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ATP结合结构域中的突变会影响有丝分裂着丝粒相关驱动蛋白(MCAK)的亚细胞分布。

Mutations in the ATP-binding domain affect the subcellular distribution of mitotic centromere-associated kinesin (MCAK).

作者信息

Wordeman L, Wagenbach M, Maney T

机构信息

Department of Physiology and Biophysics, University of Washington School of Medicine, Seattle, WA 98195, USA.

出版信息

Cell Biol Int. 1999;23(4):275-86. doi: 10.1006/cbir.1999.0359.

Abstract

Mitotic centromere-associated kinesin (MCAK) is important for anaphase chromosome segregation. MCAK is diffusely localized to both the cytoplasm and the nucleus during interphase. At prophase MCAK is recruited to mitotic centromeres. It is associated with centromeres throughout mitosis and then returns to exhibiting a diffuse nuclear and cytoplasmic localization during interphase. MCAK has several predicted nuclear localization sequences. The subcellular distribution of expressed deletion constructs of GFP-MCAK suggest that the nucleocytoplasmic ratio of MCAK protein is dependent on a balance between several predicted nuclear localization sequences (NLS) and a putative nuclear exclusion sequence (NES) in the amino-terminal region of MCAK. Amino acid substitutions in the ATP-binding domain of the MCAK motor affect nuclear localization, which, in turn, influences the degree of centromere binding.

摘要

有丝分裂着丝粒相关驱动蛋白(MCAK)对后期染色体分离很重要。在间期,MCAK分散地定位于细胞质和细胞核。在前期,MCAK被招募到有丝分裂着丝粒。在整个有丝分裂过程中它都与着丝粒相关,然后在间期又恢复为分散的核和细胞质定位。MCAK有几个预测的核定位序列。GFP-MCAK表达缺失构建体的亚细胞分布表明,MCAK蛋白的核质比取决于MCAK氨基末端区域几个预测的核定位序列(NLS)和一个假定的核输出序列(NES)之间的平衡。MCAK马达ATP结合结构域中的氨基酸替换会影响核定位,进而影响着丝粒结合程度。

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