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生存素与着丝粒内蛋白 INCENP 显示出相似的细胞周期定位和基因敲除表型。

Survivin and the inner centromere protein INCENP show similar cell-cycle localization and gene knockout phenotype.

作者信息

Uren A G, Wong L, Pakusch M, Fowler K J, Burrows F J, Vaux D L, Choo K H

机构信息

The Walter and Eliza Hall Institute of Medical Research, Post Office Royal Melbourne Hospital, 3050,., Victoria, Australia.

出版信息

Curr Biol. 2000 Nov 2;10(21):1319-28. doi: 10.1016/s0960-9822(00)00769-7.

Abstract

BACKGROUND

Survivin is a mammalian protein that carries a motif typical of the inhibitor of apoptosis (IAP)proteins, first identified in baculoviruses. Although baculoviral IAP proteins regulate cell death, the yeast Survivin homolog Bir1 is involved in cell division. To determine the function of Survivin in mammals, we analyzed the pattern of localization of Survivin protein during the cell cycle, and deleted its gene by homologous recombination in mice.

RESULTS

In human cells, Survivin appeared first on centromeres bound to a novel para-polar axis during prophase/metaphase, relocated to the spindle midzone during anaphase/telophase, and disappeared at the end of telophase. In the mouse, Survivin was required for mitosis during development. Null embryos showed disrupted microtubule formation, became polyploid, and failed to survive beyond 4.5days post coitum. This phenotype, and the cell-cycle localization of Survivin, resembled closely those of INCENP. Because the yeast homolog of INCENP, Sli15, regulates the Aurora kinase homolog Ipl1p, and the yeast Survivin homolog Bir1 binds to Ndc10p, a substrate of Ipl1p, yeast Survivin, INCENP and Aurora homologs function in concert during cell division.

CONCLUSIONS

In vertebrates, Survivin and INCENP have related roles in mitosis, coordinating events such as microtubule organization, cleavage-furrow formation and cytokinesis. Like their yeast homologs Bir1 and Sli15, they may also act together with the Aurora kinase.

摘要

背景

生存素是一种哺乳动物蛋白,带有凋亡抑制蛋白(IAP)典型的基序,最初在杆状病毒中被鉴定出来。尽管杆状病毒IAP蛋白调节细胞死亡,但酵母生存素同源物Bir1参与细胞分裂。为了确定生存素在哺乳动物中的功能,我们分析了细胞周期中生存素蛋白的定位模式,并通过小鼠同源重组删除了其基因。

结果

在人类细胞中,生存素在前期/中期首先出现在与一个新的副极轴结合的着丝粒上,在后期/末期重新定位到纺锤体中间区,并在末期结束时消失。在小鼠中,发育过程中的有丝分裂需要生存素。缺失生存素的胚胎显示微管形成紊乱,变成多倍体,并且在合子后4.5天内无法存活。这种表型以及生存素在细胞周期中的定位与染色体乘客蛋白(INCENP)的非常相似。因为INCENP的酵母同源物Sli15调节极光激酶同源物Ipl1p,并且酵母生存素同源物Bir1与Ipl1p的底物Ndc10p结合,所以酵母生存素、INCENP和极光同源物在细胞分裂过程中协同发挥作用。

结论

在脊椎动物中,生存素和INCENP在有丝分裂中具有相关作用,协调微管组织、分裂沟形成和胞质分裂等事件。与它们的酵母同源物Bir1和Sli15一样,它们也可能与极光激酶一起发挥作用。

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