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支气管败血波氏杆菌的烟酸降解途径和 6-羟基烟酸应答调控因子 BpsR 由 nic 操纵子编码。

The Bordetella bronchiseptica nic locus encodes a nicotinic acid degradation pathway and the 6-hydroxynicotinate-responsive regulator BpsR.

机构信息

Department of Microbiology and Immunology, University of Minnesota Medical School, 3-117 Microbiology Research Facility, 689 23rd Ave. S.E, Minneapolis, MN 55455-1507, USA.

出版信息

Mol Microbiol. 2018 May;108(4):397-409. doi: 10.1111/mmi.13943. Epub 2018 Mar 11.

Abstract

The classical Bordetella species use amino acids as carbon sources and can catabolize organic acids and tricarboxylic acid cycle intermediates. They are also auxotrophic for nicotinamide adenine dinucleotide (NAD) pathway precursors such as nicotinic acid. Bordetellae have a putative nicotinate catabolism gene locus highly similar to that characterized in Pseudomonas putida KT2440. This study determined the distribution of the nic genes among Bordetella species and analyzed the regulation of this nicotinic acid degradation system. Transcription of the Bordetella bronchiseptica nicC gene was repressed by the NicR ortholog, BpsR, previously shown to regulate extracellular polysaccharide synthesis genes. nicC expression was derepressed by nicotinic acid or by the first product of the degradation pathway, 6-hydroxynicotinic acid, which was shown to be the inducer. Results using mutants with either a hyperactivated pathway or an inactivated pathway showed a marked effect on growth on nicotinic acid that indicated this degradation pathway influences NAD biosynthesis. Pathway dysregulation also affected Bordetella BvgAS-mediated virulence gene regulation, demonstrating that fluctuation of intracellular nicotinic acid pools impacts Bvg phase transition responses.

摘要

经典博德特氏菌属利用氨基酸作为碳源,并能分解有机酸和三羧酸循环中间体。它们还需要烟酰胺腺嘌呤二核苷酸(NAD)途径前体,如烟酸作为营养物。博德特氏菌具有类似于假单胞菌 KT2440 中所描述的假定烟酸分解代谢基因座。本研究确定了 nic 基因在博德特氏菌属中的分布,并分析了烟酸降解系统的调控。博德特氏菌支气管败血亚种 nicC 基因的转录受到 NicR 同源物 BpsR 的抑制,先前的研究表明,BpsR 调控细胞外多糖合成基因。nicC 的表达被烟酸或降解途径的第一个产物 6-羟基烟酸去阻遏,6-羟基烟酸被证明是诱导物。使用具有超激活途径或失活途径的突变体的结果表明,烟酸对生长的显著影响表明,这种降解途径影响 NAD 生物合成。途径失调也影响博德特氏菌 BvgAS 介导的毒力基因调控,表明细胞内烟酸池的波动会影响 Bvg 相转变反应。

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