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Microglial diversity by responses and responders

机译:反应和反应者的小胶质多样性

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摘要

Microglia are the principal resident innate immune cells of the CNS. Their contributions to the normal development of the CNS, the maintenance and plasticity of neuronal networks and the safeguarding of proper functionality are becoming more and more evident. Microglia also survey the tissue homeostasis to respond rapidly to exogenous and endogenous threats, primarily with a protective outcome. However, excessive acute activation, chronic activity or an improper adaptation of their functional performance can foster neuropathologies. A key to the versatile response behavior of these cells is their ability to commit to reactive phenotypes, which reveal enormous complexity. Yet the respective profiles of induced genes and installed functions may build up on heterogeneous contributions of cellular subsets. Here, we discuss findings and concepts that consider the variety of microglial activities and response options as being based—at least in part—on a diversity of the engaged cells. Whether it is the production of proinflammatory cytokines, clearance of tissue debris, antigen presentation or the ability to sense neurotransmitters, microglial cells present with an unanticipated heterogeneity of their constitutive and inducible features. While the organizational principles of this heterogeneity are still largely unknown, functional implications are already perceptible.
机译:小胶质细胞是中枢神经系统的主要固有先天免疫细胞。它们对中枢神经系统正常发育,神经元网络的维护和可塑性以及适当功能的维护的贡献变得越来越明显。小胶质细胞也调查组织动态平衡,以快速响应外源性和内源性威胁,主要具有保护作用。但是,过度的急性激活,慢性活动或对其功能表现的不适当适应会促进神经病理学的发展。这些细胞的通用反应行为的关键是它们具有反应性表型的能力,这揭示了巨大的复杂性。然而,诱导基因和已安装功能的各自概况可能建立在细胞亚群的异质贡献上。在这里,我们讨论的发现和概念将小胶质细胞活动和反应选项的多样性视为(至少部分地)基于参与细胞的多样性。无论是促炎性细胞因子的产生,组织碎片的清除,抗原呈递还是感觉神经递质的能力,小胶质细胞都呈现出其结构性和诱导性特征出乎意料的异质性。尽管这种异质性的组织原则仍是未知之数,但功能上的含义已经可以理解。

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