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一条部分代谢途径使B族链球菌能够克服宿主细菌群落中的醌缺乏问题。

A partial metabolic pathway enables group b streptococcus to overcome quinone deficiency in a host bacterial community.

作者信息

Franza Thierry, Delavenne Emilie, Derré-Bobillot Aurélie, Juillard Vincent, Boulay Mylène, Demey Emmanuelle, Vinh Joelle, Lamberet Gilles, Gaudu Philippe

机构信息

Micalis Institute, INRA, AgroParisTech, Université Paris-Saclay, Jouy-en-Josas, 78350, France.

ESPCI Paris, SMBP USR3149 CNRS, Paris, F-75005, France.

出版信息

Mol Microbiol. 2016 Oct;102(1):81-91. doi: 10.1111/mmi.13447. Epub 2016 Jul 8.

DOI:10.1111/mmi.13447
PMID:27328751
Abstract

Aerobic respiration metabolism in Group B Streptococcus (GBS) is activated by exogenous heme and menaquinone. This capacity enhances resistance of GBS to acid and oxidative stress and improves its survival. In this work, we discovered that GBS is able to respire in the presence of heme and 1,4-dihydroxy-2-naphthoic acid (DHNA). DHNA is a biosynthetic precursor of demethylmenaquinone (DMK) in many bacterial species. A GBS gene (gbs1789) encodes a homolog of the MenA 1,4-dihydroxy-2-naphthoate prenyltransferase enzyme, involved in the synthesis of demethylmenaquinone. In this study, we showed that gbs1789 is involved in the biosynthesis of long-chain demethylmenaquinones (DMK-10). The Δgbs1789 mutant cannot respire in the presence of heme and DHNA, indicating that endogenously synthesized DMKs are cofactors of the GBS respiratory chain. We also found that isoprenoid side chains from GBS DMKs are produced by the protein encoded by the gbs1783 gene, since this gene can complement an Escherichia coli ispB mutant defective for isoprenoids chain synthesis. In the gut or vaginal microbiote, where interspecies metabolite exchanges occur, this partial DMK biosynthetic pathway can be important for GBS respiration and survival in different niches.

摘要

B族链球菌(GBS)中的有氧呼吸代谢由外源性血红素和甲萘醌激活。这种能力增强了GBS对酸和氧化应激的抵抗力,并提高了其存活率。在这项研究中,我们发现GBS能够在血红素和1,4 - 二羟基 - 2 - 萘甲酸(DHNA)存在的情况下进行呼吸。DHNA是许多细菌物种中去甲基甲萘醌(DMK)的生物合成前体。一个GBS基因(gbs1789)编码MenA 1,4 - 二羟基 - 2 - 萘酸异戊烯基转移酶的同源物,该酶参与去甲基甲萘醌的合成。在本研究中,我们表明gbs1789参与长链去甲基甲萘醌(DMK - 10)的生物合成。Δgbs1789突变体在血红素和DHNA存在的情况下无法进行呼吸,这表明内源性合成的DMKs是GBS呼吸链的辅因子。我们还发现GBS的DMKs的类异戊二烯侧链由gbs1783基因编码的蛋白质产生,因为该基因可以互补一个在类异戊二烯链合成方面有缺陷的大肠杆菌ispB突变体。在肠道或阴道微生物群中,存在种间代谢物交换,这种部分DMK生物合成途径对于GBS在不同生态位中的呼吸和存活可能很重要。

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