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Genetic and Physical Interaction Studies Reveal Functional Similarities between ALBINO3 and ALBINO4 in Arabidopsis

机译:遗传和物理相互作用研究揭示了拟南芥中ALBINO3和ALBINO4之间的功能相似性。

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ALBINO3 (ALB3) is a well-known component of a thylakoid protein-targeting complex that interacts with the chloroplast signal recognition particle (cpSRP) and the cpSRP receptor, chloroplast filamentous temperature-sensitive Y (cpFtsY). Its protein-inserting function has been established mainly for light-harvesting complex proteins, which first interact with the unique chloroplast cpSRP43 component and then are delivered to the ALB3 integrase by a GTP-dependent cpSRP-cpFtsY interaction. In Arabidopsis (Arabidopsis thaliana), a subsequently discovered ALB3 homolog, ALB4, has been proposed to be involved not in light-harvesting complex protein targeting, but instead in the stabilization of the ATP synthase complex. Here, however, we show that ALB3 and ALB4 share significant functional overlap, and that both proteins are required for the efficient insertion of cytochrome f and potentially other subunits of pigment-bearing protein complexes. Genetic and physical interactions between ALB4 and ALB3, and physical interactions between ALB4 and cpSRP, suggest that the two ALB proteins may engage similar sets of interactors for their specific functions. We propose that ALB4 optimizes the insertion of thylakoid proteins by participating in the ALB3-cpSRP pathway for certain substrates (e.g. cytochrome f and the Rieske protein). Although ALB4 has clearly diverged from ALB3 in relation to the partner-recruiting C-terminal domain, our analysis suggests that one putative cpSRP-binding motif has not been entirely lost.
机译:ALBINO3(ALB3)是类囊体蛋白靶向复合物的众所周知的成分,该复合物与叶绿体信号识别颗粒(cpSRP)和cpSRP受体叶绿体丝状温度敏感Y(cpFtsY)相互作用。它的蛋白质插入功能主要针对光捕获复杂的蛋白质而建立,该蛋白质首先与独特的叶绿体cpSRP43成分相互作用,然后通过GTP依赖的cpSRP-cpFtsY相互作用传递至ALB3整合酶。在拟南芥(Arabidopsis thaliana)中,后来发现的ALB3同源物ALB4已被提议不参与光捕获复合物的蛋白靶向,而是参与ATP合酶复合物的稳定。但是,在这里,我们显示ALB3和ALB4共享显着的功能重叠,并且这两种蛋白对于有效插入细胞色素f和可能带有色素的蛋白复合物的其他亚基都是必需的。 ALB4和ALB3之间的遗传和物理相互作用,以及ALB4和cpSRP之间的物理相互作用表明,两种ALB蛋白可能因其特定功能而参与相似的相互作用子组。我们建议ALB4通过参与某些底物(例如细胞色素f和Rieske蛋白)的ALB3-cpSRP途径来优化类囊体蛋白的插入。尽管ALB4在招募伴侣的C末端结构域方面明显不同于ALB3,但我们的分析表明,一个推定的cpSRP结合基序并没有完全消失。

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