Oligodendrocyte Progenitors in Schizophrenia: The Role in Pathogenesis and Potential Treatment Target

N. Kolomeets
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Abstract

Background:  schizophrenia is considered as a dysconnectivity disorder supported by neuroimaging studies have revealed altered myelination of white and grey matter. Altered myelination suggests oligodendrocyte (OL) family pathology. Oligodendrocyte progenitors (OP) are of special interest since they myelinate axons in mature brain at the last stage of the differentiation. The aim of review  —  to summarize modern research data concerning altered cell cycle of OL family in schizophrenia and their plausible reason. Material and methods: using the keywords “schizophrenia, OL, OP”, “OP and schizophrenia risk genes”, “OP and neuroinflamation”, “OP and antipsychotic drugs”, “OP, dopamine, serotonin” 164 studies concerning the influence of listed above factors on OP differentiation were selected the MedLine/PubMed, Google Scholar, eLibrary databases for analysis.  Conclusion: postmortem studies demonstrated essential deficit of OL family cells as well as altered correlation pattern between the number of these cells suggested altered OP differentiation. Some of OL and myelin-related gene variants caused higher schizophrenia risk play a critical role in OP differentiation. While neuroinflammation is important component of schizophrenia brain pathology proinflammatory cytokines and activated microglia exert substantial influence on OP proliferation and differentiation. Atypical antipsychotics are able to correct OP maturation and have anti-inflammatory effects. OL and OP as well as microglia and peripheral immune cells express dopamine and serotonin receptors, main  therapeutic targets of these drugs. OP pathology as important component of schizophrenia  pathogenesis, tightly linked with another abnormalities, and considers as promising target for future therapeutic strategy.
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精神分裂症中的少突胶质细胞祖细胞:在发病机制中的作用和潜在的治疗目标
背景:精神分裂症被认为是一种连接障碍性疾病,神经影像学研究显示,白质和灰质的髓鞘化发生了改变。髓鞘化改变提示少突胶质细胞(OL)家族病变。少突胶质细胞祖细胞(OP)在成熟大脑分化的最后阶段髓鞘化轴突,因此特别值得关注。综述的目的是总结有关精神分裂症 OL 家族细胞周期改变的现代研究数据及其合理原因。材料与方法:使用关键词 "精神分裂症、OL、OP"、"OP 与精神分裂症风险基因"、"OP 与神经损伤"、"OP 与抗精神病药物"、"OP、多巴胺、5-羟色胺",在 MedLine/PubMed、Google Scholar、eLibrary 数据库中选择了 164 项有关上述因素对 OP 分化影响的研究进行分析。 结论:死后研究表明,OL 家族细胞基本缺失,这些细胞数量之间的相关模式发生了改变,这表明 OP 分化发生了改变。一些导致精神分裂症风险较高的 OL 和髓鞘相关基因变异在 OP 分化过程中起着关键作用。神经炎症是精神分裂症大脑病理学的重要组成部分,而促炎细胞因子和活化的小胶质细胞对 OP 的增殖和分化有很大影响。非典型抗精神病药物能够纠正 OP 的成熟,并具有抗炎作用。OL和OP以及小胶质细胞和外周免疫细胞表达多巴胺和5-羟色胺受体,这是这些药物的主要治疗靶点。OP病理学是精神分裂症发病机制的重要组成部分,与其他异常密切相关,被认为是未来治疗策略的有希望的靶点。
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