ cells in these lesions. To relate TSPO protein expression to ligand binding, specific binding of the TSPO ligands 3H-PK11195 and 3H-PBR28 was determined in the same lesions. TSPO radioligand binding was increased up to seven times for 3H-PBR28 and up to two times for 3H-PK11195 in active lesions and the centre of chronic active lesions and a strong correlation was found between the radioligand binding signal for both tracers and the number of TSPO+ cells across all of the tissues examined. In summary, in multiple sclerosis, TSPO expression arises from microglia of different phenotypes, rather than being restricted to microglia which express classical pro-inflammatory markers. While the majority of cells expressing TSPO in active lesions or chronic active rims are microglia/macrophages, our findings also emphasize the significant contribution of activated astrocytes, as well as smaller contributions from endothelial cells. These observations establish a quantitative framework for interpretation of TSPO in multiple sclerosis and highlight the need for neuropathological characterization of TSPO expression for the interpretation of TSPO PET in other neurodegenerative disorders. [ABSTRACT FROM AUTHOR]

Published

2019

14. Axonal degeneration as substrate of fractional anisotropy abnormalities in multiple sclerosis cortex.

Author

Preziosa, Paolo, Kiljan, Svenja, Steenwijk, Martijn D, Meani, Alessandro, Berg, Wilma D J van de, Schenk, Geert J, Rocca, Maria A, Filippi, Massimo, Geurts, Jeroen J G, Jonkman, Laura E, and van de Berg, Wilma D J

Subjects

MULTIPLE sclerosis, NEUROGLIA, BRAIN anatomy, DIFFUSION magnetic resonance imaging, HUMAN abnormalities, SOCIAL degeneration

Abstract

Cortical microstructural abnormalities are associated with clinical and cognitive deterioration in multiple sclerosis. Using diffusion tensor MRI, a higher fractional anisotropy has been found in cortical lesions versus normal-appearing cortex in multiple sclerosis. The pathological substrates of this finding have yet to be definitively elucidated. By performing a combined post-mortem diffusion tensor MRI and histopathology study, we aimed to define the histopathological substrates of diffusivity abnormalities in multiple sclerosis cortex. Sixteen subjects with multiple sclerosis and 10 age- and sex-matched non-neurological control donors underwent post-mortem in situ at 3 T MRI, followed by brain dissection. One hundred and ten paraffin-embedded tissue blocks (54 from multiple sclerosis patients, 56 from non-neurological controls) were matched to the diffusion tensor sequence to obtain regional diffusivity measures. Using immunohistochemistry and silver staining, cortical density of myelin, microglia, astrocytes and axons, and density and volume of neurons and glial cells were evaluated. Correlates of diffusivity abnormalities with histological markers were assessed through linear mixed-effects models. Cortical lesions (77% subpial) were found in 27/54 (50%) multiple sclerosis cortical regions. Multiple sclerosis normal-appearing cortex had a significantly lower fractional anisotropy compared to cortex from non-neurological controls (P = 0.047), whereas fractional anisotropy in demyelinated cortex was significantly higher than in multiple sclerosis normal-appearing cortex (P = 0.012) but not different from non-neurological control cortex (P = 0.420). Compared to non-neurological control cortex, both multiple sclerosis normal-appearing and demyelinated cortices showed a lower density of axons perpendicular to the cortical surface (P = 0.012 for both) and of total axons (parallel and perpendicular to cortical surface) (P = 0.028 and 0.012). In multiple sclerosis, demyelinated cortex had a lower density of myelin (P = 0.004), parallel (P = 0.018) and total axons (P = 0.029) versus normal-appearing cortex. Regarding the pathological substrate, in non-neurological controls, cortical fractional anisotropy was positively associated with density of perpendicular, parallel, and total axons (P = 0.031 for all). In multiple sclerosis, normal-appearing cortex fractional anisotropy was positively associated with perpendicular and total axon density (P = 0.031 for both), while associations with myelin, glial and total cells and parallel axons did not survive multiple comparison correction. Demyelinated cortex fractional anisotropy was positively associated with density of neurons, and total cells and negatively with microglia density, without surviving multiple comparison correction. Our results suggest that a reduction of perpendicular axons in normal-appearing cortex and of both perpendicular and parallel axons in demyelinated cortex may underlie the substrate influencing cortical microstructural coherence and being responsible for the different patterns of fractional anisotropy changes occurring in multiple sclerosis cortex. [ABSTRACT FROM AUTHOR]

Published

2019

15. Predisposition of six well-characterized microRNAs to syndesmophytes among Chinese patients with ankylosing spondylitis.

