Mps1 Dimerization and Multisite Interactions with Ndc80 Complex Enable Responsive Spindle Assembly Checkpoint Signaling

Overview

Journal J Mol Cell Biol

Publisher Oxford University Press

Specialty Molecular Biology

Date 2020 Mar 29

PMID 32219319

Citations 11

Authors

Ping Gui

Divine M Sedzro

Xiao Yuan

Sikai Liu

Mohan Hei

Wei Tian

Najdat Zohbi

Fangwei Wang

Yihan Yao

Felix O Aikhionbare

Xinjiao Gao

Dongmei Wang

Xuebiao Yao

Zhen Dou

Affiliations

Soon will be listed here.

Abstract

Error-free mitosis depends on accurate chromosome attachment to spindle microtubules, which is monitored by the spindle assembly checkpoint (SAC) signaling. As an upstream factor of SAC, the precise and dynamic kinetochore localization of Mps1 kinase is critical for initiating and silencing SAC signaling. However, the underlying molecular mechanism remains elusive. Here, we demonstrated that the multisite interactions between Mps1 and Ndc80 complex (Ndc80C) govern Mps1 kinetochore targeting. Importantly, we identified direct interaction between Mps1 tetratricopeptide repeat domain and Ndc80C. We further identified that Mps1 C-terminal fragment, which contains the protein kinase domain and C-tail, enhances Mps1 kinetochore localization. Mechanistically, Mps1 C-terminal fragment mediates its dimerization. Perturbation of C-tail attenuates the kinetochore targeting and activity of Mps1, leading to aberrant mitosis due to compromised SAC function. Taken together, our study highlights the importance of Mps1 dimerization and multisite interactions with Ndc80C in enabling responsive SAC signaling.

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