Mitotic Down-regulation of p190RhoGAP Is Required for the Successful Completion of Cytokinesis |
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| Authors: | Sergio A. Sánchez Manchinelly Joyce Agati Miller Ling Su Tsuyoshi Miyake Lisa Palmer Masahito Mikawa Sarah J. Parsons |
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| Affiliation: | From the ‡Department of Microbiology and Cancer Center and ;the §Department of Pediatrics, University of Virginia, Charlottesville, Virginia 22908 |
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| Abstract: | p190RhoGAP-A (p190) is a GTPase-activating protein known to regulate actin cytoskeleton dynamics by decreasing RhoGTP levels through activation of Rho intrinsic GTPase activity. We have previously shown that p190 protein levels are cell cycle-regulated, decreasing in mitosis, and that this decrease is mediated by the ubiquitin-proteasome pathway. In addition, overexpression of p190 results in decreased RhoGTP levels at the cleavage furrow during cytokinesis, p190 and the RhoGEF Ect2 play opposing roles in cytokinesis, and sustained levels of p190 in mitosis are associated with cytokinesis failure, all findings that suggest but do not directly demonstrate that completion of cytokinesis is dependent on reduced levels of p190. Here we report, using an RNAi reconstitution approach with a degradation-resistant mutant, that decreased p190 levels are required for successful cytokinesis. We also show that the multinucleation phenotype is dependent on p190 RhoGAP activity, determine that the N-terminal GBDS1 region is necessary and sufficient for p190 mitotic ubiquitination and degradation, and identify four N-terminal residues as necessary for the degradation of p190 in mitosis. Our data indicate that in addition to activation of RhoGEF(s), reduction of RhoGAP (p190) is a critical mechanism by which increased RhoGTP levels are achieved in late mitosis, thereby ensuring proper cell division. |
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| Keywords: | Cell Division Microscopic Imaging Mitosis Rho Ubiquitination Cytokinesis Degradation Multinucleation p190RhoGAP |
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