Human chromokinesins promote chromosome congression and spindle microtubule dynamics during mitosis

Author:

Wandke Cornelia12,Barisic Marin13,Sigl Reinhard1,Rauch Veronika1,Wolf Frank1,Amaro Ana C.1,Tan Chia H.1,Pereira Antonio J.3,Kutay Ulrike2,Maiato Helder33,Meraldi Patrick1,Geley Stephan1

Affiliation:

1. Biocenter, Division of Molecular Pathophysiology, Innsbruck Medical University, A-6020 Innsbruck, Austria

2. Institute of Biochemistry, ETH, 8093 Zurich, Switzerland

3. Chromosome Instability and Dynamics Laboratory, Institute for Molecular and Cellular Biology, and Department of Experimental Biology, Faculdade de Medicina, Universidade do Porto, 4099-002 Porto, Portugal

Abstract

Chromokinesins are microtubule plus end–directed motor proteins that bind to chromosome arms. In Xenopus egg cell-free extracts, Xkid and Xklp1 are essential for bipolar spindle formation but the functions of the human homologues, hKID (KIF22) and KIF4A, are poorly understood. By using RNAi-mediated protein knockdown in human cells, we find that only co-depletion delayed progression through mitosis in a Mad2-dependent manner. Depletion of hKID caused abnormal chromosome arm orientation, delayed chromosome congression, and sensitized cells to nocodazole. Knockdown of KIF4A increased the number and length of microtubules, altered kinetochore oscillations, and decreased kinetochore microtubule flux. These changes were associated with failures in establishing a tight metaphase plate and an increase in anaphase lagging chromosomes. Co-depletion of both chromokinesins aggravated chromosome attachment failures, which led to mitotic arrest. Thus, hKID and KIF4A contribute independently to the rapid and correct attachment of chromosomes by controlling the positioning of chromosome arms and the dynamics of microtubules, respectively.

Publisher

Rockefeller University Press

Subject

Cell Biology

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