Author

Wenxue Yang, Xiaoping Yan, Qisheng Xia, Qingwen Tao, Xiaowei Gan, Yingze Zhang, Zhihua Chen, and Weiping Kong

Subjects

ANKYLOSING spondylitis, MICRORNA, GENE expression, C-reactive protein, HLA histocompatibility antigens

Abstract

Objectives: We quantified the expression of six well-characterized microRNAs (miRNAs) in peripheral blood mononuclear cells to see whether they can predispose to syndesmophytes in ankylosing spondylitis (AS) patients. Methods: This is a cross-sectional study involving 46 AS patients (23/23 with/without syndesmophytes) and 22 healthy controls. miRNAs expression was quantified by real-time PCR. Results: Six examined miRNAs were comparably expressed between AS patients without syndesmophytes and healthy controls (p>.05). Relative to AS patients without syndesmophytes, patients with syndesmophytes had significantly higher levels of miR-29a, miR-335-5p, miR-27a and let-7i (p=.001, .002, .013 and .029, respectively). Nine significant contributors associated with syndesmophytes in AS, including smoking, AS duration, human leukocyte antigen B27, erythrocyte sedimentation rate, C-reactive protein, miR-335-5p, miR-27a, miR-218 and sacroiliitis, were identified. The addition of miR-335-5p, miR-27a and miR-218 can significantly improve the accuracy of baseline risk factors. Based on the nine significant contributors, a nomogram was constructed, with good prediction accuracy (C-index: 0.86, p<.001). Conclusion: We provide evidence for the predisposition of miR-335-5p, miR-27a and miR-218 to syndesmophytes in AS patients, indicating a contributory role of miRNAs in the pathogenesis of syndesmophytes. Further validation is warranted. [ABSTRACT FROM AUTHOR]

Published

2019

16. Neuroinflammation and its relationship to changes in brain volume and white matter lesions in multiple sclerosis.

Author

Datta, Gourab, Colasanti, Alessandro, Rabiner, Eugenii A., Gunn, Roger N., Malik, Omar, Ciccarelli, Olga, Nicholas, Richard, Van Vlierberghe, Eline, Van Hecke, Wim, Searle, Graham, Santos-Ribeiro, Andre, and Matthews, Paul M.

Subjects

ENCEPHALITIS, MULTIPLE sclerosis, WHITE matter (Nerve tissue), MAGNETIC resonance imaging of the brain, CEREBRAL atrophy, ACETIC acid, ANTHROPOMETRY, BRAIN, CELL receptors, CELLS, DIGITAL image processing, INFLAMMATION, MAGNETIC resonance imaging, PYRIDINE, RADIOISOTOPES, POSITRON emission tomography, ATROPHY

