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A Systematic Analysis of Biosynthetic Gene Clusters in the Human Microbiome Reveals a Common Family of Antibiotics

机译:对人体微生物组中生物合成基因簇的系统分析揭示了一个共同的抗生素家族。

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In complex biological systems, small molecules often mediate microbe-microbe and microbe-host interactions. Using a systematic approach, we identified 3,118 small-molecule biosynthetic gene clusters (BGCs) in genomes of human-associated bacteria and studied their representation in 752 metagenomic samples from the NIH Human Microbiome Project. Remarkably, we discovered that BGCs for a class of antibiotics in clinical trials, thiopeptides, are widely distributed in genomes and metagenomes of the human microbiota. We purified and solved the structure of a thiopeptide antibiotic, lactocillin, from a prominent member of the vaginal microbiota. We demonstrate that lactocillin has potent antibacterial activity against a range of Gram-positive vaginal pathogens, and we show that lactocillin and other thiopeptide BGCs are expressed in vivo by analyzing human metatranscriptomic sequencing data. Our findings illustrate the widespread distribution of small-molecule-encoding BGCs in the human microbiome, and they demonstrate the bacterial production of drug-like molecules in humans.
机译:在复杂的生物系统中,小分子通常介导微生物与微生物以及微生物与宿主的相互作用。使用系统的方法,我们在人类相关细菌的基因组中鉴定了3,118个小分子生物合成基因簇(BGC),并研究了它们在来自NIH人类微生物组计划的752个宏基因组样本中的代表性。值得注意的是,我们发现在临床试验中,一类抗生素的BGC(硫肽)广泛分布于人类微生物群的基因组和基因组中。我们从阴道菌群的一个突出成员中纯化并解决了硫肽抗生素乳球菌素的结构。我们证明了乳球菌素对多种革兰氏阳性阴道病原体具有有效的抗菌活性,并且我们通过分析人类的转录组测序数据显示了乳球菌素和其他硫肽BGC在体内表达。我们的发现说明了在人类微生物组中编码小分子的BGC的广泛分布,并且它们证明了人类中类药物分子的细菌产生。

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