Department of Cellular Biology, Instituto de Biología Molecular de Barcelona (IBMB-CSIC), Barcelona, Spain.
EMBO J. 2010 Sep 1;29(17):2899-914. doi: 10.1038/emboj.2010.159. Epub 2010 Jul 20.
Myosins-I are conserved proteins that bear an N-terminal motor head followed by a Tail Homology 1 (TH1) lipid-binding domain. Some myosins-I have an additional C-terminal extension (C(ext)) that promotes Arp2/3 complex-dependent actin polymerization. The head and the tail are separated by a neck that binds calmodulin or calmodulin-related light chains. Myosins-I are known to participate in actin-dependent membrane remodelling. However, the molecular mechanisms controlling their recruitment and their biochemical activities in vivo are far from being understood. In this study, we provided evidence suggesting the existence of an inhibitory interaction between the TH1 domain of the yeast myosin-I Myo5 and its C(ext). The TH1 domain prevented binding of the Myo5 C(ext) to the yeast WIP homologue Vrp1, Myo5 C(ext)-induced actin polymerization and recruitment of the Myo5 C(ext) to endocytic sites. Our data also indicated that calmodulin dissociation from Myo5 weakened the interaction between the neck and TH1 domains and the C(ext). Concomitantly, calmodulin dissociation triggered Myo5 binding to Vrp1, extended the myosin-I lifespan at endocytic sites and activated Myo5-induced actin polymerization.
肌球蛋白-I 是一种保守的蛋白质,它具有一个 N 端的马达头部,其后是一个同源 1 型(TH1)脂质结合域。一些肌球蛋白-I 具有一个额外的 C 端延伸(C(ext)),促进 Arp2/3 复合物依赖性肌动蛋白聚合。头部和尾部由一个颈部隔开,颈部结合钙调蛋白或钙调蛋白相关的轻链。肌球蛋白-I 已知参与肌动蛋白依赖性膜重塑。然而,控制其募集和体内生化活性的分子机制远未被理解。在这项研究中,我们提供了证据表明酵母肌球蛋白-I Myo5 的 TH1 结构域与其 C(ext)之间存在抑制性相互作用。TH1 结构域阻止了 Myo5 C(ext)与酵母 WIP 同源物 Vrp1 的结合,Myo5 C(ext)诱导的肌动蛋白聚合和 Myo5 C(ext)招募到内吞部位。我们的数据还表明,钙调蛋白从 Myo5 上解离削弱了颈部和 TH1 结构域之间以及 C(ext)之间的相互作用。同时,钙调蛋白的解离触发了 Myo5 与 Vrp1 的结合,延长了肌球蛋白-I 在内吞部位的寿命,并激活了 Myo5 诱导的肌动蛋白聚合。