Abstract

Brain magnetic resonance imaging is an important tool in the diagnosis and monitoring of multiple sclerosis patients. However, magnetic resonance imaging alone provides limited information for predicting an individual patient's disability progression. In part, this is because magnetic resonance imaging lacks sensitivity and specificity for detecting chronic diffuse and multi-focal inflammation mediated by activated microglia/macrophages. The aim of this study was to test for an association between 18 kDa translocator protein brain positron emission tomography signal, which arises largely from microglial activation, and measures of subsequent disease progression in multiple sclerosis patients. Twenty-one patients with multiple sclerosis (seven with secondary progressive disease and 14 with a relapsing remitting disease course) underwent T1- and T2-weighted and magnetization transfer magnetic resonance imaging at baseline and after 1 year. Positron emission tomography scanning with the translocator protein radioligand 11C-PBR28 was performed at baseline. Brain tissue and lesion volumes were segmented from the T1- and T2-weighted magnetic resonance imaging and relative 11C-PBR28 uptake in the normal-appearing white matter was estimated as a distribution volume ratio with respect to a caudate pseudo-reference region. Normal-appearing white matter distribution volume ratio at baseline was correlated with enlarging T2-hyperintense lesion volumes over the subsequent year (ρ = 0.59, P = 0.01). A post hoc analysis showed that this association reflected behaviour in the subgroup of relapsing remitting patients (ρ = 0.74, P = 0.008). By contrast, in the subgroup of secondary progressive patients, microglial activation at baseline was correlated with later progression of brain atrophy (ρ = 0.86, P = 0.04). A regression model including the baseline normal-appearing white matter distribution volume ratio, T2 lesion volume and normal-appearing white matter magnetization transfer ratio for all of the patients combined explained over 90% of the variance in enlarging lesion volume over the subsequent 1 year. Glial activation in white matter assessed by translocator protein PET significantly improves predictions of white matter lesion enlargement in relapsing remitting patients and is associated with greater brain atrophy in secondary progressive disease over a period of short term follow-up. [ABSTRACT FROM AUTHOR]

Published

2017

17. Synaptophysin Is a Reliable Marker for Axonal Damage.

Author

Gudi, Viktoria, Gai, Lijie, Herder, Vanessa, Tejedor, Laura Salinas, Kipp, Markus, Amor, Sandra, Suhs, Kurt-Wolfram, Hansmann, Florian, Beineke, Andreas, Baumgärtner, Wolfgang, Stangel, Martin, and Skripuletz, Thomas

Published

2017

18. Pivotal role of choline metabolites in remyelination.

Author

Skripuletz, Thomas, Manzel, Arndt, Gropengießer, Karoline, Schäfer, Nora, Gudi, Viktoria, Singh, Vikramjeet, Salinas Tejedor, Laura, Jörg, Stefanie, Hammer, Anna, Voss, Elke, Vulinovic, Franca, Degen, Diane, Wolf, Rebecca, Lee, De-Hyung, Pul, Refik, Moharregh-Khiabani, Darius, Baumgärtner, Wolfgang, Gold, Ralf, Linker, Ralf A., and Stangel, Martin

Subjects

CHOLINE, MYELINATION, CYTIDINE diphosphate choline, CENTRAL nervous system physiology, LABORATORY mice, MULTIPLE sclerosis diagnosis, CLINICAL trials, THERAPEUTICS

Abstract

Skripuletz et al. show that exogenous CDP-choline enhances CNS remyelination in two different mouse models of multiple sclerosis. The substance acts via the choline metabolic pathway and has the potential to enter clinical trials in the near future, having already shown a robust safety profile in more than 11 000 individuals.Neuroprotective approaches for central nervous system regeneration have not been successful in clinical practice so far and compounds that enhance remyelination are still not available for patients with multiple sclerosis. The objective of this study was to determine potential regenerative effects of the substance cytidine-5′-diphospho (CDP)-choline in two different murine animal models of multiple sclerosis. The effects of exogenously applied CDP-choline were tested in murine myelin oligodendrocyte glycoprotein-induced experimental autoimmune encephalomyelitis. In addition, the cuprizone-induced mouse model of de- and remyelination was used to specifically test the hypothesis that CDP-choline directly increases remyelination. We found that CDP-choline ameliorated the disease course of experimental autoimmune encephalomyelitis and exerted beneficial effects on myelin, oligodendrocytes and axons. After cuprizone-induced demyelination, CDP-choline effectively enhanced myelin regeneration and reversed motor coordination deficits. The increased remyelination arose from an increase in the numbers of proliferating oligodendrocyte precursor cells and oligodendrocytes. Further in vitro studies suggest that this process is regulated by protein kinase C. We thus identified a new mechanism to enhance central nervous system remyelination via the choline pathway. Due to its regenerative action combined with an excellent safety profile, CDP-choline could become a promising substance for patients with multiple sclerosis as an add-on therapy. [ABSTRACT FROM AUTHOR]

