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Rho1- and Pkc1-dependent phosphorylation of the F-BAR protein Syp1 contributes to septin ring assembly

机译:F-BAR蛋白Syp1的Rho1-和Pkc1依赖性磷酸化有助于Septin环组装

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摘要

In many cell types, septins assemble into filaments and rings at the neck of cellular appendages and/or at the cleavage furrow to help compartmentalize the plasma membrane and support cytokinesis. How septin ring assembly is coordinated with membrane remodeling and controlled by mechanical stress at these sites is unclear. Through a genetic screen, we uncovered an unanticipated link between the conserved Rho1 GTPase and its effector protein kinase C (Pkc1) with septin ring stability in yeast. Both Rho1 and Pkc1 stabilize the septin ring, at least partly through phosphorylation of the membrane-associated F-BAR protein Syp1, which colocalizes asymmetrically with the septin ring at the bud neck. Syp1 is displaced from the bud neck upon Pkc1-dependent phosphorylation at two serines, thereby affecting the rigidity of the new-forming septin ring. We propose that Rho1 and Pkc1 coordinate septin ring assembly with membrane and cell wall remodeling partly by controlling Syp1 residence at the bud neck.
机译:在许多细胞类型中,Septins在细胞附属物的颈部和/或卵裂沟处装配成细丝和环,以帮助分隔质膜并支持胞质分裂。尚不清楚Septin环组件如何与膜重塑协调并如何在这些部位受到机械应力控制。通过遗传筛选,我们发现保守的Rho1 GTPase和其效应蛋白激酶C(Pkc1)之间具有酵母菌中的Septin环稳定性之间的意外链接。 Rho1和Pkc1都至少部分地通过与膜相关的F-BAR蛋白Syp1的磷酸化来稳定Septin环,该蛋白与Septin环在芽颈处不对称共定位。在两个丝氨酸上依赖Pkc1的磷酸化作用后,Syp1会从芽颈中移出,从而影响新形成的septin环的刚度。我们建议Rho1和Pkc1通过控制Syp1在芽颈处的驻留,部分与膜和细胞壁重塑协调septin环组装。

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