Arden Susan D, Puri Claudia, Au Josephine Sui-Yan, Kendrick-Jones John, Buss Folma
Cambridge Institute for Medical Research, University of Cambridge, Cambridge CB2 2XY, United Kingdom.
Mol Biol Cell. 2007 Dec;18(12):4750-61. doi: 10.1091/mbc.e07-02-0127. Epub 2007 Sep 19.
Myosin VI plays important roles in endocytic and exocytic membrane-trafficking pathways in cells. Because recent work has highlighted the importance of targeted membrane transport during cytokinesis, we investigated whether myosin VI plays a role in this process during cell division. In dividing cells, myosin VI undergoes dramatic changes in localization: in prophase, myosin VI is recruited to the spindle poles; and in cytokinesis, myosin VI is targeted to the walls of the ingressing cleavage furrow, with a dramatic concentration in the midbody region. Furthermore, myosin VI is present on vesicles moving into and out of the cytoplasmic bridge connecting the two daughter cells. Inhibition of myosin VI activity by small interfering RNA (siRNA)-mediated knockdown or by overexpression of dominant-negative myosin VI tail leads to a delay in metaphase progression and a defect in cytokinesis. GAIP-interacting protein COOH terminus (GIPC), a myosin VI binding partner, is associated with the function(s) of myosin VI in dividing cells. Loss of GIPC in siRNA knockdown cells results in a more than fourfold increase in the number of multinucleated cells. Our results suggest that myosin VI has novel functions in mitosis and that it plays an essential role in targeted membrane transport during cytokinesis.
肌球蛋白VI在细胞的内吞和外排膜运输途径中发挥着重要作用。由于最近的研究突出了胞质分裂过程中靶向膜运输的重要性,我们研究了肌球蛋白VI在细胞分裂过程中是否参与此过程。在分裂细胞中,肌球蛋白VI的定位发生显著变化:在前期,肌球蛋白VI被募集到纺锤体极;在胞质分裂过程中,肌球蛋白VI靶向进入的分裂沟壁,在中间体区域有显著富集。此外,肌球蛋白VI存在于进出连接两个子细胞的细胞质桥的囊泡上。通过小干扰RNA(siRNA)介导的敲低或显性负性肌球蛋白VI尾部的过表达来抑制肌球蛋白VI的活性,会导致中期进程延迟和胞质分裂缺陷。GAIP相互作用蛋白COOH末端(GIPC)是肌球蛋白VI的结合伴侣,与肌球蛋白VI在分裂细胞中的功能相关。siRNA敲低细胞中GIPC的缺失导致多核细胞数量增加四倍以上。我们的结果表明,肌球蛋白VI在有丝分裂中具有新功能,并且在胞质分裂过程中的靶向膜运输中起重要作用。