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Genomic variation landscape of the human gut microbiome

机译:人体肠道微生物基因组变异的风景

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摘要

While large-scale efforts have rapidly advanced the understanding and practical impact of human genomic variation, the latter is largely unexplored in the human microbiome. We therefore developed a framework for metagenomic variation analysis and applied it to 252 fecal metagenomes of 207 individuals from Europe and North America. Using 7.4 billion reads aligned to 101 reference species, we detected 10.3 million single nucleotide polymorphisms (SNPs), 107,991 short indels, and 1,051 structural variants. The average ratio of non-synonymous to synonymous polymorphism rates of 0.11 was more variable between gut microbial species than across human hosts. Subjects sampled at varying time intervals exhibited individuality and temporal stability of SNP variation patterns, despite considerable composition changes of their gut microbiota. This implies that individual-specific strains are not easily replaced and that an individual might have a unique metagenomic genotype, which may be exploitable for personalized diet or drug intake.
机译:尽管大规模的努力迅速提高了人类基因组变异的理解和实际影响,但人类微生物组在很大程度上尚未探索后者。因此,我们开发了宏基因组变异分析框架,并将其应用于来自欧洲和北美的207个人的252个粪便元基因组。使用与101个参考物种比对的74亿条读数,我们检测到1030万个单核苷酸多态性(SNP),107,991个短插入缺失和1,051个结构变异。肠道微生物物种之间的非同义与同义多态性比率的平均比率为0.11,比人类宿主之间的差异更大。尽管其肠道菌群的组成发生了显着变化,但在不同时间间隔采样的受试者仍表现出SNP变化模式的个性和时间稳定性。这意味着个体特异性菌株不容易被替换,个体可能具有独特的宏基因组基因型,可以用于个性化饮食或药物摄入。

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