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首页> 外文期刊>Genetics: A Periodical Record of Investigations Bearing on Heredity and Variation >Comprehensive Genetic Analysis of Paralogous Terminal Septin Subunits Shs1 and Cdc11 in Saccharomyces cerevisiae
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Comprehensive Genetic Analysis of Paralogous Terminal Septin Subunits Shs1 and Cdc11 in Saccharomyces cerevisiae

机译:酿酒酵母中同源的末端Septin亚基Shs1和Cdc11的综合遗传分析。

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摘要

Septins are a family of GTP-binding proteins considered to be cytoskeletal elements because they self-assemble into filaments and other higher-order structures in vivo. In budding yeast, septins establish a diffusion barrier at the bud neck between a mother and daughter cell, promote membrane curvature there, and serve as a scaffold to recruit other proteins to the site of cytokinesis. However, the mechanism by which any septin engages a partner protein has been unclear. The two most related and recently evolved subunits appear to be Cdc11 and Shs1, and the basic building blocks for assembling septin structures are hetero-octameric rods (Cdc11-Cdc12-Cdc3-Cdc10-Cdc10-Cdc3-Cdc12-Cdc11 and Shs1-Cdc12-Cdc3-Cdc10-Cdc10-Cdc3-Cdc12-Shs1). Loss of Cdc11 is not normally tolerated, whereas cells lacking Shs1 do not appear grossly abnormal. We established several different sensitized genetic backgrounds wherein Shs1 is indispensable, which allowed us to carry out the first comprehensive and detailed genetic analysis of Shs1 in vivo. Our analysis revealed several novel insights, including: (i) the sole portion of Shs1 essential for its function is a predicted coiled-coil-forming segment in its C-terminal extension (CTE); (ii) the CTE of Cdc11 shares this function; (iii) this role for the CTEs of Cdc11 and Shs1 is quite distinct from that of the CTEs of Cdc3 and Cdc12; and (iv) heterotypic Cdc11 and Shs1 junctions likely occur in vivo.
机译:Septins是GTP结合蛋白的一个家族,被认为是细胞骨架的元素,因为它们在体内可以自组装成细丝和其他更高阶的结构。在发芽酵母中,Septins在母细胞和子细胞之间的芽颈处建立扩散屏障,在那里促进膜弯曲,并充当将其他蛋白质募集到胞质分裂位点的支架。但是,尚不清楚任何Septin参与伴侣蛋白的机制。两个最相关且最近发展的亚基似乎是Cdc11和Shs1,组装septin结构的基本构件是异八聚体棒(Cdc11-Cdc12-Cdc3-Cdc10-Cdc10-Cdc3-Cdc12-Cdc11和Shs1-Cdc12- Cdc3-Cdc10-Cdc10-Cdc3-Cdc12-Shs1)。通常不容忍Cdc11的丢失,而缺少Shs1的细胞并未出现严重异常。我们建立了Shs1不可缺少的几种不同的致敏遗传背景,这使我们能够在体内进行Shs1的第一个全面而详细的遗传分析。我们的分析揭示了一些新颖的见解,其中包括:(i)Shs1对其功能必不可少的唯一部分是其C端延伸(CTE)的预测卷曲螺旋形成片段; (ii)Cdc11的CTE具有此功能; (iii)Cdc11和Shs1的CTE的角色与Cdc3和Cdc12的CTE的角色完全不同; (iv)异型Cdc11和Shs1连接可能在体内发生。

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