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Cell death in the neighbourhood: direct microenvironmental effects of apoptosis in normal and neoplastic tissues.细胞在邻居中死亡:细胞凋亡对正常组织和肿瘤组织的直接微环境影响。
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Microglia shape adult hippocampal neurogenesis through apoptosis-coupled phagocytosis.小胶质细胞通过凋亡偶联吞噬作用来塑造成年海马神经发生。
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Unexpected requirement for ELMO1 in clearance of apoptotic germ cells in vivo.体内凋亡生殖细胞清除过程中 ELMO1 的意外需求。
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Clearance of apoptotic cells: implications in health and disease.凋亡细胞的清除:对健康与疾病的影响
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Autoimmunity and the clearance of dead cells.自身免疫与细胞死亡的清除。
Cell. 2010 Mar 5;140(5):619-30. doi: 10.1016/j.cell.2010.02.014.
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Thrombospondin 1--a key astrocyte-derived neurogenic factor.血栓反应蛋白 1——一种关键的星形细胞衍生的神经发生因子。
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Glial precursors clear sensory neuron corpses during development via Jedi-1, an engulfment receptor.在发育过程中,神经胶质前体细胞通过一种吞噬受体Jedi-1清除感觉神经元尸体。
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A minimally invasive, translational biomarker of ketamine-induced neuronal death in rats: microPET Imaging using 18F-annexin V.大鼠中氯胺酮诱导神经元死亡的一种微创性、可转化生物标志物:使用18F-膜联蛋白V的微型正电子发射断层显像(microPET)成像
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神经元祖细胞的吞噬活性调节成年神经发生。

Phagocytic activity of neuronal progenitors regulates adult neurogenesis.

机构信息

Department of Neuroscience, University of Virginia, Charlottesville, Virginia 22901, USA.

出版信息

Nat Cell Biol. 2011 Jul 31;13(9):1076-83. doi: 10.1038/ncb2299.

DOI:10.1038/ncb2299
PMID:21804544
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3374401/
Abstract

Whereas thousands of new neurons are generated daily during adult life, only a fraction of them survive and become part of neural circuits; the rest die, and their corpses are presumably cleared by resident phagocytes. How the dying neurons are removed and how such clearance influences neurogenesis are not well understood. Here, we identify an unexpected phagocytic role for the doublecortin (DCX)-positive neuronal progenitor cells during adult neurogenesis. Our in vivo and ex vivo studies demonstrate that DCX(+) cells comprise a significant phagocytic population within the neurogenic zones. Intracellular engulfment protein ELMO1, which promotes Rac activation downstream of phagocytic receptors, was required for phagocytosis by DCX(+) cells. Disruption of engulfment in vivo genetically (in Elmo1-null mice) or pharmacologically (in wild-type mice) led to reduced uptake by DCX(+) cells, accumulation of apoptotic nuclei in the neurogenic niches and impaired neurogenesis. Collectively, these findings indicate a paradigm wherein DCX(+) neuronal precursors also serve as phagocytes, and that their phagocytic activity critically contributes to neurogenesis in the adult brain.

摘要

虽然成年期每天都会产生数千个新神经元,但其中只有一小部分能够存活下来并成为神经回路的一部分;其余的则会死亡,它们的尸体可能被驻留的吞噬细胞清除。死亡神经元是如何被清除的,以及这种清除如何影响神经发生,目前还不是很清楚。在这里,我们在成年神经发生过程中发现了双皮质素 (DCX) 阳性神经元祖细胞的一个意外吞噬作用。我们的体内和体外研究表明,DCX(+) 细胞在神经发生区构成了一个重要的吞噬细胞群体。胞内吞噬蛋白 ELMO1 在吞噬受体下游促进 Rac 的激活,是 DCX(+) 细胞吞噬作用所必需的。体内遗传(Elmo1 基因敲除小鼠)或药理学(野生型小鼠)阻断吞噬作用会导致 DCX(+) 细胞摄取减少、神经发生龛中凋亡核的积累以及神经发生受损。总之,这些发现表明了一种范例,即 DCX(+) 神经元前体细胞也作为吞噬细胞,其吞噬活性对成年大脑中的神经发生至关重要。