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Regulation of Cell Polarity by Interactions of Msb3 and Msb4 with Cdc42 and Polarisome Components

机译:通过Msb3和Msb4与Cdc42和极性小体相互作用的细胞极性调节。

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摘要

In Saccharomyces cerevisiae, polarized growth depends on interactions between the actin cytoskeleton and the secretory machinery. Here we show that the Rab GTPase-activating proteins (GAPs) Msb3 and Msb4 interact directly with Spa2, a scaffold protein of the “polarisome” that also interacts with the formin Bni1. Spa2 is required for the polarized localization of Msb3 and Msb4 at the bud tip. We also show that Msb3 and Msb4 bind specifically to Cdc42-GDP and Rho1-GDP in vitro and that Msb3 and Rho GDP dissociation inhibitor act independently but oppositely on Cdc42. Finally, we show that Msb3 and Msb4 are involved in Bni1-nucleated actin assembly in vivo. These results suggest that Msb3 and Msb4 regulate polarized growth by multiple mechanisms, directly regulating exocytosis through their GAP activity toward Sec4 and potentially coordinating the functions of Cdc42, Rho1, and Bni1 in the polarisome through their binding to these GTPases. A functional equivalent of the polarisome probably exists in other fungi and mammals.
机译:在酿酒酵母中,极化生长取决于肌动蛋白细胞骨架与分泌机制之间的相互作用。在这里,我们显示了Rab GTPase激活蛋白(GAP)Msb3和Msb4与Spa2直接相互作用,Spa2是“极化体”的支架蛋白,也与福尔明Bni1相互作用。 Spa2是芽尖端Msb3和Msb4极化定位所必需的。我们还显示,Msb3和Msb4在体外与Cdc42-GDP和Rho1-GDP特异性结合,并且Msb3和Rho GDP离解抑制剂对Cdc42的独立作用相反。最后,我们显示Msb3和Msb4参与体内Bni1核化的肌动蛋白组装。这些结果表明,Msb3和Msb4通过多种机制调节极化生长,通过它们对Sec4的GAP活性直接调节胞吐作用,并可能通过与这些GTPases结合来协调Cdc42,Rho1和Bni1在极化体中的功能。极性体的功能等同物可能存在于其他真菌和哺乳动物中。

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