Published

2015

19. Therapeutic uses of anti-α4-integrin (anti-VLA-4) antibodies in multiple sclerosis

Author

Schwab, Nicholas, Schneider-Hohendorf, Tilman, and Wiendl, Heinz

Abstract

Multiple sclerosis (MS) is a disorder of putative autoimmune origin, where immune cells invade the central nervous system and cause damage by attacking the myelin sheath of nerve cells. The blockade of the integrin very late antigen-4 (VLA-4) with the monoclonal antibody natalizumab has become the most effective therapy against MS since its approval in 2004. It is assumed that the inhibition of VLA-4-mediated immune cell adhesion to the endothelium of the blood–brain barrier (BBB) alleviates pathogenic processes of MS and, therefore, reduces disease severity and burden. Not all approaches to treat additional immune-mediated disorders (e.g. Rasmussen encephalitis and neuromyelitis optica) with natalizumab have been successful, but allowed researchers to gain additional insight into mechanisms of specific immune cell subsets’ migration through the BBB in the human system. While the long-term efficacy and general tolerability of natalizumab in MS are clear, the over 400 cases of natalizumab-associated progressive multifocal leukoencephalopathy (PML) have been of great concern and methods of risk stratification in patients have become a major area of research. Modern risk stratification includes established factors such as treatment duration, previous immune-suppressive therapy, and anti-John Cunningham virus (JCV) antibody seropositivity, but also experimental factors such as anti-JCV antibody titers and levels of L-selectin. Today, anti-VLA-4 therapy is reserved for patients with highly active relapsing-remitting MS and patients are monitored closely for early signs of potential PML. [ABSTRACT FROM AUTHOR]

Published

2015

20. Time Course and Spatial Profile of Nogo-A Expression in Experimental Autoimmune Encephalomyelitis in C57BL/6 Mice.

Author

Theotokis, Paschalis, Lourbopoulos, Athanasios, Touloumi, Olga, Lagoudaki, Roza, Kofidou, Evangelia, Nousiopoulou, Evangelia, Poulatsidou, Kyriaki-Nepheli, Kesidou, Evangelia, Tascos, Nikolaos, Spandou, Evangelia, and Grigoriadis, Nikolaos

Published

2012

21. Functional role of brain-derived neurotrophic factor in neuroprotective autoimmunity: therapeutic implications in a model of multiple sclerosis.

Author

Linker, Ralf A., Lee, De-Hyung, Demir, Seray, Wiese, Stefan, Kruse, Niels, Siglienti, Ines, Gerhardt, Ellen, Neumann, Harald, Sendtner, Michael, Lühder, Fred, and Gold, Ralf

Subjects

NERVE growth factor, NEUROPROTECTIVE agents, AUTOIMMUNITY, MULTIPLE sclerosis, AUTOIMMUNE diseases, ENCEPHALOMYELITIS, AXONS, LABORATORY mice

Abstract

Brain-derived neurotrophic factor plays a key role in neuronal and axonal survival. Brain-derived neurotrophic factor is expressed in the immune cells in lesions of experimental autoimmune encephalomyelitis and multiple sclerosis, thus potentially mediating neuroprotective effects. We investigated the functional role of brain-derived neurotrophic factor in myelin oligodendrocyte glycoprotein-induced experimental autoimmune encephalomyelitis, an animal model of multiple sclerosis. Mice deficient for brain-derived neurotrophic factor in immune cells displayed an attenuated immune response in the acute phase of experimental autoimmune encephalomyelitis, but progressive disability with enhanced axonal loss in the chronic phase of the disease. In mice deficient for central nervous system-derived brain-derived neurotrophic factor via glial fibrillary acidic protein-crescentin-mediated deletion, a more severe course of experimental autoimmune encephalomyelitis and an overall increased axonal loss was observed. In a lentiviral approach, injection of brain-derived neurotrophic factor-overexpressing T cells led to a less severe course of experimental autoimmune encephalomyelitis and direct axonal protection. Our data imply a functional role of brain-derived neurotrophic factor in autoimmune demyelination by mediating axon protection. [ABSTRACT FROM AUTHOR]

