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基于噬菌体展示的功能性宏基因组筛选技术鉴定的人肠道微生物群新的碳水化合物结合结构域。

New carbohydrate binding domains identified by phage display based functional metagenomic screens of human gut microbiota.

机构信息

CSIR- Institute of Microbial Technology, Sector 39-A, Chandigarh, 160036, India.

Emory Vaccine Center, Emory University, Atlanta, GA, USA.

出版信息

Commun Biol. 2023 Apr 5;6(1):371. doi: 10.1038/s42003-023-04718-0.

Abstract

Uncultured microbes represent a huge untapped biological resource of novel genes and gene products. Although recent genomic and metagenomic sequencing efforts have led to the identification of numerous genes that are homologous to existing annotated genes, there remains, yet, an enormous pool of unannotated genes that do not find significant sequence homology to existing annotated genes. Functional metagenomics offers a way to identify and annotate novel gene products. Here, we use functional metagenomics to mine novel carbohydrate binding domains that might aid human gut commensals in adherence, gut colonization, and metabolism of complex carbohydrates. We report the construction and functional screening of a metagenomic phage display library from healthy human fecal samples against dietary, microbial and host polysaccharides/glycoconjugates. We identify several protein sequences that do not find a hit to any known protein domain but are predicted to contain carbohydrate binding module-like folds. We heterologously express, purify and biochemically characterize some of these protein domains and demonstrate their carbohydrate-binding function. Our study reveals several previously unannotated carbohydrate-binding domains, including a levan binding domain and four complex N-glycan binding domains that might be useful for the labeling, visualization, and isolation of these glycans.

摘要

未培养的微生物代表了一种巨大的、尚未开发的新型基因和基因产物的生物资源。尽管最近的基因组学和宏基因组学测序工作已经鉴定出了许多与现有注释基因同源的基因,但仍然存在大量未注释的基因,它们与现有注释基因没有显著的序列同源性。功能宏基因组学为鉴定和注释新的基因产物提供了一种方法。在这里,我们使用功能宏基因组学来挖掘可能有助于人类肠道共生菌黏附、肠道定植和复杂碳水化合物代谢的新型碳水化合物结合结构域。我们报告了从健康人粪便样本中构建和功能筛选针对饮食、微生物和宿主多糖/糖缀合物的宏基因组噬菌体展示文库。我们鉴定了几个序列,它们与任何已知的蛋白质结构域都不匹配,但预测含有碳水化合物结合模块样折叠。我们异源表达、纯化并对这些蛋白质结构域进行了生化特性分析,并证明了它们的碳水化合物结合功能。我们的研究揭示了几个以前未注释的碳水化合物结合结构域,包括一个纤维二糖结合结构域和四个复杂的 N-糖结合结构域,这些结构域可能有助于这些聚糖的标记、可视化和分离。

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