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通过表达R183A D184A突变型β-肌动蛋白在HeLa细胞中建立对拉春库林-A的抗性。

Establishment of latrunculin-A resistance in HeLa cells by expression of R183A D184A mutant beta-actin.

作者信息

Fujita Masatoshi, Ichinose Sachiyo, Kiyono Tohru, Tsurumi Tatsuya, Omori Akira

机构信息

Laboratory of Viral Oncology, Research Institute, Aichi Cancer Center, Nagoya, Japan.

出版信息

Oncogene. 2003 Jan 30;22(4):627-31. doi: 10.1038/sj.onc.1206173.

Abstract

Actin plays central roles in cell motility through formation of the actin cytoskeleton. Recently, the very intriguing possibility that actin also contributes to processes in the cell nucleus has been emerging. To dissect its dynamics and functions, several actin-disrupting drugs have been widely and effectively employed. Among them, latrunculin-A has proved particularly useful, supplanting the classical drug cytochalasin-D. One reason is that latrunculin-A appears to bind only to actin monomers impairing the nucleotide exchange, the mode being simpler than with cytochalasin. This property may be especially crucial when studying actin functions as a monomer, as suggested for nuclear actin. Very importantly, actin mutations that cause cells to become resistant to the effects of latrunculin-A have been identified in budding yeast. However, it remains controversial as to whether all of the various phenotypes observed with latrunculin in mammalian cells more complicated than yeast are truly the consequence of its specific actions against actin. Here, we show that the expression of R183A D184A mutant beta-actin specifically confers resistance to the effects of latrunculin-A on actin cytoskeleton formation and cell growth in HeLa cells. The established system provides a strong tool to address the various functions of actin in mammalian cells.

摘要

肌动蛋白通过形成肌动蛋白细胞骨架在细胞运动中发挥核心作用。最近,肌动蛋白也参与细胞核内过程这一非常有趣的可能性逐渐显现出来。为了剖析其动力学和功能,几种破坏肌动蛋白的药物已被广泛且有效地应用。其中,拉特罗毒素 - A已被证明特别有用,取代了经典药物细胞松弛素 - D。一个原因是拉特罗毒素 - A似乎仅与肌动蛋白单体结合,损害核苷酸交换,其作用方式比细胞松弛素更简单。当研究肌动蛋白作为单体的功能时,如核肌动蛋白的情况,这种特性可能尤为关键。非常重要的是,在芽殖酵母中已鉴定出导致细胞对拉特罗毒素 - A的作用产生抗性的肌动蛋白突变。然而,对于在哺乳动物细胞中观察到的比酵母更复杂的用拉特罗毒素处理后的各种表型是否真的是其对肌动蛋白的特异性作用的结果,仍存在争议。在这里,我们表明R183A D184A突变型β - 肌动蛋白的表达特异性地赋予了HeLa细胞对拉特罗毒素 - A对肌动蛋白细胞骨架形成和细胞生长的影响的抗性。所建立的系统为研究肌动蛋白在哺乳动物细胞中的各种功能提供了一个强大的工具。

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