Published

2010

22. Meningeal Inflammation is not Associated With Cortical Demyelination in Chronic Multiple Sclerosis.

Author

Kooi, Evert-Jan, Geurts, Jeroen J.G., van Horssen, Jack, B⊘, Lars, and van der Valk, Paul

Published

2009

23. Effects of pre-commercial thinning on transpiration in young post-fire maritime pine stands.

Author

Jiménez, E., Vega, J.A., P. Pérez-Gorostiaga, Cuiñas, P., Fonturbel, T., Fernández, C., Madrigal, J., Hernando, C., and Guijarro, M.

Subjects

FOREST thinning, PLANT transpiration, PINE, SOIL moisture, FOREST management, FORESTS & forestry

Abstract

In the present study, the effect of heavy thinning on soil water content was investigated in relation to water use in an 8-year-old post-fire-regenerated maritime pine (Pinus pinaster Ait.) stand in northwestern Spain over two growing seasons. Three different treatment levels were selected: control (unthinned, 40 200 saplings ha-1), intense thinning (leaving 3850 saplings ha-1) and very intense thinning (leaving 1925 saplings ha-1); sap flow measurements were made on 10 saplings in each treatment throughout two growing seasons following thinning. Soil water availability in thinned plots was 1.8 times higher in the first growing season and 2.5 times higher in the second season, than in the control plots. Sap flow density in very intensely thinned plots was lower than in the control plots 3-S months after treatment. However, for the whole study period the mean sap flow density in saplings was higher in thinned plots than in unthinned plots (about double in the first growing season and 1.7 times higher in the second). Monthly transpiration at plot level was 8.8 and 4.4 times higher in control plots, than in very intensely and intensely thinned plots, respectively, in the first growing season, and 4.5 and 2.8 in the second season. Very intense thinning did not result in significant differences in saplings sap flow and transpiration at plot level, compared with intense thinning. Some consequences of these results for the management of such juvenile stands are discussed. [ABSTRACT FROM AUTHOR]

Published

2008

24. Millions of Life-Years Saved with Potent Antiretroviral Drugs in the United States: A Celebration, with Challenges.

Author

Vermund, Sten H.

Subjects

ANTIRETROVIRAL agents, HIV, AIDS prevention, AIDS, AZIDOTHYMIDINE

Abstract

The article focuses on the potent antiretroviral drugs in the United States. The drugs haved save many lives and will continue to save lives in many years to come. One of the uses of the drug is that it prevents the transfer of HIV virus from mothers to infants. The first antiretroviral drug to be approved is the zidovudine. There is a great importance in the detection of the HIV disease.

Published

2006

25. Multiple characterizations of Listeria monocytogenes sensitive and insensitive variants to divergicin M35, a new pediocin-like bacteriocin.

Author

Naghmouchi, K., Drider, D., Kheadr, E., Lacroix, C., Prévost, H., and Fliss, I.

Subjects

LISTERIA monocytogenes, LISTERIA, BACTERIOCINS, ANTIBIOTICS, ANTIBACTERIAL agents

