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内吞内化过程中受体、衔接蛋白和肌动蛋白的关联途径。

A pathway for association of receptors, adaptors, and actin during endocytic internalization.

作者信息

Kaksonen Marko, Sun Yidi, Drubin David G

机构信息

Department of Molecular and Cell Biology, 16 Barker Hall, University of California, Berkeley, Berkeley, CA 94720, USA.

出版信息

Cell. 2003 Nov 14;115(4):475-87. doi: 10.1016/s0092-8674(03)00883-3.

Abstract

In budding yeast, many proteins involved in endocytic internalization, including adaptors and actin cytoskeletal proteins, are localized to cortical patches of differing protein composition. Using multicolor real-time fluorescence microscopy and particle tracking algorithms, we define an early endocytic pathway wherein an invariant sequence of changes in cortical patch protein composition correlates with changes in patch motility. Three Arp2/3 activators each showed a distinct behavior, suggesting distinct patch-related endocytic functions. Actin polymerization occurs late in the endocytic pathway and is required both for endocytic internalization and for patch disassembly. In cells lacking the highly conserved endocytic protein Sla2p, patch motility was arrested and actin comet tails associated with endocytic patch complexes. Fluorescence recovery after photobleaching of the actin comet tails revealed that endocytic complexes are nucleation sites for rapid actin polymerization. Attention is now focused on the mechanisms by which the order and timing of events in this endocytic pathway are achieved.

摘要

在出芽酵母中,许多参与胞吞内化的蛋白质,包括衔接蛋白和肌动蛋白细胞骨架蛋白,都定位于蛋白质组成不同的皮质斑。利用多色实时荧光显微镜和粒子追踪算法,我们定义了一条早期胞吞途径,其中皮质斑蛋白质组成的不变变化序列与斑的运动性变化相关。三种Arp2/3激活剂各表现出独特的行为,表明与斑相关的胞吞功能不同。肌动蛋白聚合发生在胞吞途径的后期,是胞吞内化和斑解体所必需的。在缺乏高度保守的胞吞蛋白Sla2p的细胞中,斑的运动性被阻断,肌动蛋白彗星尾与胞吞斑复合物相关联。对肌动蛋白彗星尾进行光漂白后的荧光恢复显示,胞吞复合物是快速肌动蛋白聚合的成核位点。现在人们的注意力集中在实现这条胞吞途径中事件的顺序和时间的机制上。

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