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Phagocytic Roles of Glial Cells in Healthy and Diseased Brains

机译:吞噬细胞在健康和患病脑中的吞噬作用

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摘要

Glial cells are receiving much attention since they have been recognized as important regulators of many aspects of brain function and disease. Recent evidence has revealed that two different glial cells, astrocytes and microglia, control synapse elimination under normal and pathological conditions via phagocytosis. Astrocytes use the MEGF10 and MERTK phagocytic pathways, and microglia use the classical complement pathway to recognize and eliminate unwanted synapses. Notably, glial phagocytosis also contributes to the clearance of disease-specific protein aggregates, such as beta-amyloid, huntingtin, and a-synuclein. Here we reivew recent findings showing that glial cells are active regulators in brain functions through phagocytosis and that changes in glial phagocytosis contribute to the pathogenesis of various neurodegenerative diseases. A better understanding of the cellular and molecular mechanisms of glial phagocytosis in healthy and diseased brains will greatly improve our current approach in treating these diseases.
机译:胶质细胞正在受到很多关注,因为它们被认为是脑功能和疾病的许多方面的重要调节因素。最近的证据表明,两种不同的胶质细胞,星形胶质细胞和小胶质细胞,通过吞噬作用控制正常和病理条件下的突触消除。星形胶质细胞使用Megf10和Mertk吞噬途径,并且微胶质细胞使用经典的补充途径来识别和消除不需要的突触。值得注意的是,胶质吞噬作用也有助于疾病特异性蛋白质聚集体的清除,例如β-淀粉样蛋白,亨廷顿和突触核蛋白。在这里,我们最近的发现表明,胶质细胞是通过吞噬作用的脑功能中的活性调节剂,并且胶虫吞噬作用的变化有助于各种神经变性疾病的发病机制。更好地了解健康和患病脑中胶质细胞增多症的细胞和分子机制将大大提高我们目前治疗这些疾病的方法。

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