The fission yeast NDR kinase Orb6 and its signalling pathway MOR regulate cytoplasmic microtubule organization during the cell cycle

Author:

Kume Kazunori12ORCID,Nishikawa Kenji1,Furuyama Rikuto1,Fujimoto Takahiro1,Koyano Takayuki3,Matsuyama Makoto4,Mizunuma Masaki12,Hirata Dai56

Affiliation:

1. Graduate School of Integrated Sciences for Life, Hiroshima University, 1-3-1 Kagamiyama, Higashi-Hiroshima, Hiroshima 739-8530, Japan

2. Hiroshima Research Center for Healthy Aging (HiHA), Hiroshima University, Higashi-Hiroshima, Hiroshima 739-8530, Japan

3. Division of Cell Biology, Shigei Medical Research Institute, 2117 Yamada, Minami-ku, Okayama 701-0202, Japan

4. Division of Molecular Genetics, Shigei Medical Research Institute, 2117 Yamada, Minami-ku, Okayama 701-0202, Japan

5. Faculty of Agriculture, Niigata University, 2-8050 Ikarashi, Niigata 950-2181, Japan

6. Sakeology Center, Niigata University, 2-8050 Ikarashi, Niigata 950-2181, Japan

Abstract

Microtubule organization and reorganization during the cell cycle are achieved by regulation of the number, distribution and activity of microtubule-organizing centres (MTOCs). In fission yeast, the Mto1/2 complex determines the activity and distribution of cytoplasmic MTOCs. Upon mitosis, cytoplasmic microtubule nucleation ceases; inactivation of the Mto1/2 complex is triggered by Mto2 hyperphosphorylation. However, the protein kinase(s) that phosphorylates Mto2 remains elusive. Here we show that a conserved signalling network, called MOR (morphogenesis Orb6 network) in fission yeast, negatively regulates cytoplasmic MTOCs through Mto2 phosphorylation to ensure proper microtubule organization. Inactivation of Orb6 kinase, the most downstream MOR component, by attenuation of MOR signalling leads to reduced Mto2 phosphorylation, coincident with increased number of both Mto2 puncta and cytoplasmic microtubules. These defects cause the emergence of uncoordinated mitotic cells with cytoplasmic microtubules, resulting in reduced spindle assembly. Thus, the regulation of Mto2 by the MOR is crucial for cytoplasmic microtubule organization and contributes to reorganization of the microtubule cytoskeletons during the cell cycle.

Funder

Japan Society for the Promotion of Science

The Institute for Fermentation, Osaka

Publisher

The Royal Society

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