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CENP-E kinesin interacts with SKAP protein to orchestrate accurate chromosome segregation in mitosis
Authors:Huang Yuejia  Wang Wenwen  Yao Phil  Wang Xiwei  Liu Xing  Zhuang Xiaoxuan  Yan Feng  Zhou Jinhua  Du Jian  Ward Tarsha  Zou Hanfa  Zhang Jiancun  Fang Guowei  Ding Xia  Dou Zhen  Yao Xuebiao
Affiliation:Anhui Key Laboratory of Cellular Dynamics and Chemical Biology, University of Science and Technology of China School of Life Sciences, Hefei 230027, China.
Abstract:
Mitotic chromosome segregation is orchestrated by the dynamic interaction of spindle microtubules with the kinetochore. Although previous studies show that the mitotic kinesin CENP-E forms a link between attachment of the spindle microtubule to the kinetochore and the mitotic checkpoint signaling cascade, the molecular mechanism underlying dynamic kinetochore-microtubule interactions in mammalian cells remains elusive. Here, we identify a novel interaction between CENP-E and SKAP that functions synergistically in governing dynamic kinetochore-microtubule interactions. SKAP binds to the C-terminal tail of CENP-E in vitro and is essential for an accurate kinetochore-microtubule attachment in vivo. Immunoelectron microscopic analysis indicates that SKAP is a constituent of the kinetochore corona fibers of mammalian centromeres. Depletion of SKAP or CENP-E by RNA interference results in a dramatic reduction of inter-kinetochore tension, which causes chromosome mis-segregation with a prolonged delay in achieving metaphase alignment. Importantly, SKAP binds to microtubules in vitro, and this interaction is synergized by CENP-E. Based on these findings, we propose that SKAP cooperates with CENP-E to orchestrate dynamic kinetochore-microtubule interaction for faithful chromosome segregation.
Keywords:Centromeres   Checkpoint Control   Kinetochore   Mass Spectrometry (MS)   Tubulin   CENP-E   SKAP   Chromosome Alignment   Chromosome Dynamics   Syntelin
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