首页> 美国卫生研究院文献>The EMBO Journal >Recombinant forms of M13 procoat with an OmpA leader sequence or a large carboxy-terminal extension retain their independence of secY function.
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Recombinant forms of M13 procoat with an OmpA leader sequence or a large carboxy-terminal extension retain their independence of secY function.

机译:具有OmpA前导序列或较大的羧基末端延伸的M13前涂层的重组形式保留了其secY功能的独立性。

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摘要

The assembly of phage M13 procoat protein into the plasma membrane of Escherichia coli is independent of the secY protein. To test whether this is caused by the unusually small size of procoat, we fused DNA encoding 103 amino acids to the carboxy-terminal end of the procoat gene. The resulting fusion protein, which attains the same membrane-spanning conformation as mature coat protein, still does not require the secY function for membrane assembly. To determine whether the leader sequence governs interaction with the secY protein, we genetically exchanged the leader peptides between procoat and pro-OmpA, a protein which does require secY for its membrane assembly. Each of the resulting hybrid proteins assembles across the plasma membrane, though at a reduced rate. Membrane assembly of the fusion of procoat leader and OmpA required secY function, whereas assembly of the pro-OmpA leader/coat protein fusion was independent of secY. Properties of the entire procoat molecule, rather than its small size or a specific property of its leader peptide determines its mode of membrane assembly.
机译:噬菌体M13前涂层蛋白组装到大肠杆菌的质膜中与secY蛋白无关。为了测试这是否是由于Procoat的尺寸过小所致,我们将编码103个氨基酸的DNA融合到Procoat基因的羧基末端。得到的融合蛋白与成熟的外壳蛋白具有相同的跨膜构象,但仍不需要secY进行膜组装。为了确定前导序列是否支配与secY蛋白的相互作用,我们在procoat和pro-OmpA之间进行了前导肽的遗传交换,pro-OmpA是一种需要secY进行膜组装的蛋白。尽管以降低的速度,每个产生的杂合蛋白在质膜上组装。 procoat前导蛋白和OmpA融合蛋白的膜组件需要secY功能,而pro-OmpA前导蛋白/外壳蛋白融合蛋白的组件与secY无关。整个前涂层分子的性质,而不是其小尺寸或前导肽的特定性质,决定了其膜组装的模式。

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