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ADAM10通过JAMC/RAP1Gap信号通路促进神经干细胞在脑室下区生态位内快速循环并正确定位。

ADAM10 facilitates rapid neural stem cell cycling and proper positioning within the subventricular zone niche via JAMC/RAP1Gap signaling.

作者信息

McMillan Nadia, Kirschen Gregory W, Desai Sanket, Xia Emma, Tsirka Stella E, Aguirre Adan

机构信息

Program in Neuroscience and Medical Scientist Training Program; Department of Pharmacological Sciences, Renaissance School of Medicine at Stony Brook University, Stony Brook, NY; Department of Neurology, Beth Israel Deaconess Medical Center/Harvard Medical School, Boston, MA, USA.

Department of Gynecology and Obstetrics, Johns Hopkins Hospital, Baltimore, MD, USA.

出版信息

Neural Regen Res. 2022 Nov;17(11):2472-2483. doi: 10.4103/1673-5374.339007.

Abstract

The mechanisms that regulate neural stem cell (NSC) lineage progression and maintain NSCs within different domains of the adult neural stem cell niche, the subventricular zone are not well defined. Quiescent NSCs are arranged at the apical ventricular wall, while mitotically activated NSCs are found in the basal, vascular region of the subventricular zone. Here, we found that ADAM10 (a disintegrin and metalloproteinase 10) is essential in NSC association with the ventricular wall, and via this adhesion to the apical domain, ADAM10 regulates the switch from quiescent and undifferentiated NSC to an actively proliferative and differentiating cell state. Processing of JAMC (junctional adhesion molecule C) by ADAM10 increases Rap1GAP activity. This molecular machinery promotes NSC transit from the apical to the basal compartment and subsequent lineage progression. Understanding the molecular mechanisms responsible for regulating the proper positioning of NSCs within the subventricular zone niche and lineage progression of NSCs could provide new targets for drug development to enhance the regenerative properties of neural tissue.

摘要

调节神经干细胞(NSC)谱系进展并在成体神经干细胞生态位(即脑室下区)的不同区域维持神经干细胞的机制尚未完全明确。静止的神经干细胞排列在脑室顶壁,而有丝分裂激活的神经干细胞则位于脑室下区的基底血管区域。在此,我们发现ADAM10(一种解整合素和金属蛋白酶10)对于神经干细胞与脑室壁的结合至关重要,并且通过这种与顶端区域的黏附,ADAM10调节从静止未分化的神经干细胞向活跃增殖和分化细胞状态的转变。ADAM10对JAMC(连接黏附分子C)的加工增加了Rap1GAP活性。这种分子机制促进神经干细胞从顶端向基底区室的转运以及随后的谱系进展。了解负责调节神经干细胞在脑室下区生态位内正确定位以及神经干细胞谱系进展的分子机制,可为药物开发提供新靶点,以增强神经组织的再生特性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b606/9120697/435d4ca91b76/NRR-17-2472-g002.jpg

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