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RED 是一个纺锤体极相关蛋白,对于 MAD1 向动粒的定位、有丝分裂的进行以及纺锤体组装检查点的激活是必需的。

RED, a spindle pole-associated protein, is required for kinetochore localization of MAD1, mitotic progression, and activation of the spindle assembly checkpoint.

机构信息

Institute of Medical Sciences, Tzu-Chi University, Hualien 97004, Taiwan.

出版信息

J Biol Chem. 2012 Apr 6;287(15):11704-16. doi: 10.1074/jbc.M111.299131. Epub 2012 Feb 18.

Abstract

The spindle assembly checkpoint (SAC) is essential for ensuring the proper attachment of kinetochores to the spindle and, thus, the precise separation of paired sister chromatids during mitosis. The SAC proteins are recruited to the unattached kinetochores for activation of the SAC in prometaphase. However, it has been less studied whether activation of the SAC also requires the proteins that do not localize to the kinetochores. Here, we show that the nuclear protein RED, also called IK, a down-regulator of human leukocyte antigen (HLA) II, interacts with the human SAC protein MAD1. Two RED-interacting regions identified in MAD1 are from amino acid residues 301-340 and 439-480, designated as MAD1(301-340) and MAD1(439-480), respectively. Our observations reveal that RED is a spindle pole-associated protein that colocalizes with MAD1 at the spindle poles in metaphase and anaphase. Depletion of RED can cause a shorter mitotic timing, a failure in the kinetochore localization of MAD1 in prometaphase, and a defect in the SAC. Furthermore, the RED-interacting peptides MAD1(301-340) and MAD1(439-480), fused to enhanced green fluorescence protein, can colocalize with RED at the spindle poles in prometaphase, and their expression can abrogate the SAC. Taken together, we conclude that RED is required for kinetochore localization of MAD1, mitotic progression, and activation of the SAC.

摘要

纺锤体组装检查点 (SAC) 对于确保动粒正确附着在纺锤体上,从而在有丝分裂过程中精确分离配对的姐妹染色单体至关重要。SAC 蛋白被募集到未附着的动粒上,以在前期激活 SAC。然而,对于激活 SAC 是否也需要不定位在动粒上的蛋白质,研究较少。在这里,我们表明核蛋白 RED(也称为 IK),一种人类白细胞抗原 (HLA) II 的下调因子,与人类 SAC 蛋白 MAD1 相互作用。在 MAD1 中鉴定的两个 RED 相互作用区域位于氨基酸残基 301-340 和 439-480 处,分别命名为 MAD1(301-340)和 MAD1(439-480)。我们的观察结果表明,RED 是一种纺锤体极相关蛋白,在中期和后期与 MAD1 共定位于纺锤体极。RED 的耗竭会导致有丝分裂时间缩短、前期 MAD1 动粒定位失败以及 SAC 缺陷。此外,与增强型绿色荧光蛋白融合的 RED 相互作用肽 MAD1(301-340)和 MAD1(439-480)可以在前期与 RED 共定位于纺锤体极,并且它们的表达可以消除 SAC。总之,我们得出结论,RED 对于 MAD1 的动粒定位、有丝分裂进展和 SAC 的激活是必需的。

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