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The Constitutive Centromere Component CENP-50 Is Required for Recovery from Spindle Damage

机译:从主轴损坏中恢复时需要本构着丝粒成分CENP-50

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摘要

We identified CENP-50 as a novel kinetochore component. We found that CENP-50 is a constitutive component of the centromere that colocalizes with CENP-A and CENP-H throughout the cell cycle in vertebrate cells. To determine the precise role of CENP-50, we examined its role in centromere function by generating a loss-of-function mutant in the chicken DT40 cell line. The CENP-50 knockout was not lethal; however, the growth rate of cells with this mutation was slower than that of wild-type cells. We observed that the time for CENP-50-deficient cells to complete mitosis was longer than that for wild-type cells. Centromeric localization of CENP-50 was abolished in both CENP-H- and CENP-I-deficient cells. Coimmunoprecipitation experiments revealed that CENP-50 interacted with the CENP-H/CENP-I complex in chicken DT40 cells. We also observed severe mitotic defects in CENP-50-deficient cells with apparent premature sister chromatid separation when the mitotic checkpoint was activated, indicating that CENP-50 is required for recovery from spindle damage.
机译:我们确定CENP-50是一种新型的动粒体成分。我们发现CENP-50是着丝粒的组成成分,在脊椎动物细胞的整个细胞周期中,CENP-50与CENP-A和CENP-H共定位。为了确定CENP-50的确切作用,我们通过在鸡DT40细胞系中产生功能丧失突变体来检查其在着丝粒功能中的作用。 CENP-50敲除并不致命。然而,具有这种突变的细胞的生长速度比野生型细胞慢。我们观察到,CENP-50缺陷细胞完成有丝分裂的时间比野生型细胞更长。 CENP-50的着丝粒定位在CENP-H和CENP-1缺陷细胞中均被取消。免疫沉淀实验表明,CENP-50与鸡DT40细胞中的CENP-H / CENP-1复合物相互作用。当激活有丝分裂检查点时,我们还观察到CENP-50缺陷型细胞中出现严重的有丝分裂缺陷,明显出现过早的姐妹染色单体分离,表明从纺锤体损伤中恢复需要CENP-50。

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