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Microglia and macrophages of the central nervous system: the contribution of microglia priming and systemic inflammation to chronic neurodegeneration

机译:小胶质细胞和中枢神经系统的巨噬细胞:小胶质细胞引发和全身性炎症对慢性神经变性的贡献

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摘要

Microglia, the resident immune cells of the central nervous system (CNS), play an important role in CNS homeostasis during development, adulthood and ageing. Their phenotype and function have been widely studied, but most studies have focused on their local interactions in the CNS. Microglia are derived from a particular developmental niche, are long-lived, locally replaced and form a significant part of the communication route between the peripheral immune system and the CNS; all these components of microglia biology contribute to maintaining homeostasis. Microglia function is tightly regulated by the CNS microenvironment, and increasing evidence suggests that disturbances, such as neurodegeneration and ageing, can have profound consequences for microglial phenotype and function. We describe the possible biological mechanisms underlying the altered threshold for microglial activation, also known as ‘microglial priming’, seen in CNS disease and ageing and consider how priming may contribute to turning immune-to-brain communication from a homeostatic pathway into a maladaptive response that contributes to symptoms and progression of diseases of the CNS.
机译:小胶质细胞是中枢神经系统(CNS)的固有免疫细胞,在发育,成年和衰老过程中对CNS体内平衡起着重要作用。它们的表型和功能已被广泛研究,但大多数研究集中在它们在中枢神经系统中的局部相互作用。小胶质细胞起源于特定的发育环境,是长寿的,被局部取代的,并构成外周免疫系统和中枢神经系统之间通信途径的重要组成部分。小胶质细胞生物学的所有这些成分都有助于维持体内稳态。小胶质细胞的功能受到中枢神经系统微环境的严格调节,越来越多的证据表明,神经变性和衰老等疾病可能对小胶质细胞的表型和功能产生深远的影响。我们描述了中枢神经系统疾病和衰老中所见的改变的小胶质细胞激活阈值(也称为“小胶质细胞引发”)背后的可能生物学机制,并考虑了引发可能如何将免疫-脑通讯从稳态途径转变为适应不良反应。导致中枢神经系统疾病的症状和进展。

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