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网格蛋白通过稳定中心体 ch-TOG 促进有丝分裂早期中心体的完整性。

Clathrin promotes centrosome integrity in early mitosis through stabilization of centrosomal ch-TOG.

机构信息

Department of Bioengineering and Therapeutic Sciences, University of California San Francisco, San Francisco, CA 94143, USA.

出版信息

J Cell Biol. 2012 Aug 20;198(4):591-605. doi: 10.1083/jcb.201205116. Epub 2012 Aug 13.

Abstract

Clathrin depletion by ribonucleic acid interference (RNAi) impairs mitotic spindle stability and cytokinesis. Depletion of several clathrin-associated proteins affects centrosome integrity, suggesting a further cell cycle function for clathrin. In this paper, we report that RNAi depletion of CHC17 (clathrin heavy chain 17) clathrin, but not the CHC22 clathrin isoform, induced centrosome amplification and multipolar spindles. To stage clathrin function within the cell cycle, a cell line expressing SNAP-tagged clathrin light chains was generated. Acute clathrin inactivation by chemical dimerization of the SNAP-tag during S phase caused reduction of both clathrin and ch-TOG (colonic, hepatic tumor overexpressed gene) at metaphase centrosomes, which became fragmented. This was phenocopied by treatment with Aurora A kinase inhibitor, suggesting a centrosomal role for the Aurora A-dependent complex of clathrin, ch-TOG, and TACC3 (transforming acidic coiled-coil protein 3). Clathrin inactivation in S phase also reduced total cellular levels of ch-TOG by metaphase. Live-cell imaging showed dynamic clathrin recruitment during centrosome maturation. Therefore, we propose that clathrin promotes centrosome maturation by stabilizing the microtubule-binding protein ch-TOG, defining a novel role for the clathrin-ch-TOG-TACC3 complex.

摘要

通过核糖核酸干扰 (RNAi) 耗尽网格蛋白会损害有丝分裂纺锤体的稳定性和胞质分裂。几种网格蛋白相关蛋白的耗竭会影响中心体的完整性,这表明网格蛋白具有进一步的细胞周期功能。在本文中,我们报告说,RNAi 耗尽网格蛋白重链 17 (CHC17) 网格蛋白,但不是 CHC22 网格蛋白同工型,会诱导中心体扩增和多极纺锤体。为了在细胞周期内分期网格蛋白的功能,生成了表达 SNAP 标记的网格蛋白轻链的细胞系。在 S 期通过 SNAP 标记的化学二聚化急性失活网格蛋白导致中期中心体的网格蛋白和 ch-TOG(结直肠、肝肿瘤过表达基因)减少,而 ch-TOG 变得碎片化。用 Aurora A 激酶抑制剂处理可复制这种现象,表明 Aurora A 依赖性网格蛋白、ch-TOG 和 TACC3(转化酸性卷曲螺旋蛋白 3)复合物具有中心体作用。S 期的网格蛋白失活也会降低中期细胞中 ch-TOG 的总水平。活细胞成像显示在中心体成熟过程中有网格蛋白的动态募集。因此,我们提出网格蛋白通过稳定微管结合蛋白 ch-TOG 来促进中心体成熟,这为网格蛋白-ch-TOG-TACC3 复合物定义了一个新的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ca45/3514040/bbb963b37c8a/JCB_201205116_Fig1.jpg

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