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Common formin-regulating sequences in Smy1 and Bud14 are required for the control of actin cable assembly in vivo

机译:在体内控制肌动蛋白电缆组装需要Smy1和Bud14中常见的甲酰胺调节序列

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摘要

Formins comprise a large family of proteins with diverse roles in remodeling the actin cytoskeleton. However, the spatiotemporal mechanisms used by cells to control formin activities are only beginning to be understood. Here we dissected Smy1, which has dual roles in regulating formins and myosin. Using mutagenesis, we identified specific sequences in Smy1 critical for its in vitro inhibitory effects on the FH2 domain of the formin Bnr1. By integrating smy1 alleles targeting those sequences, we genetically uncoupled Smy1's functions in regulating formins and myosin. Quantitative imaging analysis further demonstrated that the ability of Smy1 to directly control Bnr1 activity is crucial in vivo for proper actin cable length, shape, and velocity and, in turn, efficient secretory vesicle transport. A Smy1-like sequence motif was also identified in a different Bnr1 regulator, Bud14, and found to be essential for Bud14 functions in regulating actin cable architecture and function in vivo. Together these observations reveal unanticipated mechanistic ties between two distinct formin regulators. Further, they emphasize the importance of tightly controlling formin activities in vivo to generate specialized geometries and dynamics of actin structures tailored to their physiological roles.
机译:Formins包含一个大家族的蛋白质,在重塑肌动蛋白的细胞骨架中具有多种作用。然而,细胞用来控制有组织活动的时空机制才刚刚开始被理解。在这里,我们剖析了Smy1,它在调节formins和myosin中具有双重作用。使用诱变,我们在Smy1中鉴定了特定的序列,该序列对Sform1对Formin Bnr1的FH2结构域的体外抑制作用至关重要。通过整合靶向这些序列的smy1等位基因,我们在遗传上解耦了Smy1在调节formins和肌球蛋白中的功能。定量成像分析进一步证明,Smy1直接控制Bnr1活性的能力在体内对于适当的肌动蛋白电缆长度,形状和速度以及有效的分泌性囊泡运输至关重要。在不同的Bnr1调节器Bud14中也鉴定出了Smy1样的序列基序,发现它对Bud14在调节肌动蛋白电缆的结构和体内功能中至关重要。这些观察结果共同揭示了两个截然不同的甲醛调节器之间意想不到的机械联系。此外,他们强调了严密控制体内福尔明活动以产生适合其生理作用的特定几何形状和肌动蛋白结构动力学的重要性。

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