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Bifidobacterium bifidum strains synergize with immune checkpoint inhibitors to reduce tumour burden in mice

Cited 118 time in Web of Science Cited 126 time in Scopus
Authors

Lee, Se-Hoon; Cho, Sung Yup; Yoon, Youngmin; Park, Changho; Sohn, Jinyoung; Jeong, Jin-Ju; Jeon, Bu-Nam; Jang, Mongjoo; An, Choa; Lee, Suro; Kim, Yun Yeon; Kim, Gihyeon; Kim, Sujeong; Kim, Yunjae; Lee, Gwang Bin; Lee, Eun Ju; Kim, Sang Gyun; Kim, Hong Sook; Kim, Yeongmin; Kim, Hyun; Yang, Hyun-Suk; Kim, Sarang; Kim, Seonggon; Chung, Hayung; Moon, Myeong Hee; Nam, Myung Hee; Kwon, Jee Young; Won, Sungho; Park, Joon-Suk; Weinstock, George M.; Lee, Charles; Yoon, Kyoung Wan; Park, Hansoo

Issue Date
2021-03
Publisher
NATURE PUBLISHING GROUP
Citation
Nature Microbiology, Vol.6 No.3, pp.277-+
Abstract
The gut microbiome can influence the development of tumours and the efficacy of cancer therapeutics(1-5); however, the multi-omics characteristics of antitumour bacterial strains have not been fully elucidated. In this study, we integrated metagenomics, genomics and transcriptomics of bacteria, and analyses of mouse intestinal transcriptome and serum metabolome data to reveal an additional mechanism by which bacteria determine the efficacy of cancer therapeutics. In gut microbiome analyses of 96 samples from patients with non-small-cell lung cancer, Bifidobacterium bifidum was abundant in patients responsive to therapy. However, when we treated syngeneic mouse tumours with commercial strains of B. bifidum to establish relevance for potential therapeutic uses, only specific B. bifidum strains reduced tumour burden synergistically with PD-1 blockade or oxaliplatin treatment by eliciting an antitumour host immune response. In mice, these strains induced tuning of the immunological background by potentiating the production of interferon-gamma, probably through the enhanced biosynthesis of immune-stimulating molecules and metabolites.
ISSN
2058-5276
URI
https://hdl.handle.net/10371/202737
DOI
https://doi.org/10.1038/s41564-020-00831-6
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  • College of Medicine
Research Area Cancer genomics, Drug resistance, Targeted therapeutics

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