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S100B protein in neurodegenerative disorders.

机译:S100B蛋白在神经退行性疾病中。

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"Classic" neurodegenerative disorders, such as Alzheimer's disease and amyotrophic lateral sclerosis share common pathophysiological features and involve progressive loss of specific neuronal populations, axonal or synaptic loss and dysfunction, reactive astrogliosis, and reduction in myelin. Furthermore, despite the absence of astrogliosis, impaired expression of astrocyte- and oligodendrocyte-related genes has been observed in patients with major psychiatric disorders, including schizophrenia and mood disorders. Because S100B is expressed in astrocytes and oligodendrocytes, its concentration in cerebrospinal fluid (CSF) or serum has been considered a suitable surrogate marker for the diagnostic or prognostic assessment of neurodegeneration. This review summarizes previous postmortem, CSF and serum studies regarding the role of S100B in this context. A general drawback is that only small single-center studies have been performed. Many potential confounding factors exist because of the wide extra-astrocytic and extracerebral expression of S100B. Due to lack of disease specificity, reliance on S100B concentrations for differential diagnostic purposes in cases of suspected neurodegenerative disorders is not recommended. Moreover, there is no consistent evidence for a correlation between disease severity and concentrations of S100B in CSF or serum. Therefore, S100B has limited usefulness for monitoring disease progression.
机译:“经典的”神经退行性疾病,例如阿尔茨海默氏病和肌萎缩性侧索硬化症具有共同的病理生理特征,并且涉及特定神经元群体的进行性丧失,轴突或突触丧失和功能障碍,反应性星形胶质增生和髓磷脂减少。此外,尽管没有星形胶质细胞增生,在患有精神分裂症和情绪障碍等主要精神疾病的患者中也观察到星形胶质细胞和少突胶质细胞相关基因的表达受损。因为S100B在星形胶质细胞和少突胶质细胞中表达,所以它在脑脊液(CSF)或血清中的浓度被认为是诊断或预测神经变性的合适替代指标。这篇综述总结了先前关于S100B在这种情况下的作用的验尸,脑脊液和血清研究。一个普遍的缺点是只进行了小的单中心研究。由于S100B的广泛的星形细胞外和脑外表达,存在许多潜在的混淆因素。由于缺乏疾病特异性,不建议在怀疑有神经退行性疾病的情况下依赖S100B浓度进行鉴别诊断。此外,尚无一致的证据表明疾病严重程度与脑脊液或血清中S100B的浓度之间存在相关性。因此,S100B在监测疾病进展方面的用途有限。

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