Abstract

Aims: Divergicin M35 is a new class IIa bacteriocin produced by Carnobacterium divergicin M35. The bactericidal activity of this antimicrobial peptide was tested against a set of 11 strains of Listeria monocytogenes isolated from food. Methods and Results: The minimal inhibitory concentration (MIC) was determined by the microdilution method. The strains tested displayed a different level of sensitivity to divergicin M35. L. monocytogenes LSD530, referred to as DivS strain, was the most sensitive and appeared to be inhibited by concentration of divergicin M35 below 0·13 μg ml−1. The mutant resistant to divergicin M35, called DivM, was obtained from L. monocytogenes LSD530 (DivS) by gradually increasing the amounts of divergicin M35 until 1·3 μg ml−1. Notably, DivM was stable after 50 generations. DivS parental strain was inhibited by a concentration of 4 μg ml−1. L. monocytogenes LSD530 was shown to be resistant to divergicin M35 at 1·3 μg ml−1. Remarkably, in the presence of divalent cations such as Ca2+, Mg2+ and Mn2+, the lethality caused by divergicin M35 was reduced by 0·48, 0·54 and 0·63 log CFU per ml (after 18 h at 30°C), respectively. The total DNA profiles of DivS and DivM were similar. DivS and DivM showed variable sensitivity to antibiotics. The two-dimensional (2-D) electrophoresis of cell wall proteins did not show any significant difference between DivS and DivM strains but their fatty acid composition showed a significant difference in C16:0 content. Conclusions: Resistance to divergicin M35 is likely ascribed to modification in cell wall fatty acid composition rather than protein modification. Significance and Impact of the Study: This study provides original results contributing to understanding of the resistance of L. monocytogenes to divergicin M35, a new class IIa bacteriocin. [ABSTRACT FROM AUTHOR]

Published

2006

26. The autolytic phenotype of the Bacillus cereus group.

Author

Raddadi, N., Cherif, A., Mora, D., Brusetti, L., Borin, S., Boudabous, A., and Daffonchio, D.

Subjects

BACILLUS cereus, HYDROGEN-ion concentration, AUTOLYSIS, PEPTIDOGLYCANS, POLYACRYLAMIDE gel electrophoresis, MICROCOCCUS luteus, LISTERIA monocytogenes

Abstract

Aim: To determine the autolytic phenotype of five species in the Bacillus cereus group. Methods and Results: The autolytic rate of 96 strains belonging to five species in the B. cereus group was examined under starvation conditions at pH 6, 6·5 and 8·5 in different buffers. The autolytic rate was strain-dependent with a wide variability at pH 6, but higher and more uniform at pH 6·5. At pH 8·5, and respect to the extent of autolysis at pH 6·5, it was relatively low for most of the strains with the lowest values between 13 and 52% in Bacillus mycoides and Bacillus pseudomycoides. Peptidoglycan hydrolase patterns evaluated by renaturing sodium dodecyl sulfate-polyacrylamide gel electrophoresis using cells of Bacillus thuringiensis ssp. tolworthi HD125 as an indicator, revealed complex profiles with lytic bands of about 90, 63, 46, 41, 38, 32, 28 and 25 kDa in B. cereus, B. thuringiensis and Bacillus weihenstephanensis. Bacillus mycoides and B. pseudomycoides had simpler profiles with lytic bands of 63, 46 and 38 kDa. Changes in the autolytic pattern were observed for cells harvested at the stationary phase of growth (72 h) showing an increase in the intensity of the 25 kDa band in the case of B. cereus, B. thuringiensis and B. weihenstephanensis, while no changes were observed for B. mycoides. Using Micrococcus lysodeicticus and Listeria monocytogenes as indicators lytic activity was retained by proteins of 63, 46, 38, 32 and 25 kDa and a new one of about 20 kDa in B. mycoides. Growth in the different media did not affect the autolytic pattern. NaCl abolished the activity of all the peptidoglycan hydrolases except for those of B. mycoides and B. weihenstephanensis. Lytic activity was retained in the presence of MgCl2, MnCl2 and EDTA and increased at basic pH. Conclusions: Bacillus cereus/ B. thuringiensis/ B. weihenstephanensis showed a high extent of autolysis around neutral pH, even though they presented relatively complex autolysin profiles at alkaline pH. Bacillus mycoides/ B. pseudomycoides had a higher extent of autolysis at acidic pH and a simpler autolysin pattern. Significance and Impact of the Study: Information on the autolytic phenotype expand the phenotypic characterization of the different species in the B. cereus group. [ABSTRACT FROM AUTHOR]

Published

2005

27. Microbial solutions to microbial problems; lactococcal bacteriocins for the control of undesirable biota in food.

Author

Guinane, C. M., Cotter, P. D., Hill, C., and Ross, R. P.

