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Effects of Nonpolar Mutations in Each of the Seven Bacillus subtilis mrp Genes Suggest Complex Interactions among the Gene Products in Support of Na+ and Alkali but Not Cholate Resistance

机译:七个枯草芽孢杆菌mrp基因每个基因的非极性突变的影响表明基因产物之间的复杂相互作用支持Na +和碱,但不具有抗胆碱性

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摘要

The Bacillus subtilis mrp (multiple resistance and pH) operon supports Na+ and alkali resistance via an Na+/H+ antiport, as well as cholate efflux and resistance. Among the individual mutants with nonpolar mutations in each of the seven mrp genes, only the mrpF mutant exhibited cholate sensitivity and a cholate efflux defect that were complemented by expression of the deleted gene in trans. Expression of mrpF in the mrp null (VKN1) strain also restored cholate transport and increased Na+ efflux, indicating that MrpF does not require even low levels of other mrp gene expression for its own function. In contrast to MrpF, MrpA function had earlier seemed to depend upon at least modest expression of other mrp genes, i.e., mrpA restored Na+ resistance and efflux to strain VK6 (a polar mrpA mutant which expresses low levels of mrpB to -G) but not to the null strain VKN1. In a wild-type background, each nonpolar mutation in individual mrp genes caused profound Na+ sensitivity at both pH 7.0 and 8.3. The mrpA and mrpD mutants were particularly sensitive to alkaline pH even without added Na+. While transport assays in membrane vesicles from selected strains indicated that MrpA-dependent antiport can occur by a secondary, proton motive force-dependent mechanism, the requirement for multiple mrp gene products suggests that there are features of energization, function, or stabilization that differ from typical secondary membrane transporters. Northern analyses indicated regulatory relationships among mrp genes as well. All the mrp mutants, especially the mrpA, -B, -D, -E, and -G mutants, had elevated levels of mrp RNA relative to the wild type. Expression of an upstream gene, maeN, that encodes an Na+/malate symporter, was coordinately regulated with mrp, although it is not part of the operon.
机译:枯草芽孢杆菌mrp(多重抗性和pH)操纵子通过Na + / H +反端口支持Na +和碱抗性,以及胆酸盐外排和抗性。在七个mrp基因的每一个中均具有非极性突变的单个突变体中,只有mrpF突变体显示出胆酸盐敏感性和胆汁外排缺陷,这些缺陷可通过缺失基因的反式表达来补充。在mrp null(VKN1)株中mrpF的表达也恢复了胆酸盐转运,并增加了Na +流出,这表明MrppF不需要其他功能的mrp基因就可以发挥其功能。与MrpF相反,MrppA的功能先前似乎至少依赖于其他mrp基因的适度表达,即mrpA恢复了Na +抗性和对菌株VK6的外排(极性mrpA突变体,其表达低水平的mrpB到-G),但不是零应变VKN1。在野生型背景下,单个mrp基因中的每个非极性突变都会在pH 7.0和8.3时引起Na +敏感性高。即使不添加Na +,mrpA和mrpD突变体对碱性pH值也特别敏感。虽然从选定菌株的膜囊泡中进行转运分析表明,MrpA依赖的反向转运可以通过质子原动力依赖的次级机制发生,但对多种mrp基因产物的需求表明,其能量,功能或稳定化功能不同于典型的二级膜转运蛋白。 Northern分析也表明了mrp基因之间的调节关系。与野生型相比,所有的mrp突变体,特别是mrpA,-B,-D,-E和-G突变体,其mrp RNA的水平均升高。编码Na + /苹果酸同向转运体的上游基因maeN的表达受mrp协调调控,尽管它不是操纵子的一部分。

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