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霍乱弧菌中阳离子-质子反向转运蛋白Vc-NhaP旁系同源组的生理学

Physiology of the Vc-NhaP paralogous group of cation-proton antiporters in Vibrio cholerae.

作者信息

Mourin Muntahi, Schubiger Carla B, Resch Craig T, Häse Claudia C, Dibrov Pavel

机构信息

Department of Microbiology, Faculty of Science, University of Manitoba, Rm. 430 Buller Building, Winnipeg, MB, R3T 2N2, Canada.

Department of Biomedical Sciences, College of Veterinary Medicine, Oregon State University, Corvallis, OR, 97331, USA.

出版信息

Mol Cell Biochem. 2017 Apr;428(1-2):87-99. doi: 10.1007/s11010-016-2919-3. Epub 2017 Jan 13.

DOI:10.1007/s11010-016-2919-3
PMID:28083717
Abstract

The genome of Vibrio cholerae encodes three cation-proton antiporters of NhaP-type, Vc-NhaP1, 2, and 3. To examine physiological roles of Vc-NhaP antiporters, triple ΔnhaP1ΔnhaP2ΔnhaP3 and single ΔnhaP3 deletion mutants of V. cholerae were constructed and characterized. Vc-NhaP3 was, for the first time, cloned and biochemically characterized. Activity measurements on the inside-out membrane vesicle experimental model defined Vc-NhaP3 as a potassium-specific cation-proton antiporter. While elimination of functional Vc-NhaP3 resulted in only minor growth defect in potassium-rich medium at pH 6.0, the triple Vc-NhaP mutant demonstrated severe growth defects at both low and high [K] at pH 6.0 and failed to grow at high [K] in mildly alkaline (pH 8.0 and 8.5) media, as well. Expressed from a plasmid, neither of the Vc-NhaP paralogues was able to complement the severe potassium-sensitive phenotype of the triple deletion mutant completely. Vc-NhaP1 provided much better complementation at acidic pH compared to Vc-NhaP2, despite the fact that Vc-NhaP2 showed much higher antiport activity in sub-bacterial vesicles. In mildly alkaline pH only Vc-NhaP2 complemented the potassium-sensitive phenotype of the triple deletion mutant. Taken together, these data suggest that in vivo all three isoforms operate in concert, contributing to K resistance of V. cholerae. We suggest that the Vc-NhaP paralogue group might play a role in passing gastric acid barrier by ingested V. cholerae cells.

摘要

霍乱弧菌的基因组编码三种 NhaP 型阳离子-质子反向转运蛋白,即 Vc-NhaP1、2 和 3。为了研究 Vc-NhaP 反向转运蛋白的生理作用,构建并表征了霍乱弧菌的三重 ΔnhaP1ΔnhaP2ΔnhaP3 和单重 ΔnhaP3 缺失突变体。首次克隆并对 Vc-NhaP3 进行了生化表征。在内翻膜囊泡实验模型上进行的活性测量将 Vc-NhaP3 定义为一种钾特异性阳离子-质子反向转运蛋白。虽然功能性 Vc-NhaP3 的缺失在 pH 6.0 的富钾培养基中仅导致轻微的生长缺陷,但三重 Vc-NhaP 突变体在 pH 6.0 的低[K]和高[K]条件下均表现出严重的生长缺陷,并且在轻度碱性(pH 8.0 和 8.5)培养基中的高[K]条件下也无法生长。从质粒表达时,Vc-NhaP 的任何一个旁系同源物都不能完全互补三重缺失突变体的严重钾敏感表型。尽管 Vc-NhaP2 在亚细菌囊泡中表现出更高的反向转运活性,但与 Vc-NhaP2 相比,Vc-NhaP1 在酸性 pH 下提供了更好的互补作用。在轻度碱性 pH 下,只有 Vc-NhaP2 能互补三重缺失突变体的钾敏感表型。综上所述,这些数据表明,在体内所有三种异构体协同作用,有助于霍乱弧菌的钾抗性。我们认为,Vc-NhaP 旁系同源物组可能在摄入的霍乱弧菌细胞通过胃酸屏障中发挥作用。

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The LysR-type regulator LeuO regulates the acid tolerance response in Vibrio cholerae.LysR 型调节因子 LeuO 调控霍乱弧菌的耐酸反应。
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The C-terminal cytoplasmic portion of the NhaP2 cation-proton antiporter from Vibrio cholerae affects its activity and substrate affinity.霍乱弧菌 NhaP2 阳离子-质子反向转运蛋白的 C 端胞质部分影响其活性和底物亲和力。
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NhaP1 is a K+(Na+)/H+ antiporter required for growth and internal pH homeostasis of Vibrio cholerae at low extracellular pH.NhaP1 是一种 K+(Na+)/H+反向转运蛋白,是霍乱弧菌在低细胞外 pH 值条件下生长和内部 pH 值动态平衡所必需的。
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