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首页> 外文期刊>Cell cycle >Human ninein is a centrosomal autoantigen recognized by CREST patient sera and plays a regulatory role in microtubule nucleation.
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Human ninein is a centrosomal autoantigen recognized by CREST patient sera and plays a regulatory role in microtubule nucleation.

机译:人丁质蛋白是一种CREST患者血清识别的中心体自身抗原,在微管成核中起调节作用。

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摘要

Centrosome is the major microtubule organizing center in mammalian cells that plays a critical role in a variety of cellular events by the microtubule arrays emanating from it. Despite its significance, the molecular mechanisms underlying the structure and function of the centrosome are still not clear. Herein we describe the identification of three isotypes of human ninein by expression library screening with autoimmune sera from CREST patients. All three ninein isotypes exhibit centrosomal localization throughout the cell cycle when GFP-tagged fusion proteins are expressed transiently in mammalian cells. Construction of serial deletions of GFP-tagged ninein reveals that a stretch of three leucine zippers with a flanking sequence is required and sufficient for centrosomal targeting. Overexpression of ninein results in mislocalization of gamma-tubulin, recruiting it to ectopic (noncentrosomal) ninein-containing sites which are not active in nucleating microtubules. In these cells, nucleation of microtubules from the centrosome is also inhibited. These results thus suggest a regulatory role for ninein in microtubule nucleation.
机译:中心体是哺乳动物细胞中的主要微管组织中心,它通过发出的微管阵列在各种细胞事件中起关键作用。尽管其重要性,中心体的结构和功能的分子机制仍不清楚。在本文中,我们描述了通过用来自CREST患者的自身免疫血清进行表达文库筛选来鉴定人九蛋白的三种同种型。当GFP标记的融合蛋白在哺乳动物细胞中瞬时表达时,所有三个九蛋白同种型在整个细胞周期中均表现出中心体定位。带有GFP标记的ninein的系列缺失的构建显示,需要一条带有侧翼序列的三个亮氨酸拉链,并且足以用于中心体靶向。九蛋白的过度表达导致γ-微管蛋白的定位错误,将其募集到异位的(非中心体)含九蛋白的位点,该位点在微管的成核中没有活性。在这些细胞中,来自中心体的微管成核也受到抑制。因此,这些结果表明了九蛋白在微管成核中的调节作用。

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