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Mitochondria can recognize and assemble fragments of a β-barrel structure

机译:线粒体可以识别并组装β桶结构的片段

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β-barrel proteins are found in the outer membranes of eukaryotic organelles of endosymbiotic origin as well as in the outer membrane of Gram-negative bacteria. Precursors of mitochondrial β-barrel proteins are synthesized in the cytosol and have to be targeted to the organelle. Currently, the signal that assures their specific targeting to mitochondria is poorly defined. To characterize the structural features needed for specific mitochondrial targeting and to test whether a full β-barrel structure is required, we expressed in yeast cells the β-barrel domain of the trimeric autotransporter Yersinia adhesin A (YadA). Trimeric autotransporters are found only in prokaryotes, where they are anchored to the outer membrane by a single 12-stranded β-barrel structure to which each monomer is contributing four β-strands. Importantly, we found that YadA is solely localized to the mitochondrial outer membrane, where it exists in a native trimeric conformation. These findings demonstrate that, rather than a linear sequence or a complete β-barrel structure, four β-strands are sufficient for the mitochondria to recognize and assemble a β-barrel protein. Remarkably, the evolutionary origin of mitochondria from bacteria enables them to import and assemble even proteins belonging to a class that is absent in eukaryotes.
机译:β-桶蛋白存在于内共生起源的真核细胞器的外膜以及革兰氏阴性细菌的外膜中。线粒体β-桶状蛋白的前体在细胞质中合成,必须靶向细胞器。当前,确保其特异性针对线粒体的信号的定义较差。为了表征特定线粒体靶向所需的结构特征并测试是否需要完整的β桶结构,我们在酵母细胞中表达了三聚体自转运耶尔森氏菌粘附素A(YadA)的β桶结构域。三聚体自转运蛋白仅在原核生物中发现,在原核生物中,它们通过单个12链β-桶结构锚定至外膜,每个单体在其中贡献了4条β链。重要的是,我们发现YadA仅位于线粒体外膜上,并以天然三聚体构象存在。这些发现表明,不是线性序列或完整的β-桶结构,而是四个β链足以使线粒体识别并组装β-桶蛋白。值得注意的是,线粒体从细菌的进化起源使它们能够导入和组装甚至属于真核生物中不存在的一类蛋白质。

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