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首页> 外文期刊>Molecular biology of the cell >Bim1p/Yeb1p mediates the Kar9p-dependent cortical attachment of cytoplasmic microtubules
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Bim1p/Yeb1p mediates the Kar9p-dependent cortical attachment of cytoplasmic microtubules

机译:Bim1p / Yeb1p介导细胞质微管的Kar9p依赖性皮质附着。

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摘要

In Saccharomyces cerevisiae, positioning of the mitotic spindle depends on the interaction of cytoplasmic microtubules with the cell cortex. Ln this process, cortical Kar9p in the bud acts as a link between the actin and microtubule cytoskeletons. To identify Kar9p-interacting proteins, a two-hybrid screen was conducted with the use of full-length Kar9p as bait, and three genes were identified: BIM1, STU2, and KAR9 itself. STU2 encodes a component of the spindle pole body. Bim1p is the yeast homologue of the human microtubule-binding protein EB1, which is a binding partner to the adenomatous polyposis coli protein involved in colon cancer. Eighty-nine amino acids within the third quarter of Bim1p was sufficient to confer interaction with Kar9p. The two-hybrid interactions were confirmed with the use of coimmunoprecipitation experiments. Genetic analysis placed Bim1p in the Kar9p pathway for nuclear migration. Bim1p was not required for Kar9p's cortical or spindle pole body localization. However, deletion of BIM1 eliminated Kar9p localization along cytoplasmic microtubules. Furthermore, in the bim1 mutants, the cytoplasmic microtubules no longer intersected the cortical dot of Green Fluorescent Protein-Kar9p. These experiments demonstrate that the interaction of cytoplasmic microtubules with the Kar9p cortical attachment site requires the microtubule-binding protein Bim1p. [References: 48]
机译:在酿酒酵母中,有丝分裂纺锤体的定位取决于细胞质微管与细胞皮层的相互作用。在此过程中,芽中的皮质Kar9p充当肌动蛋白与微管细胞骨架之间的链接。为了鉴定与Kar9p相互作用的蛋白,使用全长Kar9p作为诱饵进行了两次杂交筛选,并鉴定了三个基因:BIM1,STU2和KAR9本身。 STU2对主轴极体的一个组件进行编码。 Bim1p是人微管结合蛋白EB1的酵母同源物,它是与结肠癌相关的腺瘤性息肉病大肠杆菌蛋白的结合伴侣。 Bim1p第三季度中的89个氨基酸足以赋予与Kar9p的相互作用。通过使用共免疫沉淀实验证实了两种杂交的相互作用。遗传分析将Bim1p置于核迁移的Kar9p途径中。 Kar9p的皮质或纺锤体极体定位不需要Bim1p。但是,BIM1的删除消除了Kar9p沿细胞质微管的定位。此外,在bim1突变体中,胞质微管不再与绿色荧光蛋白Kar9p的皮质点相交。这些实验表明,胞质微管与Kar9p皮质附着位点的相互作用需要微管结合蛋白Bim1p。 [参考:48]

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