A non-canonical role of the inner kinetochore in regulating sister-chromatid cohesion at centromeres

Author:

Yan Lu,Yuan Xueying,Liu Mingjie,Chen QinfuORCID,Zhang Miao,Xu Junfen,Zeng Ling-Hui,Zhang LongORCID,Huang JunORCID,Lu WeiguoORCID,He XiaojingORCID,Yan HaiyanORCID,Wang FangweiORCID

Abstract

AbstractThe 16-subunit Constitutive Centromere-associated Network (CCAN)-based inner kinetochore is well-known for connecting centromeric chromatin to the spindle-binding outer kinetochore. Here, we report a non-canonical role for the inner kinetochore in directly regulating sister-chromatid cohesion at centromeres. We provide biochemical, X-ray crystal structure, and intracellular ectopic localization evidence that the inner kinetochore directly binds cohesin, a ring-shaped multi-subunit complex that holds sister chromatids together from S-phase until anaphase onset. This interaction is mediated by binding of the 5-subunit CENP-OPQUR sub-complex of CCAN to the Scc1-SA2 sub-complex of cohesin. Mutation in the CENP-U subunit of the CENP-OPQUR complex that abolishes its binding to the composite interface between Scc1 and SA2 weakens centromeric cohesion, leading to premature separation of sister chromatids during delayed metaphase. We further show that CENP-U competes with the cohesin release factor Wapl for binding the interface of Scc1-SA2, and that the cohesion-protecting role for CENP-U can be bypassed by depleting Wapl. Taken together, this study reveals an inner kinetochore-bound pool of cohesin, which strengthens centromeric sister-chromatid cohesion to resist metaphase spindle pulling forces.

Funder

MOST | National Natural Science Foundation of China

MOST | National Key Research and Development Program of China

MOST | NSFC | NSFC-Zhejiang Joint Fund | 浙江省科学技术厅 | Natural Science Foundation of Zhejiang Province

Newton Fund

China Postdoctoral Foundation Project | Postdoctoral Research Foundation of China

Publisher

Springer Science and Business Media LLC

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