Genomic and functional diversity of cultivated Bifidobacterium from human gut microbiota

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  • Wenxi Li
  • Hewei Liang
  • Wenxin He
  • Xiaowei Gao
  • Zhinan Wu
  • Tongyuan Hu
  • Xiaoqian Lin
  • Mengmeng Wang
  • Yiyi Zhong
  • Haifeng Zhang
  • Lan Ge
  • Xin Jin
  • Liang Xiao
  • Yuanqiang Zou
The genus Bifidobacterium widely exists in human gut and has been increasingly used as the adjuvant probiotics for the prevention and treatment of diseases. However, the functional differences of Bifidobacterium genomes from different regions of the world remain unclear. We here describe an extensive study on the genomic characteristics and function annotations of 1512 genomes (clustered to 849 non-redundant genomes) of Bifidobacterium cultured from human gut. The distribution of some carbohydrate-active enzymes varied among different Bifidobacterium species and continents. More than 36% of the genomes of B. pseudocatenulatum harbored biosynthetic gene clusters of lanthipeptide-class-iv. 99.76% of the cultivated genomes of Bifidobacterium harbored genes of bile salt hydrolase. Most genomes of B. adolescentis, and all genomes of B. dentium harbored genes involved in gamma-aminobutyric acid synthesis. B. longum subsp. infantis were characterized harboring most genes related to human milk oligosaccharide utilization. Significant differences between the distribution of antibiotic resistance genes among different species and continents revealed the importance to use antibiotics precisely in the clinical treatment. Phages infecting Bifidobacterium and horizontal gene transfers occurring in genomes of Bifidobacterium were dependent on species and region sources, and might help Bifidobacterium adapt to the environment. In addition, the distribution of Bifidobacterium in human gut was found varied from different regions of the world. This study represents a comprehensive view of characteristics and functions of genomes of cultivated Bifidobacterium from human gut, and enables clinical advances in the future.
OriginalsprogEngelsk
Artikelnummere27270
TidsskriftHeliyon
Vol/bind10
Udgave nummer5
Antal sider14
ISSN2405-8440
DOI
StatusUdgivet - 2024

Bibliografisk note

Funding Information:
This study was supported by a grant from the National Natural Science Foundation of China (No. 32100009 ). This study was supported by Henan Supercomputer Center.

Publisher Copyright:
© 2024 The Authors

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