A mitotic kinesin-6, Pav-KLP, mediates interdependent cortical reorganization and spindle dynamics inDrosophilaembryos

Author:

Sommi Patrizia1,Ananthakrishnan Revathi1,Cheerambathur Dhanya K.1,Kwon Mijung1,Morales-Mulia Sandra1,Brust-Mascher Ingrid12,Mogilner Alex3

Affiliation:

1. LCCB, Center for Genetics and Development, University of California at Davis, Davis, CA 95616, USA

2. Department of Molecular and Cellular Biology, University of California at Davis, Davis, CA 95616, USA

3. Department of Neurobiology, Physiology and Behavior and Department of Mathematics, University of California at Davis, Davis, CA 95616, USA

Abstract

We investigated the role of Pav-KLP, a kinesin-6, in the coordination of spindle and cortical dynamics during mitosis in Drosophila embryos. In vitro, Pav-KLP behaves as a dimer. In vivo, it localizes to mitotic spindles and furrows. Inhibition of Pav-KLP causes defects in both spindle dynamics and furrow ingression, as well as causing changes in the distribution of actin and vesicles. Thus, Pav-KLP stabilizes the spindle by crosslinking interpolar microtubule bundles and contributes to actin furrow formation possibly by transporting membrane vesicles, actin and/or actin regulatory molecules along astral microtubules. Modeling suggests that furrow ingression during cellularization depends on: (1) a Pav-KLP-dependent force driving an initial slow stage of ingression; and (2) the subsequent Pav-KLP-driven transport of actin- and membrane-containing vesicles to the furrow during a fast stage of ingression. We hypothesize that Pav-KLP is a multifunctional mitotic motor that contributes both to bundling of interpolar microtubules, thus stabilizing the spindle, and to a biphasic mechanism of furrow ingression by pulling down the furrow and transporting vesicles that deliver new material to the descending furrow.

Publisher

The Company of Biologists

Subject

Cell Biology

Reference60 articles.

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