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活细胞中肌动蛋白组装的可视化与分子分析

Visualization and molecular analysis of actin assembly in living cells.

作者信息

Schafer D A, Welch M D, Machesky L M, Bridgman P C, Meyer S M, Cooper J A

机构信息

Department of Cell Biology and Physiology, Washington University School of Medicine, St. Louis, Missouri 63110, USA.

出版信息

J Cell Biol. 1998 Dec 28;143(7):1919-30. doi: 10.1083/jcb.143.7.1919.

Abstract

Actin filament assembly is critical for eukaryotic cell motility. Arp2/3 complex and capping protein (CP) regulate actin assembly in vitro. To understand how these proteins regulate the dynamics of actin filament assembly in a motile cell, we visualized their distribution in living fibroblasts using green flourescent protein (GFP) tagging. Both proteins were concentrated in motile regions at the cell periphery and at dynamic spots within the lamella. Actin assembly was required for the motility and dynamics of spots and for motility at the cell periphery. In permeabilized cells, rhodamine-actin assembled at the cell periphery and at spots, indicating that actin filament barbed ends were present at these locations. Inhibition of the Rho family GTPase rac1, and to a lesser extent cdc42 and RhoA, blocked motility at the cell periphery and the formation of spots. Increased expression of phosphatidylinositol 5-kinase promoted the movement of spots. Increased expression of LIM-kinase-1, which likely inactivates cofilin, decreased the frequency of moving spots and led to the formation of aggregates of GFP-CP. We conclude that spots, which appear as small projections on the surface by whole mount electron microscopy, represent sites of actin assembly where local and transient changes in the cortical actin cytoskeleton take place.

摘要

肌动蛋白丝组装对于真核细胞运动至关重要。Arp2/3复合物和封端蛋白(CP)在体外调节肌动蛋白组装。为了解这些蛋白质如何在运动细胞中调节肌动蛋白丝组装的动力学,我们使用绿色荧光蛋白(GFP)标记在活的成纤维细胞中观察它们的分布。这两种蛋白质都集中在细胞周边的运动区域以及片层内的动态斑点处。斑点的运动和动力学以及细胞周边的运动都需要肌动蛋白组装。在通透细胞中,罗丹明标记的肌动蛋白在细胞周边和斑点处组装,表明这些位置存在肌动蛋白丝的带刺末端。Rho家族GTP酶rac1的抑制,以及程度较轻的cdc42和RhoA的抑制,会阻断细胞周边的运动和斑点的形成。磷脂酰肌醇5激酶表达的增加促进了斑点的移动。LIM激酶-1表达的增加可能使丝切蛋白失活,降低了移动斑点的频率并导致GFP-CP聚集体的形成。我们得出结论,通过整装电子显微镜观察到的在表面上呈现为小突起的斑点代表肌动蛋白组装位点,在此处皮质肌动蛋白细胞骨架发生局部和瞬时变化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1b84/2175235/939c6dcb8dd1/JCB9805067.f1.jpg

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