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Stably bridging a great divide: Localization of the SpoIIQ landmark protein in Bacillus subtilis

机译:稳定弥合鸿沟:枯草芽孢杆菌中SpoIIQ标志性蛋白的定位

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Summary: Many bacterial proteins involved in fundamental processes such as cell shape maintenance, cell cycle regulation, differentiation, division and motility localize dynamically to specific subcellular regions. However, the mechanisms underlying dynamic protein localization are incompletely understood. Using the SpoIIQ protein in Bacillus subtilis as a case study, two reports present important novel insights into how a protein finds its right place at the right time and remains stably bound. During sporulation, SpoIIQ localizes in clusters in the forespore membrane at the interface that separates the forespore and mother cell and functions as a landmark protein for SpoIIIAH in the mother cell membrane. The extracellular domains of SpoIIQ and SpoIIIAH interact directly effectively bridging the gap between the two membranes. Here, SpoIIQ localization is shown to depend on two pathways, one involves SpoIIIAH, the second involves two peptidoglycan-degrading enzymes SpoIIP and SpoIID; and, SpoIIQ is only delocalized in the absence of all three proteins. Importantly, in the absence of SpoIIIAH, SpoIIQ apparently localizes normally. However, FRAP experiments demonstrated that SpoIIQ is not stably maintained in the clusters in this mutant. Thus, a second targeting pathway can mask significant changes in the localization of a protein.
机译:摘要:许多参与基本过程(例如细胞形状维持,细胞周期调节,分化,分裂和运动)的细菌蛋白动态地定位于特定的亚细胞区域。但是,尚不完全了解动态蛋白质定位的基础机制。以枯草芽孢杆菌中的SpoIIQ蛋白为案例研究,有两个报告提供了关于该蛋白如何在正确的时间找到正确的位置并保持稳定结合的重要新颖见解。在孢子形成过程中,SpoIIQ定位在前孢子膜中的簇中,位于将前孢子和母细胞分开的界面上,并充当母细胞膜中SpoIIIAH的标志性蛋白。 SpoIIQ和SpoIIIAH的胞外域直接相互作用,有效地弥合了两个膜之间的间隙。在这里,SpoIIQ的定位取决于两个途径,一个途径涉及SpoIIIAH,第二个途径涉及两种降解肽聚糖的酶SpoIIP和SpoIID。并且,SpoIIQ仅在所有这三种蛋白质均不存在的情况下才被去域化。重要的是,在没有SpoIIIAH的情况下,SpoIIQ显然可以正常定位。但是,FRAP实验表明该突变体的簇中SpoIIQ不能稳定维持。因此,第二种靶向途径可以掩盖蛋白质定位的重大变化。

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