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Ndc80 动粒复合物直接调节微管动力学。

The Ndc80 kinetochore complex directly modulates microtubule dynamics.

机构信息

Department of Biochemistry, Department of Physiology and Biophysics, Howard Hughes Medical Institute, University of Washington, Seattle, WA 98195, USA.

出版信息

Proc Natl Acad Sci U S A. 2012 Oct 2;109(40):16113-8. doi: 10.1073/pnas.1209615109. Epub 2012 Aug 20.

Abstract

The conserved Ndc80 complex is an essential microtubule-binding component of the kinetochore. Recent findings suggest that the Ndc80 complex influences microtubule dynamics at kinetochores in vivo. However, it was unclear if the Ndc80 complex mediates these effects directly, or by affecting other factors localized at the kinetochore. Using a reconstituted system in vitro, we show that the human Ndc80 complex directly stabilizes the tips of disassembling microtubules and promotes rescue (the transition from microtubule shortening to growth). In vivo, an N-terminal domain in the Ndc80 complex is phosphorylated by the Aurora B kinase. Mutations that mimic phosphorylation of the Ndc80 complex prevent stable kinetochore-microtubule attachment, and mutations that block phosphorylation damp kinetochore oscillations. We find that the Ndc80 complex with Aurora B phosphomimetic mutations is defective at promoting microtubule rescue, even when robustly coupled to disassembling microtubule tips. This impaired ability to affect dynamics is not simply because of weakened microtubule binding, as an N-terminally truncated complex with similar binding affinity is able to promote rescue. Taken together, these results suggest that in addition to regulating attachment stability, Aurora B controls microtubule dynamics through phosphorylation of the Ndc80 complex.

摘要

保守的 Ndc80 复合物是动粒的必需微管结合成分。最近的研究结果表明,Ndc80 复合物在体内影响动粒处的微管动力学。然而,尚不清楚 Ndc80 复合物是通过直接影响动粒上的其他因素,还是通过直接影响这些作用来介导这些影响。我们使用体外重建的系统表明,人 Ndc80 复合物直接稳定正在解聚的微管的尖端并促进恢复(从微管缩短到生长的转变)。在体内,动粒处的 Aurora B 激酶会使 Ndc80 复合物的 N 端结构域发生磷酸化。模拟 Ndc80 复合物磷酸化的突变会阻止稳定的动粒-微管附着,而阻止磷酸化的突变会抑制动粒的振荡。我们发现,即使与正在解聚的微管尖端强烈偶联,具有 Aurora B 磷酸化模拟突变的 Ndc80 复合物在促进微管恢复方面存在缺陷。这种影响动力学的能力受损并不仅仅是因为微管结合减弱,因为具有相似结合亲和力的 N 端截断复合物能够促进恢复。总之,这些结果表明,除了调节附着稳定性外,Aurora B 还通过磷酸化 Ndc80 复合物来控制微管动力学。

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