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纺锤体蛋白对于人类细胞的快速迁移是必需的。

Spindly is required for rapid migration of human cells.

作者信息

Conte Claudia, Baird Michelle A, Davidson Michael W, Griffis Eric R

机构信息

Centre for Gene Regulation and Expression, College of Life Sciences, University of Dundee, Dundee DD1 5EH, UK

Department of Biological Science, National High Magnetic Field Laboratory, Florida State University, Tallahassee, FL 32306, USA.

出版信息

Biol Open. 2018 May 29;7(5):bio033233. doi: 10.1242/bio.033233.

Abstract

Dynein is the sole processive minus-end-directed microtubule motor found in animals. It has roles in cell division, membrane trafficking, and cell migration. Together with dynactin, dynein regulates centrosomal orientation to establish and maintain cell polarity, controls focal adhesion turnover and anchors microtubules at the leading edge. In higher eukaryotes, dynein/dynactin requires additional components such as Bicaudal D to form an active motor complex and for regulating its cellular localization. Spindly is a protein that targets dynein/dynactin to kinetochores in mitosis and can activate its motility However, no role for Spindly in interphase dynein/dynactin function has been found. We show that Spindly binds to the cell cortex and microtubule tips and colocalizes with dynein/dynactin at the leading edge of migrating U2OS cells and primary fibroblasts. U2OS cells that lack Spindly migrated slower in 2D than control cells, although centrosome polarization appeared to happen properly in the absence of Spindly. Re-expression of Spindly rescues migration, but the expression of a mutant, which is defective for dynactin binding, failed to rescue this defect. Taken together, these data demonstrate that Spindly plays an important role in mediating a subset of dynein/dynactin's function in cell migration.

摘要

动力蛋白是动物体内唯一的一种沿微管负端定向移动的持续性马达蛋白。它在细胞分裂、膜运输和细胞迁移中发挥作用。动力蛋白与动力蛋白激活蛋白一起,调节中心体方向以建立和维持细胞极性,控制粘着斑周转并将微管锚定在前缘。在高等真核生物中,动力蛋白/动力蛋白激活蛋白需要其他成分(如双尾D)来形成活性马达复合体并调节其细胞定位。纺锤体蛋白是一种在有丝分裂过程中将动力蛋白/动力蛋白激活蛋白靶向至动粒的蛋白质,并且能够激活其运动性。然而,尚未发现纺锤体蛋白在间期动力蛋白/动力蛋白激活蛋白功能中发挥作用。我们发现,纺锤体蛋白结合到细胞皮层和微管末端,并与动力蛋白/动力蛋白激活蛋白在迁移的U2OS细胞和原代成纤维细胞的前缘共定位。缺乏纺锤体蛋白的U2OS细胞在二维环境中的迁移速度比对照细胞慢,尽管在缺乏纺锤体蛋白的情况下中心体极化似乎仍能正常发生。纺锤体蛋白的重新表达可挽救迁移缺陷,但一种与动力蛋白激活蛋白结合存在缺陷的突变体的表达未能挽救此缺陷。综上所述,这些数据表明,纺锤体蛋白在介导动力蛋白/动力蛋白激活蛋白在细胞迁移中的部分功能方面发挥重要作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c54b/5992534/4192f95b02a2/biolopen-7-033233-g1.jpg

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