Subjects

FOOD microbiology, SANITARY microbiology, LACTOCOCCUS, LACTIC acid bacteria, PATHOGENIC microorganisms, FOOD handling

Abstract

This review will discuss the potential for certain lactococcal bacteriocins to be used as tools for influencing food safety and quality. The focus will be on the potential use of a broadspectrum bacteriocin, lacticin 3147, as a tool to control nonstarter lactic acid bacteria (NSLAB) in cheese, to inhibit pathogens in fermented and nonfermented foods and to extend the shelf life of certain products. Different strategies used to incorporate this bacteriocin into foods will also be described, as will possible problems that may arise when using a bacteriocin in foods. The narrow spectrum bacteriocins, lactococcin ABM (which actually corresponds to three bacteriocins, lactococcins A, B and M produced in a single strain) and the medium-spectrum bacteriocin lacticin 481, also have certain potential applications (albeit limited) in the food industry. In particular, these bacteriocins exhibit a bacteriolytic effect on target cells and so can be used for inducing lysis on sensitive cells during cheese manufacture which concomitantly can lead to accelerated flavour development. [ABSTRACT FROM AUTHOR]

Published

2005

28. The autolytic phenotype of Bacillus thuringiensis.

Author

Raddadi, N., Cherif, A., Mora, D., Ouzari, H., Boudabous, A., Molinari, F., and Daffonchio, D.

Subjects

BACILLUS thuringiensis, PHENOTYPES, AUTOLYSIS, LYSOZYMES, STREPTOMYCES, PROTEINS

Abstract

To evaluate the autolytic phenotype of Bacillus thuringiensis. The autolytic rate of 87 strains belonging to different subsp. of B. thuringiensis was examined at pH 6, 6·5 and 8·5 in different buffers under starvation conditions. At pH 6 the extent of autolysis (average in the strain collection 38·3 ± 21·1) was strain-dependent with wide variability, while at pH 6·5 and 8·5 (averages 72·0 ± 9·0 and 63·1 ± 8·2, respectively) it was much more uniform with only a few strains showing low autolytic rates. Forty-one per cent of the strains showed high resistance (≥80%) to mutanolysin, a commercial muramidase from Streptomyces. The peptidoglycan hydrolase pattern was evaluated by renaturing SDS-PAGE using cells of B. thuringiensis subsp. tolworthi HD125 as indicator. The strain collection showed seven major lytic bands of about 90, 63, 46, 38, 32, 28 and 25 kDa, and in the stationary growth phase (72 h) there was a more intense 25 kDa band in the autolytic pattern. Using Micrococcus lysodeicticus and Listeria monocytogenes as the indicators lytic activity was retained, as seen by the bands of 63, 46, 38, 32 and 25 kDa. Growth in the different media did not affect the autolytic pattern. NaCl abolished the activity of all the peptidoglycan hydrolases in the gel, but in the presence of KCl, MgCl2, MnCl2 and EDTA some activity was retained. At basic pH the lytic activity increased. The autolytic phenotype of B. thuringiensis was found to be strain-dependent, and different proteins exibited peptidoglycan hydrolase activity, particularly at alkaline pH. Several of these proteins retained lytic activity against other bacterial species. The characterisation of the autolytic phenotype of B. thuringiensis should expand the prospects of using this species in bacterial bio-control and field applications. [ABSTRACT FROM AUTHOR]

Published

2004

29. COMPARISON OF CYANAMIDE AND PLACEBO IN THE TREATMENT OF ALCOHOL DEPENDENCE OF ADOLESCENTS.

Author

Niederhofer, Helmut, Staffen, Wolfgang, and Mair, Alois

Subjects

PEOPLE with alcoholism, CYANIC acid, DOSE-response relationship in biochemistry, DISEASE relapse

