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PASK (proline-alanine-rich Ste20-related kinase) binds to tubulin and microtubules and is involved in microtubule stabilization
Authors:Tsutsumi Tomonari  Kosaka Takamitsu  Ushiro Hiroshi  Kimura Kazushi  Honda Tomoyuki  Kayahara Tetsuro  Mizoguchi Akira
Affiliation:aDepartment of Neural Regeneration and Cell Communication, Mie University Graduate School of Medicine, Tsu, Mie 514-8507, Japan;bDepartment of Food and Nutrition, Tsu City College, 157 Ishinden-Nakano, Tsu, Mie 514-0112, Japan;cFaculty of Rehabilitation, Kobe Gakuin University, 518 Arise Ikawadani-cho, Nishi-ku, Kobe, 651-2180, Japan
Abstract:
Proline–alanine-rich Ste20-related kinase (PASK, also referred to as SPAK) has been linked to ion transport regulation. Here, we report two novel activities of PASK: binding to tubulin and microtubules and the promotion of microtubule assembly. Tubulin binding assay showed that full-length PASK and its kinase domain bound to purified tubulin whereas the N-terminal or C-terminal non-catalytic domains of PASK did not. The full-length PASK and its kinase domain were sedimented with paclitaxel-stabilized microtubules by ultracentrifugation. These results indicate that the kinase domain of PASK can interact directly with both microtubules and soluble tubulin in vitro. Truncated PASK lacking the N-terminal non-catalytic domain promoted microtubule assembly at a subcritical concentration of purified tubulin. FLAG–PASK expressed in COS-7 cells translocated to the cytoskeleton when the cells were stimulated with hypertonic sodium chloride, and stabilized microtubules against depolymerization by nocodazole. Our findings suggest that PASK may regulate the cytoskeleton by modulating microtubule stability.
Keywords:Hyperosmotic stress   Microtubule   Microtubule-associated protein   Proline–  alanine-rich Ste20-related kinase (PASK)   Protein kinase   Ste20-related proline–  alanine-rich kinase (SPAK)
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