Gut pathobionts underlie intestinal barrier dysfunction and liver T helper 17 cell immune response in primary sclerosing cholangitis

Nobuhiro Nakamoto; Nobuo Sasaki; Ryo Aoki; Kentaro Miyamoto; Wataru Suda; Toshiaki Teratani; Takahiro Suzuki; Yuzo Koda; Po Sung Chu; Nobuhito Taniki; Akihiro Yamaguchi; Mitsuhiro Kanamori; Nobuhiko Kamada; Masahira Hattori; Hiroshi Ashida; Michiie Sakamoto; Koji Atarashi; Seiko Narushima; Akihiko Yoshimura; Kenya Honda; Toshiro Sato; Takanori Kanai

doi:10.1038/s41564-018-0333-1

Gut pathobionts underlie intestinal barrier dysfunction and liver T helper 17 cell immune response in primary sclerosing cholangitis

Nobuhiro Nakamoto, Nobuo Sasaki, Ryo Aoki, Kentaro Miyamoto, Wataru Suda, Toshiaki Teratani, Takahiro Suzuki, Yuzo Koda, Po Sung Chu, Nobuhito Taniki, Akihiro Yamaguchi, Mitsuhiro Kanamori, Nobuhiko Kamada, Masahira Hattori, Hiroshi Ashida, Michiie Sakamoto, Koji Atarashi, Seiko Narushima, Akihiko Yoshimura, Kenya HondaToshiro Sato, Takanori Kanai

研究成果: ジャーナルへの寄稿 › 学術誌 › 査読

165 被引用数 (Scopus)

抄録

Primary sclerosing cholangitis (PSC) is a chronic inflammatory liver disease and its frequent complication with ulcerative colitis highlights the pathogenic role of epithelial barrier dysfunction. Intestinal barrier dysfunction has been implicated in the pathogenesis of PSC, yet its underlying mechanism remains unknown. Here, we identify Klebsiella pneumonia in the microbiota of patients with PSC and demonstrate that K. pneumoniae disrupts the epithelial barrier to initiate bacterial translocation and liver inflammatory responses. Gnotobiotic mice inoculated with PSC-derived microbiota exhibited T helper 17 (T _H 17) cell responses in the liver and increased susceptibility to hepatobiliary injuries. Bacterial culture of mesenteric lymph nodes in these mice isolated K. pneumoniae, Proteus mirabilis and Enterococcus gallinarum, which were prevalently detected in patients with PSC. A bacterial-organoid co-culture system visualized the epithelial-damaging effect of PSC-derived K. pneumoniae that was associated with bacterial translocation and susceptibility to T _H 17-mediated hepatobiliary injuries. We also show that antibiotic treatment ameliorated the T _H 17 immune response induced by PSC-derived microbiota. These results highlight the role of pathobionts in intestinal barrier dysfunction and liver inflammation, providing insights into therapeutic strategies for PSC.

本文言語	英語
ページ（範囲）	492-503
ページ数	12
ジャーナル	Nature Microbiology
巻	4
号	3
DOI	https://doi.org/10.1038/s41564-018-0333-1
出版ステータス	出版済み - 3月 1 2019
外部発表	はい

!!!All Science Journal Classification (ASJC) codes

微生物学
免疫学
応用微生物学とバイオテクノロジー
遺伝学
微生物学（医療）
細胞生物学

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10.1038/s41564-018-0333-1

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引用スタイル

Nakamoto, N., Sasaki, N., Aoki, R., Miyamoto, K., Suda, W., Teratani, T., Suzuki, T., Koda, Y., Chu, P. S., Taniki, N., Yamaguchi, A., Kanamori, M., Kamada, N., Hattori, M., Ashida, H., Sakamoto, M., Atarashi, K., Narushima, S., Yoshimura, A., ... Kanai, T. (2019). Gut pathobionts underlie intestinal barrier dysfunction and liver T helper 17 cell immune response in primary sclerosing cholangitis. Nature Microbiology, 4(3), 492-503. https://doi.org/10.1038/s41564-018-0333-1

Nakamoto, N, Sasaki, N, Aoki, R, Miyamoto, K, Suda, W, Teratani, T, Suzuki, T, Koda, Y, Chu, PS, Taniki, N, Yamaguchi, A, Kanamori, M, Kamada, N, Hattori, M, Ashida, H, Sakamoto, M, Atarashi, K, Narushima, S, Yoshimura, A, Honda, K, Sato, T & Kanai, T 2019, 'Gut pathobionts underlie intestinal barrier dysfunction and liver T helper 17 cell immune response in primary sclerosing cholangitis', Nature Microbiology, vol. 4, no. 3, pp. 492-503. https://doi.org/10.1038/s41564-018-0333-1

