4.4 Article

Ste20-related protein kinase LOSK (SLK) controls microtubule radial array in interphase

Journal

MOLECULAR BIOLOGY OF THE CELL
Volume 19, Issue 5, Pages 1952-1961

Publisher

AMER SOC CELL BIOLOGY
DOI: 10.1091/mbc.E06-12-1156

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Funding

  1. Program of the Presidium of Russian Academy of Science
  2. Russian Foundation for Basic Research [02-04-48783, 05-04-49015]
  3. German DAAD Leonhard-Euler-Program

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Interphase microtubules are organized into a radial array with centrosome in the center. This organization is a subject of cellular regulation that can be driven by protein phosphorylation. Only few protein kinases that regulate microtubule array in interphase cells have been described. Ste20-like protein kinase LOSK (SLK) was identified as a microtubule and centrosome-associated protein. In this study we have shown that the inhibition of LOSK activity by dominant-negative mutant K63R-Delta T or by LOSK depletion with RNAi leads to unfocused microtubule arrangement. Microtubule disorganization is prominent in Vero, CV-1, and CHO-K1 cells but less distinct in HeLa cells. The effect is a result neither of microtubule stabilization nor of centrosome disruption. In cells with suppressed LOSK activity centrosomes are unable to anchor or to cap microtubules, though they keep nucleating microtubules. These centrosomes are depleted of dynactin. Vero cells overexpressing K63R-Delta T have normal dynactin comets at microtubule ends and unaltered morphology of Golgi complex but are unable to polarize it at the wound edge. We conclude that protein kinase LOSK is required for radial microtubule organization and for the proper localization of Golgi complex in various cell types.

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