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Cdc42 GTPase-activating proteins (GAPs) regulate generational inheritance of cell polarity and cell shape in fission yeast
Authors:Marbelys Rodriguez Pino  Illyce Nuez  Chuan Chen  Maitreyi E Das  David J Wiley  Gennaro D&#x;Urso  Peter Buchwald  Dimitrios Vavylonis  Fulvia Verde
Institution:University of Lausanne;aDepartment of Molecular and Cellular Pharmacology, University of Miami Miller School of Medicine, Miami, FL 33101-1015;bDepartment of Biology, Health & Wellness, Miami Dade College, Miami, FL 33176;cDepartment of Biochemistry and Cellular and Molecular Biology, University of Tennessee, Knoxville, TN 37996;dDepartment of Physics, Lehigh University, 16 Memorial Drive East, Bethlehem, PA, 18015
Abstract:The highly conserved small GTPase Cdc42 regulates polarized cell growth and morphogenesis from yeast to humans. We previously reported that Cdc42 activation exhibits oscillatory dynamics at cell tips of Schizosaccharomyces pombe cells. Mathematical modeling suggests that this dynamic behavior enables a variety of symmetric and asymmetric Cdc42 activation distributions to coexist in cell populations. For individual wild-type cells, however, Cdc42 distribution is initially asymmetrical and becomes more symmetrical as cell volume increases, enabling bipolar growth activation. To explore whether different patterns of Cdc42 activation are possible in vivo, we examined S. pombe rga4∆ mutant cells, lacking the Cdc42 GTPase-activating protein (GAP) Rga4. We found that monopolar rga4∆ mother cells divide asymmetrically leading to the emergence of both symmetric and asymmetric Cdc42 distributions in rga4∆ daughter cells. Motivated by different hypotheses that can mathematically reproduce the unequal fate of daughter cells, we used genetic screening to identify mutants that alter the rga4∆ phenotype. We found that the unequal distribution of active Cdc42 GTPase is consistent with an unequal inheritance of another Cdc42 GAP, Rga6, in the two daughter cells. Our findings highlight the crucial role of Cdc42 GAP localization in maintaining consistent Cdc42 activation and growth patterns across generations.
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