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钙蛋白酶-1将 Rad21 裂解以促进姐妹染色单体分离。

Calpain-1 cleaves Rad21 to promote sister chromatid separation.

机构信息

Department of Pediatric Hematology/Oncology, Baylor College of Medicine, 1102 Bates Avenue, Suite 1220, Houston, TX 77030.

出版信息

Mol Cell Biol. 2011 Nov;31(21):4335-47. doi: 10.1128/MCB.06075-11. Epub 2011 Aug 29.

Abstract

Defining the mechanisms of chromosomal cohesion and dissolution of the cohesin complex from chromatids is important for understanding the chromosomal missegregation seen in many tumor cells. Here we report the identification of a novel cohesin-resolving protease and describe its role in chromosomal segregation. Sister chromatids are held together by cohesin, a multiprotein ring-like complex comprised of Rad21, Smc1, Smc3, and SA2 (or SA1). Cohesin is known to be removed from vertebrate chromosomes by two distinct mechanisms, namely, the prophase and anaphase pathways. First, PLK1-mediated phosphorylation of SA2 in prophase leads to release of cohesin from chromosome arms, leaving behind centromeric cohesins that continue to hold the sisters together. Then, at the onset of anaphase, activated separase cleaves the centromeric cohesin Rad21, thereby opening the cohesin ring and allowing the sister chromatids to separate. We report here that the calcium-dependent cysteine endopeptidase calpain-1 is a Rad21 peptidase and normally localizes to the interphase nuclei and chromatin. Calpain-1 cleaves Rad21 at L192, in a calcium-dependent manner. We further show that Rad21 cleavage by calpain-1 promotes separation of chromosome arms, which coincides with a calcium-induced partial loss of cohesin at several chromosomal loci. Engineered cleavage of Rad21 at the calpain-cleavable site without activation of calpain-1 can lead to a loss of sister chromatid cohesion. Collectively, our work reveals a novel function of calpain-1 and describes an additional pathway for sister chromatid separation in humans.

摘要

定义染色单体中黏连蛋白复合物的染色体凝聚和溶解的机制对于理解许多肿瘤细胞中观察到的染色体错误分离非常重要。在这里,我们报告了一种新型黏连蛋白解聚蛋白酶的鉴定,并描述了其在染色体分离中的作用。姐妹染色单体由黏连蛋白保持在一起,黏连蛋白是一种由 Rad21、Smc1、Smc3 和 SA2(或 SA1)组成的多蛋白环状复合物。已知黏连蛋白通过两种不同的机制从脊椎动物染色体上被去除,即前期和后期途径。首先,前期 PLK1 介导的 SA2 磷酸化导致黏连蛋白从染色体臂上释放,留下继续将姐妹染色单体保持在一起的着丝粒黏连蛋白。然后,在后期开始时,激活的 separase 切割着丝粒黏连蛋白 Rad21,从而打开黏连蛋白环,允许姐妹染色单体分离。我们在这里报告钙依赖性半胱氨酸内肽酶钙蛋白酶-1 是 Rad21 肽酶,通常定位于间期中核和染色质。钙蛋白酶-1 以钙依赖性方式在 L192 切割 Rad21。我们进一步表明,钙蛋白酶-1 切割 Rad21 促进染色体臂的分离,这与钙诱导的几个染色体位置处的黏连蛋白的部分丢失一致。在没有钙蛋白酶-1 激活的情况下,在钙蛋白酶可切割位点上构建 Rad21 的切割可导致姐妹染色单体的凝聚丧失。总之,我们的工作揭示了钙蛋白酶-1 的新功能,并描述了人类姐妹染色单体分离的另一种途径。

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