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The APC-associated protein EB1 associates with components of the dynactin complex and cytoplasmic dynein intermediate chain

机译:APC相关蛋白EB1与Dynactin复合物和细胞质Dynein中间链的成分结合

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摘要

Human EB1 is a highly conserved protein that binds to the carboxyl terminus of the human adenomatous polyposis coil (APC) tumor suppressor protein, a domain of APC that is commonly deleted in colorectal neoplasia. EB1 belongs to a family of microtubule-associated proteins that includes Schizosaccharomyces pombe Mal3 and Saccharomyces cerevisiae Bim1p. Bim1p appears to regulate the timing of cytokinesis as demonstrated by a genetic interaction with Act5, a component of the yeast dynactin complex. Whereas the predominant function of the dynactin complex in yeast appears to be in positioning the mitotic spindle, in animal cells, dynactin has been shown to function in diverse processes, including organelle transport, formation of the mitotic spindle, and perhaps cytokinesis. Here, we demonstrate that human EB1 can be coprecipitated with p150 super(Glued), a member of the dynactin protein complex. EB1 was also found associated with the intermediate chain of cytoplasmic dynein (CDIC) and with dynamitin (p50), another component of the dynactin complex, but not with dynein heavy chain, in a complex that sedimented at approximately 5S in a sucrose density gradient. The association of EB1 with members of the dynactin complex was independent of APC and was preserved in the absence of an intact microtubule cytoskeleton. The molecular interaction of EB1 with members of the dynactin complex and with CDIC may be important for microtubule-based processes.
机译:人EB1是高度保守的蛋白,可与人腺瘤性息肉病(APC)肿瘤抑制蛋白的羧基末端结合,后者是APC的结构域,通常在结直肠肿瘤中被删除。 EB1属于微管相关蛋白家族,包括粟酒裂殖酵母Mal3和酿酒酵母Bim1p。 Bim1p似乎可以调节胞质分裂的时机,这是通过与Act5(酵母Dynactin复合物的组成部分)之间的遗传相互作用来证明的。尽管酵母中dynactin复合物的主要功能似乎是定位有丝分裂纺锤体,但在动物细胞中,dynactin已显示出在多种过程中起作用的功能,包括细胞器运输,有丝分裂纺锤体的形成以及胞质分裂。在这里,我们证明了人类EB1可以与D150 dynactin蛋白复合物的成员p150 super(Glued)共沉淀。还发现EB1与细胞质动力蛋白(CDIC)的中间链和动力蛋白(p50)(动力蛋白复合物的另一种成分)相关联,但与动力蛋白重链不相关,该复合物在大约5S的蔗糖密度梯度下沉淀。 EB1与动力蛋白复合物成员之间的关联独立于APC,并且在没有完整的微管细胞骨架的情况下得以保留。 EB1与动力蛋白复合物成员以及CDIC的分子相互作用对于基于微管的过程可能很重要。

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