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波形蛋白在培养细胞中的组装因细胞类型而异。

Assembly of vimentin in cultured cells varies with cell type.

作者信息

Isaacs W B, Cook R K, Van Atta J C, Redmond C M, Fulton A B

机构信息

Department of Biochemistry, University of Iowa, Iowa City 52242.

出版信息

J Biol Chem. 1989 Oct 25;264(30):17953-60.

PMID:2808358
Abstract

To examine how vimentin assembles into the cytoskeletons of cultured cells, we used pulse labeling with [35S]methionine, cell fractionation with Triton X-100, and immunoprecipitation with a monoclonal antibody that binds both nascent and full-length vimentin polypeptides. In embryonic muscle cells, fibroblasts, and erythroid cells, we find two populations of newly synthesized vimentin. One population is found on the cytoskeleton immediately after a 2-min pulse with labeled methionine; the other is delayed in its association with the cytoskeleton and has a measurable rate of disappearance from the extractable pool. This rate varies with cell type, being over 3-fold faster in muscle and fibroblast cells than in erythroid cells. By using [3H]puromycin to specifically label nascent chains, we detect nascent vimentin chains that are bound to the cytoskeleton independently of ribosomes. The fraction of newly synthesized, full-length vimentin that associates with the cytoskeleton immediately correlates in these cell types with the fraction of nascent vimentin chains that are not released from the cytoskeleton by puromycin, RNase, or 0.6 M NaCl. Over one-half of the newly synthesized vimentin associates immediately in muscle and fibroblasts, whereas this value is less than 15% in erythroid cells. These data suggest that the process of vimentin assembly may vary both kinetically and mechanistically in different cell types.

摘要

为了研究波形蛋白如何组装到培养细胞的细胞骨架中,我们使用了[35S]甲硫氨酸脉冲标记、Triton X-100细胞分级分离以及用一种能结合新生和全长波形蛋白多肽的单克隆抗体进行免疫沉淀。在胚胎肌细胞、成纤维细胞和红细胞中,我们发现了两个新合成的波形蛋白群体。一个群体在用标记甲硫氨酸进行2分钟脉冲后立即出现在细胞骨架上;另一个群体与细胞骨架的结合延迟,并且从可提取池中消失的速率可测。该速率因细胞类型而异,在肌细胞和成纤维细胞中比在红细胞中快3倍以上。通过使用[3H]嘌呤霉素特异性标记新生链,我们检测到与细胞骨架结合的新生波形蛋白链独立于核糖体。在这些细胞类型中,新合成的全长波形蛋白与细胞骨架结合的比例与新生波形蛋白链未被嘌呤霉素、核糖核酸酶或0.6 M氯化钠从细胞骨架上释放的比例直接相关。超过一半新合成的波形蛋白在肌细胞和成纤维细胞中立即结合,而在红细胞中这一比例小于15%。这些数据表明波形蛋白组装过程在不同细胞类型中可能在动力学和机制上都有所不同。

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