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title = "Gut pathobionts underlie intestinal barrier dysfunction and liver T helper 17 cell immune response in primary sclerosing cholangitis",

abstract = " Primary sclerosing cholangitis (PSC) is a chronic inflammatory liver disease and its frequent complication with ulcerative colitis highlights the pathogenic role of epithelial barrier dysfunction. Intestinal barrier dysfunction has been implicated in the pathogenesis of PSC, yet its underlying mechanism remains unknown. Here, we identify Klebsiella pneumonia in the microbiota of patients with PSC and demonstrate that K. pneumoniae disrupts the epithelial barrier to initiate bacterial translocation and liver inflammatory responses. Gnotobiotic mice inoculated with PSC-derived microbiota exhibited T helper 17 (T H 17) cell responses in the liver and increased susceptibility to hepatobiliary injuries. Bacterial culture of mesenteric lymph nodes in these mice isolated K. pneumoniae, Proteus mirabilis and Enterococcus gallinarum, which were prevalently detected in patients with PSC. A bacterial-organoid co-culture system visualized the epithelial-damaging effect of PSC-derived K. pneumoniae that was associated with bacterial translocation and susceptibility to T H 17-mediated hepatobiliary injuries. We also show that antibiotic treatment ameliorated the T H 17 immune response induced by PSC-derived microbiota. These results highlight the role of pathobionts in intestinal barrier dysfunction and liver inflammation, providing insights into therapeutic strategies for PSC. ",

author = "Nobuhiro Nakamoto and Nobuo Sasaki and Ryo Aoki and Kentaro Miyamoto and Wataru Suda and Toshiaki Teratani and Takahiro Suzuki and Yuzo Koda and Chu, {Po Sung} and Nobuhito Taniki and Akihiro Yamaguchi and Mitsuhiro Kanamori and Nobuhiko Kamada and Masahira Hattori and Hiroshi Ashida and Michiie Sakamoto and Koji Atarashi and Seiko Narushima and Akihiko Yoshimura and Kenya Honda and Toshiro Sato and Takanori Kanai",

note = "Funding Information: We thank S. Chiba, S. Shiba, R. Morikawa, T. Katayama, A. Ikura, Y. Mikami and T. Sujino (Division of Gastroenterology and Hepatology, Keio University) for technical assistance and critical reading of this manuscript. This study was supported by the Japan Society for the Promotion of Science (JSPS) KAKENHI Grant-in-Aid (C) 16K09374 and (A) 15H02534, the Advanced Research and Development Programs for Medical Innovation (AMED-CREST; 16gm1010003h0001), the TAKEDA Science Fund, Ezaki Glico Co. Ltd and Keio University Medical Fund. K.H. was funded through AMED LEAP under grant number JP17gm0010003. A. Yoshimura was supported by the JSPS KAKENHI Grant-in-Aid (S) JP17H06175, Challenging Research (P) JP18H05376 and AMED-CREST JP18gm0510019 and JP18gm1110009. Publisher Copyright: {\textcopyright} 2019, The Author(s), under exclusive licence to Springer Nature Limited.",

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T1 - Gut pathobionts underlie intestinal barrier dysfunction and liver T helper 17 cell immune response in primary sclerosing cholangitis

AU - Nakamoto, Nobuhiro

AU - Sasaki, Nobuo

AU - Aoki, Ryo

AU - Miyamoto, Kentaro

AU - Suda, Wataru

AU - Teratani, Toshiaki

AU - Suzuki, Takahiro

AU - Koda, Yuzo

AU - Chu, Po Sung

AU - Taniki, Nobuhito

AU - Yamaguchi, Akihiro

AU - Kanamori, Mitsuhiro

AU - Kamada, Nobuhiko

AU - Hattori, Masahira

AU - Ashida, Hiroshi

AU - Sakamoto, Michiie

AU - Atarashi, Koji

AU - Narushima, Seiko

AU - Yoshimura, Akihiko

AU - Honda, Kenya

AU - Sato, Toshiro

AU - Kanai, Takanori

N1 - Funding Information: We thank S. Chiba, S. Shiba, R. Morikawa, T. Katayama, A. Ikura, Y. Mikami and T. Sujino (Division of Gastroenterology and Hepatology, Keio University) for technical assistance and critical reading of this manuscript. This study was supported by the Japan Society for the Promotion of Science (JSPS) KAKENHI Grant-in-Aid (C) 16K09374 and (A) 15H02534, the Advanced Research and Development Programs for Medical Innovation (AMED-CREST; 16gm1010003h0001), the TAKEDA Science Fund, Ezaki Glico Co. Ltd and Keio University Medical Fund. K.H. was funded through AMED LEAP under grant number JP17gm0010003. A. Yoshimura was supported by the JSPS KAKENHI Grant-in-Aid (S) JP17H06175, Challenging Research (P) JP18H05376 and AMED-CREST JP18gm0510019 and JP18gm1110009. Publisher Copyright: © 2019, The Author(s), under exclusive licence to Springer Nature Limited.

PY - 2019/3/1

Y1 - 2019/3/1

N2 - Primary sclerosing cholangitis (PSC) is a chronic inflammatory liver disease and its frequent complication with ulcerative colitis highlights the pathogenic role of epithelial barrier dysfunction. Intestinal barrier dysfunction has been implicated in the pathogenesis of PSC, yet its underlying mechanism remains unknown. Here, we identify Klebsiella pneumonia in the microbiota of patients with PSC and demonstrate that K. pneumoniae disrupts the epithelial barrier to initiate bacterial translocation and liver inflammatory responses. Gnotobiotic mice inoculated with PSC-derived microbiota exhibited T helper 17 (T H 17) cell responses in the liver and increased susceptibility to hepatobiliary injuries. Bacterial culture of mesenteric lymph nodes in these mice isolated K. pneumoniae, Proteus mirabilis and Enterococcus gallinarum, which were prevalently detected in patients with PSC. A bacterial-organoid co-culture system visualized the epithelial-damaging effect of PSC-derived K. pneumoniae that was associated with bacterial translocation and susceptibility to T H 17-mediated hepatobiliary injuries. We also show that antibiotic treatment ameliorated the T H 17 immune response induced by PSC-derived microbiota. These results highlight the role of pathobionts in intestinal barrier dysfunction and liver inflammation, providing insights into therapeutic strategies for PSC.

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