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帕瓦罗蒂动力蛋白样蛋白(Pavarotti-KLP)在活体果蝇胚胎中的定位表明其在有丝分裂周期中重组皮质细胞骨架时发挥作用。

Localization of Pavarotti-KLP in living Drosophila embryos suggests roles in reorganizing the cortical cytoskeleton during the mitotic cycle.

作者信息

Minestrini Gianluca, Harley Alyssa S, Glover David M

机构信息

Cancer Research UK, Cell Cycle Genetics Group, University of Cambridge, Department of Genetics, Cambridge CB2 3EH, United Kingdom.

出版信息

Mol Biol Cell. 2003 Oct;14(10):4028-38. doi: 10.1091/mbc.e03-04-0214. Epub 2003 Jun 27.

Abstract

Pav-KLP is the Drosophila member of the MKLP1 family essential for cytokinesis. In the syncytial blastoderm embryo, GFP-Pav-KLP cyclically associates with astral, spindle, and midzone microtubules and also to actomyosin pseudocleavage furrows. As the embryo cellularizes, GFP-Pav-KLP also localizes to the leading edge of the furrows that form cells. In mononucleate cells, nuclear localization of GFP-Pav-KLP is mediated through NLS elements in its C-terminal domain. Mutants in these elements that delocalize Pav-KLP to the cytoplasm in interphase do not affect cell division. In mitotic cells, one population of wild-type GFP-Pav-KLP associates with the spindle and concentrates in the midzone at anaphase B. A second is at the cell cortex on mitotic entry and later concentrates in the region of the cleavage furrow. An ATP binding mutant does not localize to the cortex and spindle midzone but accumulates on spindle pole microtubules to which actin is recruited. This leads either to failure of the cleavage furrow to form or later defects in which daughter cells remain connected by a microtubule bridge. Together, this suggests Pav-KLP transports elements of the actomyosin cytoskeleton to plus ends of astral microtubules in the equatorial region of the cell to permit cleavage ring formation.

摘要

Pav-KLP是胞质分裂所必需的MKLP1家族的果蝇成员。在合胞体胚盘胚胎中,GFP-Pav-KLP周期性地与星体、纺锤体和中间区微管结合,也与肌动球蛋白假分裂沟结合。随着胚胎细胞化,GFP-Pav-KLP也定位于形成细胞的沟的前沿。在单核细胞中,GFP-Pav-KLP的核定位是通过其C末端结构域中的核定位信号元件介导的。这些元件中的突变体使Pav-KLP在间期定位于细胞质中,但不影响细胞分裂。在有丝分裂细胞中,野生型GFP-Pav-KLP的一部分与纺锤体结合,并在后期B集中在中间区。另一部分在有丝分裂开始时位于细胞皮层,随后集中在分裂沟区域。一个ATP结合突变体不定位到皮层和纺锤体中间区,而是聚集在募集了肌动蛋白的纺锤体极微管上。这要么导致分裂沟形成失败,要么导致后期缺陷,即子细胞通过微管桥保持连接。总之,这表明Pav-KLP将肌动球蛋白细胞骨架的元件运输到细胞赤道区域星体微管的正端,以允许形成分裂环。

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