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Arabidopsis SCARs function interchangeably to meet actin-related protein 2/3 activation thresholds during morphogenesis

机译:拟南芥SCAR的功能互换,以在形态发生过程中满足肌动蛋白相关蛋白2/3激活阈值

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During polarized growth and tissue morphogenesis, cells must reorganize their cytoplasm and change shape in response to growth signals. Dynamic polymerization of actin filaments is one cellular component of polarized growth, and the actin-related protein 2/3 (ARP2/3) complex is an important actin filament nucleator in plants. ARP2/3 alone is inactive, and the Arabidopsis thaliana WAVE complex translates Rho-family small GTPase signals into an ARP2/3 activation response. The SCAR subunit of the WAVE complex is the primary activator of ARP2/3, and plant and vertebrate SCARs are encoded by a small gene family. However, it is unclear if SCAR isoforms function interchangeably or if they have unique properties that customize WAVE complex functions. We used the Arabidopsis distorted group mutants and an integrated analysis of SCAR gene and protein functions to address this question directly. Genetic results indicate that each of the four SCARs functions in the context of the WAVE-ARP2/3 pathway and together they define the lone mechanism for ARP2/3 activation. Genetic interactions among the scar mutants and transgene complementation studies show that the activators function interchangeably to meet the threshold for ARP2/3 activation in the cell. Interestingly, double, triple, and quadruple mutant analyses indicate that individual SCAR genes vary in their relative importance depending on the cell type, tissue, or organ that is analyzed. Differences among SCARs in mRNA levels and the biochemical efficiency of ARP2/3 activation may explain the functional contributions of individual genes.
机译:在极化生长和组织形态发生过程中,细胞必须重组其细胞质并响应生长信号而改变形状。肌动蛋白丝的动态聚合是极化生长的一种细胞成分,肌动蛋白相关蛋白2/3(ARP2 / 3)复合物是植物中重要的肌动蛋白丝成核剂。单独的ARP2 / 3无效,而拟南芥WAVE复合物将Rho家族的小GTPase信号转化为ARP2 / 3激活响应。 WAVE复合物的SCAR亚基是ARP2 / 3的主要激活剂,植物和脊椎动物SCAR由一个小基因家族编码。但是,尚不清楚SCAR亚型是否可以互换使用,或者它们是否具有可自定义WAVE复杂功能的独特属性。我们使用拟南芥扭曲的群体突变体和SCAR基因和蛋白质功能的综合分析直接解决了这个问题。遗传结果表明,四种SCAR均在WAVE-ARP2 / 3途径的背景下起作用,它们共同定义了ARP2 / 3激活的唯一机制。疤痕突变体之间的遗传相互作用和转基因互补研究表明,激活剂可互换运行,以满足细胞中ARP2 / 3激活的阈值。有趣的是,两次,三次和四次突变分析表明,单个SCAR基因的相对重要性会有所不同,具体取决于所分析的细胞类型,组织或器官。 SCAR在mRNA水平和ARP2 / 3激活的生化效率之间的差异可能解释了单个基因的功能贡献。

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