粘蛋白
着丝粒
姐妹染色单体结合力的建立
染色体分离
动细胞
细胞生物学
有丝分裂
生物
CTCF公司
染色单体
主轴装置
微管
遗传学
染色体
细胞分裂
细胞
转录因子
基因
增强子
作者
Alberto García-Nieto,Amrita Patel,Yan Li,Roel Oldenkamp,Leonardo Feletto,Joshua J. Graham,Laureen Willems,Kyle Muir,Daniel Panne,Benjamin D. Rowland
标识
DOI:10.1038/s41594-023-00968-y
摘要
In the early stages of mitosis, cohesin is released from chromosome arms but not from centromeres. The protection of centromeric cohesin by SGO1 maintains the sister chromatid cohesion that resists the pulling forces of microtubules until all chromosomes are attached in a bipolar manner to the mitotic spindle. Here we present the X-ray crystal structure of a segment of human SGO1 bound to a conserved surface of the cohesin complex. SGO1 binds to a composite interface formed by the SA2 and SCC1RAD21 subunits of cohesin. SGO1 shares this binding interface with CTCF, indicating that these distinct chromosomal regulators control cohesin through a universal principle. This interaction is essential for the localization of SGO1 to centromeres and protects centromeric cohesin against WAPL-mediated cohesin release. SGO1-cohesin binding is maintained until the formation of microtubule-kinetochore attachments and is required for faithful chromosome segregation and the maintenance of a stable karyotype.
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