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人侵袭增强因子簇,一种有丝分裂通过所需的卷曲螺旋蛋白。

Human enhancer of invasion-cluster, a coiled-coil protein required for passage through mitosis.

作者信息

Einarson Margret B, Cukierman Edna, Compton Duane A, Golemis Erica A

机构信息

Division of Basic Science, Fox Chase Cancer Center, Philadelphia, Pennsylvania 19111, USA.

出版信息

Mol Cell Biol. 2004 May;24(9):3957-71. doi: 10.1128/MCB.24.9.3957-3971.2004.

DOI:10.1128/MCB.24.9.3957-3971.2004
PMID:15082789
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC387757/
Abstract

In a cross-species overexpression approach, we used the pseudohyphal transition of Saccharomyces cerevisiae as a model screening system to identify human genes that regulate cell morphology and the cell cycle. Human enhancer of invasion-cluster (HEI-C), encoding a novel evolutionarily conserved coiled-coil protein, was isolated in a screen for human genes that induce agar invasion in S. cerevisiae. In human cells, HEI-C is primarily localized to the spindle during mitosis. Depletion of HEI-C in vivo with short interfering RNAs results in severe mitotic defects. Analysis by immunofluorescence, flow cytometry analysis, and videomicroscopy indicates that HEI-C-depleted cells form metaphase plates with normal timing after G(2)/M transition, although in many cases cells have disorganized mitotic spindles. Subsequently, severe defects occur at the metaphase-anaphase transition, characterized by a significant delay at this stage or, more commonly, cellular disintegration accompanied by the display of classic biochemical markers of apoptosis. These mitotic defects occur in spite of the fact that HEI-C-depleted cells retain functional cell cycle checkpoints, as these cells arrest normally following nocodazole or hydroxyurea treatment. These results place HEI-C as a novel regulator of spindle function and integrity during the metaphase-anaphase transition.

摘要

在一种跨物种过表达方法中,我们使用酿酒酵母的假菌丝转变作为模型筛选系统,以鉴定调控细胞形态和细胞周期的人类基因。侵袭簇人类增强子(HEI-C)编码一种新型的进化保守的卷曲螺旋蛋白,它是在筛选诱导酿酒酵母琼脂侵袭的人类基因时分离得到的。在人类细胞中,HEI-C在有丝分裂期间主要定位于纺锤体。用小干扰RNA在体内耗尽HEI-C会导致严重的有丝分裂缺陷。免疫荧光分析、流式细胞术分析和视频显微镜观察表明,耗尽HEI-C的细胞在G(2)/M转变后能正常时间形成中期板,尽管在许多情况下细胞的有丝分裂纺锤体紊乱。随后,在中期-后期转变时出现严重缺陷,其特征是在这个阶段显著延迟,或者更常见的是细胞解体并伴有典型的凋亡生化标志物表现。尽管耗尽HEI-C的细胞保留了功能性的细胞周期检查点,因为这些细胞在用诺考达唑或羟基脲处理后能正常停滞,但仍会出现这些有丝分裂缺陷。这些结果表明HEI-C是中期-后期转变期间纺锤体功能和完整性的新型调节因子。

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本文引用的文献

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Securin and B-cyclin/CDK are the only essential targets of the APC.分裂后期促进复合物的唯一重要靶点是securin和B型细胞周期蛋白/细胞周期蛋白依赖性激酶。
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The mitotic checkpoint: a signaling pathway that allows a single unattached kinetochore to inhibit mitotic exit.有丝分裂检查点:一种信号通路,允许单个未附着的动粒抑制有丝分裂退出。
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