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环境宏基因组文库的活性筛选揭示了新型羧酸酯酶家族。

Activity screening of environmental metagenomic libraries reveals novel carboxylesterase families.

机构信息

Department of Chemical Engineering and Applied Chemistry, University of Toronto, Toronto, ON, M5S 3E5, Canada.

School of Biological Sciences, Bangor University, Gwynedd LL57 2UW, UK.

出版信息

Sci Rep. 2017 Mar 8;7:44103. doi: 10.1038/srep44103.

Abstract

Metagenomics has made accessible an enormous reserve of global biochemical diversity. To tap into this vast resource of novel enzymes, we have screened over one million clones from metagenome DNA libraries derived from sixteen different environments for carboxylesterase activity and identified 714 positive hits. We have validated the esterase activity of 80 selected genes, which belong to 17 different protein families including unknown and cyclase-like proteins. Three metagenomic enzymes exhibited lipase activity, and seven proteins showed polyester depolymerization activity against polylactic acid and polycaprolactone. Detailed biochemical characterization of four new enzymes revealed their substrate preference, whereas their catalytic residues were identified using site-directed mutagenesis. The crystal structure of the metal-ion dependent esterase MGS0169 from the amidohydrolase superfamily revealed a novel active site with a bound unknown ligand. Thus, activity-centered metagenomics has revealed diverse enzymes and novel families of microbial carboxylesterases, whose activity could not have been predicted using bioinformatics tools.

摘要

宏基因组学使全球生物化学多样性的巨大储备成为可能。为了利用这一新型酶的巨大资源,我们从 16 个不同环境中衍生的宏基因组 DNA 文库中筛选了超过 100 万个克隆,以寻找羧酸酯酶活性,并鉴定出 714 个阳性克隆。我们已经验证了 80 个选定基因的酯酶活性,这些基因属于 17 种不同的蛋白质家族,包括未知和环化酶样蛋白。三种宏基因组酶表现出脂肪酶活性,七种蛋白对聚乳酸和聚己内酯表现出聚酯解聚活性。对四种新酶的详细生化特性进行了研究,揭示了它们的底物偏好,而使用定点突变确定了它们的催化残基。来自酰胺水解酶超家族的金属离子依赖酯酶 MGS0169 的晶体结构揭示了一个具有结合未知配体的新型活性位点。因此,基于活性的宏基因组学揭示了具有不同活性的各种酶和新型微生物羧酸酯酶家族,这些酶的活性无法使用生物信息学工具进行预测。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b3cb/5341072/ff8223a5dcf9/srep44103-f1.jpg

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