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Titlebook: Early Indicators Early Treatments Neuroprotection in Multiple Sclerosis; Otto R. Hommes,Giancarlo Comi Book 2004 Springer-Verlag Italia 20

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https://doi.org/10.1007/978-3-7091-4484-8en 5% and 60% [7, 10, 11]. Notably, no single HLA type seems to exclude MS. It is therefore clear that as yet unidentified genes residing outside the HLA must also be of importance for disease susceptibility in MS.
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Einleitung und rechtliche Bestimmungen,phological analysis of brain sections [4, 9]. Immunohistochemical studies have recently emphasized the correlation between inflammation and axonal damage during the early stages of MS [4, 9]. In addition, long-term axonal pathology has been described in a number of myelin protein gene knockout and t
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ctive of this study was to investigate the efficacy of IVIg treatment, administered at 0.4 g/kg per day for 5 consecutive days, as a loading dose, and 0.4 g/kg per day every 6 weeks thereafter as a booster dose, for a 1-year period, on the risk of patients with clinically probable MS and positive br
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ential independent markers of the MS disease process compared with the conventional MR measures of subclinical disease — the T2-lesions, and markers of inflammation, the enhancing lesions [7, 8]. Here we summarize the analyses of T1-black holes from the MS Collaborative Research Group Trial of inter
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cells are even found in the CSF in the absence of anti-myelin Abs, suggesting that antibodies rapidly bind to target structures, such as the corresponding auto-antigens or to Fcreceptors, and therefore become undetectable [8, 9]. In organotypic, myelinated cultures of CNS tissue, sera of MS patients
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Welfare Economics in English Utopiasneity occurs is currently unknown. Are RR and PPMS different diseases or are they part of the same clinical spectrum? Why do some patients develop progressive disease whilst others do not? Answers to these questions will not only improve our understanding of MS, but will also have major implications
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Anti-MOG Antibodies as Early Predictors for Conversion to Relapsing-Remitting Disease Course in Patgen for autoreactive antibodies might be the central nervous system (CNS) specific myelin oligodendrocyte glycoprotein (MOG), which is exclusively localized on the surface of myelin sheaths and oligodendrocytes.
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Sunlight, Vitamin D, and Multiple Sclerosis,pairs are discordant for MS, indicating that inheriting MS susceptibility genes is not sufficient for disease development [3]. Thus, MS development requires exposure to one or more environmental risk factors. This suggests that MS may be preventable if these risk factors can be identified and avoided.
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