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解析两株人体肠道产乙酸菌的体内代谢潜能。

Dissecting the in vivo metabolic potential of two human gut acetogens.

机构信息

Center for Genome Sciences, Washington University School of Medicine, St. Louis, Missouri 63108, USA.

出版信息

J Biol Chem. 2010 Jul 16;285(29):22082-90. doi: 10.1074/jbc.M110.117713. Epub 2010 May 5.

Abstract

Fermenting microbial communities generate hydrogen; its removal through the production of acetate, methane, or hydrogen sulfide modulates the efficiency of energy extraction from available nutrients in many ecosystems. We noted that pathway components for acetogenesis are more abundantly and consistently represented in the gut microbiomes of monozygotic twins and their mothers than components for methanogenesis or sulfate reduction and subsequently analyzed the metabolic potential of two sequenced human gut acetogens, Blautia hydrogenotrophica and Marvinbryantia formatexigens in vitro and in the intestines of gnotobiotic mice harboring a prominent saccharolytic bacterium. To do so, we developed a generally applicable method for multiplex sequencing of expressed microbial mRNAs (microbial RNA-Seq) and, together with mass spectrometry of metabolites, showed that these organisms have distinct patterns of substrate utilization. B. hydrogenotrophica targets aliphatic and aromatic amino acids. It increases the efficiency of fermentation by consuming reducing equivalents, thereby maintaining a high NAD(+)/NADH ratio and boosting acetate production. In contrast, M. formatexigens consumes oligosaccharides, does not impact the redox state of the gut, and boosts the yield of succinate. These findings have strategic implications for those who wish to manipulate the hydrogen economy of gut microbial communities in ways that modulate energy harvest.

摘要

发酵微生物群落产生氢气;通过产生乙酸、甲烷或硫化氢来去除氢气,可调节许多生态系统中从可用营养物质中提取能量的效率。我们注意到,产乙酸途径的组成部分在同卵双胞胎及其母亲的肠道微生物组中更为丰富和一致,而产甲烷或硫酸盐还原途径的组成部分则不然,随后我们分析了两种已测序的人类肠道产乙酸菌——产氢脱硫肠杆菌和产甲酸甲烷杆菌在体外和含有一种突出的产糖细菌的无菌小鼠肠道中的代谢潜力。为此,我们开发了一种用于表达微生物 mRNA(微生物 RNA-Seq)的多重测序的通用方法,并与代谢物的质谱分析相结合,表明这些生物体具有不同的底物利用模式。产氢脱硫肠杆菌以脂肪族和芳香族氨基酸为目标。它通过消耗还原当量来提高发酵效率,从而维持高 NAD(+)/NADH 比并促进乙酸的产生。相比之下,产甲酸甲烷杆菌消耗低聚糖,不会影响肠道的氧化还原状态,并提高琥珀酸的产量。这些发现对于那些希望以调节能量收获的方式操纵肠道微生物群落的氢气经济的人具有战略意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/be50/2903421/2d8fa95679e7/zbc0301023170001.jpg

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