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Escherichia coli transport mutants lacking binding protein and other components of the branched-chain amino acid transport systems.

机译:大肠杆菌运输突变体缺乏结合蛋白和支链氨基酸运输系统的其他组件。

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摘要

Further evidence on the role of binding proteins in branched-chain amino acid transport in Escherichia coli was obtained by selecting mutants with altered expression of the binding proteins. The mutator phage Mu was used to induce E. coli L-valine-resistant mutants defective in branched-chain amino acid transport. By making use of mild selective conditions and strain backgrounds with derepressed high-affinity, binding protein-mediated transport systems, we were able to isolate a new class of transport mutants defective in these systems. Mutant strains AE84084 (livK::Mucts) and AE840102 (livJ) were found to be defective in leucine-specific and LIV binding proteins, respectively, by transport assay, in vitro binding activity, and by sodium dodecyl sulfate-polyacrylamide gel electrophoresis. Mutant strain AE4107 (livH::Mu), although lacking high-affinity, branched-chain amino acid transport, retained functional binding proteins and therefore evidently codes for an additional component of high-affinity transport. The livH, livJ, and livK mutations were mapped by transduction and shown to be closely linked to each other in the malT region (min 74) of the E. coli genetic map.
机译:通过选择结合蛋白表达改变的突变体,获得了结合蛋白在大肠杆菌中支链氨基酸运输中的作用的进一步证据。突变体噬菌体Mu用于诱导分支链氨基酸转运缺陷的大肠杆菌L-缬氨酸抗性突变体。通过使用温和的选择性条件和具有低阻抑的高亲和力,结合蛋白介导的转运系统的菌株背景,我们能够分离出在这些系统中有缺陷的新型转运突变体。通过转运测定,体外结合活性和十二烷基硫酸钠-聚丙烯酰胺凝胶电泳,发现突变株AE84084(livK :: Mucts)和AE840102(livJ)分别在亮氨酸特异性蛋白和LIV结合蛋白中有缺陷。突变菌株AE4107(livH :: Mu)尽管缺乏高亲和力,支链氨基酸转运,但保留了功能结合蛋白,因此显然编码了高亲和力转运的其他成分。通过转导定位了livH,livJ和livK突变,并显示在大肠杆菌遗传图谱的malT区域(最小74)中彼此紧密联系。

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