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Literature DB >> 30872395

Intestinal dysbiosis augments liver disease progression via NLRP3 in a murine model of primary sclerosing cholangitis.

Lijun Liao^1,2, Kai Markus Schneider¹, Francisco J Cubero^1,3,4, Christian Trautwein¹, Eric J C Galvez⁵, Mick Frissen¹, Hanns-Ulrich Marschall⁶, Huan Su¹, Maximilian Hatting¹, Annika Wahlström⁷, Johannes Haybaeck^8,9, Philip Puchas¹⁰, Antje Mohs¹, Jin Peng¹, Ina Bergheim¹¹, Anika Nier¹¹, Julia Hennings¹, Johanna Reißing¹, Henning W Zimmermann¹, Thomas Longerich¹², Till Strowig⁵, Christian Liedtke¹.

Abstract

OBJECTIVE: There is a striking association between human cholestatic liver disease (CLD) and inflammatory bowel disease. However, the functional implications for intestinal microbiota and inflammasome-mediated innate immune response in CLD remain elusive. Here we investigated the functional role of gut-liver crosstalk for CLD in the murine Mdr2 knockout (Mdr2-/-) model resembling human primary sclerosing cholangitis (PSC).
DESIGN: Male Mdr2 -/-, Mdr2-/- crossed with hepatocyte-specific deletion of caspase-8 (Mdr2-/- /Casp8∆hepa) and wild-type (WT) control mice were housed for 8 or 52 weeks, respectively, to characterise the impact of Mdr2 deletion on liver and gut including bile acid and microbiota profiling. To block caspase activation, a pan-caspase inhibitor (IDN-7314) was administered. Finally, the functional role of Mdr2-/- -associated intestinal dysbiosis was studied by microbiota transfer experiments.
RESULTS: Mdr2-/- mice displayed an unfavourable intestinal microbiota signature and pronounced NLRP3 inflammasome activation within the gut-liver axis. Intestinal dysbiosis in Mdr2-/- mice prompted intestinal barrier dysfunction and increased bacterial translocation amplifying the hepatic NLRP3-mediated innate immune response. Transfer of Mdr2-/- microbiota into healthy WT control mice induced significant liver injury in recipient mice, highlighting the causal role of intestinal dysbiosis for disease progression. Strikingly, IDN-7314 dampened inflammasome activation, ameliorated liver injury, reversed serum bile acid profile and cholestasis-associated microbiota signature.
CONCLUSIONS: MDR2-associated cholestasis triggers intestinal dysbiosis. In turn, translocation of endotoxin into the portal vein and subsequent NLRP3 inflammasome activation contribute to higher liver injury. This process does not essentially depend on caspase-8 in hepatocytes, but can be blocked by IDN-7314. © Author(s) (or their employer(s)) 2019. No commercial re-use. See rights and permissions. Published by BMJ.

Entities: Chemical Disease Gene Species

Keywords: cholestatic liver diseases; enteric bacterial microflora; gut inflammation; intestinal barrier function; primary sclerosing cholangitis

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Year: 2019 PMID： 30872395 DOI： 10.1136/gutjnl-2018-316670

Source DB: PubMed Journal: Gut ISSN： 0017-5749 Impact factor: 23.059

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Cited

27 in total

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8. Gut Microbiome Directs Hepatocytes to Recruit MDSCs and Promote Cholangiocarcinoma.

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Review 9. Gut microbiome in primary sclerosing cholangitis: A review.

Authors: Rebecca Little; Eytan Wine; Binita M Kamath; Anne M Griffiths; Amanda Ricciuto
Journal: World J Gastroenterol Date: 2020-06-07 Impact factor: 5.742

10. Fecal Microbiomes Distinguish Patients With Autoimmune Hepatitis From Healthy Individuals.

Authors: Jiamin Lou; Yan Jiang; Benchen Rao; Ang Li; Suying Ding; Hang Yan; Heqi Zhou; Zhenguo Liu; Qingmiao Shi; Guangying Cui; Zujiang Yu; Zhigang Ren
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