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MTSS1 通过调控树突丝状伪足中的肌动蛋白成核形成蛋白 DAAM1 来决定浦肯野细胞的最终树突形态。

MTSS1 Regulation of Actin-Nucleating Formin DAAM1 in Dendritic Filopodia Determines Final Dendritic Configuration of Purkinje Cells.

机构信息

Institute for Integrated Cell-Material Sciences (WPI-iCeMS), Kyoto 606-8501, Japan; Graduate School of Biostudies, Kyoto University, Kyoto 606-8501, Japan.

Institute for Integrated Cell-Material Sciences (WPI-iCeMS), Kyoto 606-8501, Japan.

出版信息

Cell Rep. 2018 Jul 3;24(1):95-106.e9. doi: 10.1016/j.celrep.2018.06.013.

Abstract

Dendritic filopodia of developing neurons function as environmental sensors, regulating the spatial organization of dendrites and proper targeting to presynaptic partners. Dendritic filopodia morphology is determined by the balance of F-actin assembled via two major nucleating pathways, the ARP2/3 complex and formins. The inverse-BAR protein MTSS1 is highly expressed in Purkinje cells (PCs) and has been shown to upregulate ARP2/3 activity. PCs in MTSS1 conditional knockout mice showed dendrite hypoplasia due to excessive contact-induced retraction during development. This phenotype was concomitant with elongated dendritic filopodia and was phenocopied by overactivation of the actin nucleator formin DAAM1 localized in the tips of PC dendritic protrusions. Cell biology assays including single-molecule speckle microscopy demonstrated that MTSS1's C terminus binds to DAAM1 and paused DAAM1-mediated F-actin polymerization. Thus, MTSS1 plays a dual role as a formin inhibitor and ARP2/3 activator in dendritic filopodia, determining final neuronal morphology.

摘要

发育中的神经元树突丝状伪足作为环境传感器发挥作用,调节树突的空间组织并与突触前伴侣正确靶向。树突丝状伪足的形态由通过两种主要成核途径组装的 F-肌动蛋白的平衡决定,这两种途径是 ARP2/3 复合物和formin。反向 BAR 蛋白 MTSS1 在浦肯野细胞(PC)中高度表达,并已被证明上调 ARP2/3 活性。MTSS1 条件性敲除小鼠中的 PC 显示出树突发育不良,这是由于在发育过程中过度接触诱导的回缩引起的。这种表型与伸长的树突丝状伪足并存,并通过位于 PC 树突突起尖端的肌动蛋白成核因子formin DAAM1 的过度激活来模拟。包括单分子斑点显微镜在内的细胞生物学测定表明,MTSS1 的 C 末端与 DAAM1 结合并暂停了 DAAM1 介导的 F-肌动蛋白聚合。因此,MTSS1 在树突丝状伪足中作为formin 抑制剂和 ARP2/3 激活剂发挥双重作用,决定最终的神经元形态。

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