Abstract

Aims: About 50% of alcoholic patients relapse within 3 months of treatment. Previous studies have suggested that cyanamide may help to prevent such relapse. The aim of our study was to assess the efficacy and safety of long-term cyanamide treatment in alcohol dependence of adolescents. Methods: In this, double-blind, placebo-controlled study, we recruited 26 patients, aged 16-19 years, with chronic (frequent and regular) or episodic (frequent, but irregular) alcohol dependence. Patients were randomly allocated treatment with cyanamide (200 mg daily) or a placebo for 90 days. Patients were assessed on the day the treatment was started, and on days 30 and 90, by interview, self-report, questionnaire and laboratory screening. Patients were classified as abstinent, relapsing or non-attending. Time to first treatment failure (relapse or non-attendance) was the primary outcome measure. Results: The cyanamide (n = 13) and placebo (n = 13) groups were well matched in terms of baseline demographic and alcohol-related variables. Mean cumulative abstinence duration was significantly greater in the cyanamide group than in the placebo group. Apart from occasional diarrhoea, there was no difference in side effects between groups. Conclusions: Cyanamide seems to be an effective and well tolerated pharmacological adjunct to psychosocial and behavioural treatment programrnes for the treatment of some adolescent alcohol-dependent patients. Because of reported hepatotoxic, haematological and dermatological side effects, patients should be observed continuously by experienced clinicians. Further studies are necessary to prove the efficacy of cyanamide in adolescents. [ABSTRACT FROM AUTHOR]

Published

2003

30. Successful treatment of aphthous ulcerations in AIDS patients using topical granulocyte-macrophage colony-stimulating factor.

Author

Herranz, P., Arribas, J.R., Navarro, A., Peña, J.M., González, J., Rubio, F.A., and Casado, M.

Subjects

ULCER treatment, HIV

Abstract

Oral recurrent aphthous ulceration (RAU) is a well-recognized complication in patients infected with human immunodeficiency virus. RAU can be progressive and destructive, causing dysphagia and secondary malnutrition. The aetiology of RAU remains unknown, and its response to available treatments is often unsatisfactory. We describe three patients with advanced AIDS who suffered from extensive RAU which failed to respond to several treatments, including topical viscous lidocaine and topical and systemic glucocorticoids. Owing to difficulties in using thalidomide (two patients had neurological conditions which precluded thalidomide use), all three patients were treated with an oral solution containing recombinant human granulocyte-macrophage colony-stimulating factor (GM-CSF, 400 μg in 5% glucose 200 mL). From the first application, all three patients showed significant improvement of their lesions and amelioration of pain, and they were completely cured in a few days. No adverse effects were recorded. The patients did not show relapses of RAU over a prolonged follow-up. Controlled trials are warranted in order to establish the role of GM-CSF as a valid, alternative option for aphthous ulcerations of the mouth in AIDS patients in whom corticosteroids or thalidomide are not suitable. [ABSTRACT FROM AUTHOR]

Published

2000

31. Short peptides derived from the NH2-terminus of subclass IIa bacteriocin enterocin CRL35 show antimicrobial activity.

Author

Emiliano Salvucci, Lucila Saavedra, and Fernando Sesma

Subjects

BACTERIOCINS, PEPTIDES, LISTERIA monocytogenes, PROTEINS

Abstract

: Objectives Subclass IIa bacteriocins are characterized by a hydrophilic N-terminal domain that shares a YGNGVxCxxxxC consensus and a variable hydrophobic C-terminus. Enterocin CRL35 is a 43-amino-acid heat stable peptide with antilisterial activity. Short synthetic peptides derived from the N-terminal half of enterocin CRL35 and other subclass IIa bacteriocins were evaluated for antimicrobial properties. : Methods In vitro activities of synthetic peptides were evaluated in complex, chemically defined and minimal media. MIC assays were performed by the agar well-diffusion method. Fluorescence assays to evaluate the dissipation of membrane potentials in intact cells were carried out. Time–kill kinetics of Listeria innocua cells with the active peptide were performed. : Results and conclusions A 15-mer peptide derived from enterocin CRL35 inhibited the growth of L. innocua and Listeria monocytogenes in synthetic/minimal media and dissipated the membrane potential of sensitive cells, with MICs of 10 and 50 µM, respectively. 15-mer derivatives from other class IIa bacteriocins (mesentericin Y105, pediocin PA-1 and piscicolin 126) also showed antimicrobial activities. [ABSTRACT FROM AUTHOR]

Published

2007