4.5 Article

Intestinal virome in patients with alcohol use disorder and after abstinence

期刊

HEPATOLOGY COMMUNICATIONS
卷 6, 期 8, 页码 2058-2069

出版社

JOHN WILEY & SONS LTD
DOI: 10.1002/hep4.1947

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资金

  1. Deutsche Forschungsgemeinschaft [LA 4286/1-1]
  2. American Association for the Study of Liver Diseases, Clinical and Translational Research Fellowship in Liver Disease
  3. National Institutes of Health [K12 HD85036, R01 AA24726, R37 AA020703, U01 AA026939, U01 AA026939-04S1, P50 AA011999]
  4. Fond National de Recherche Scientifique Belgium [FRS-FNRS J.0146.17, T.0217.18]
  5. Federation Wallonie-Bruxelle, Action de Recherche Concertee [ARC18-23/092]
  6. Biomedical Laboratory Research and Development Service of the VA Office of Research and Development [BX004594]
  7. Biocodex Microbiota Foundation
  8. San Diego Digestive Diseases Research Center [P30 DK120515]

向作者/读者索取更多资源

Alcohol use contributes to the progression of liver disease through changes in the intestinal virome. Patients with alcohol use disorder (AUD) have a different virome composition compared to controls, and the virome signature is also different between patients with progressive and nonprogressive liver disease. The interactions between bacteriophages and their target bacteria play a role in the progression of alcohol-associated liver disease.
Alcohol use is a leading cause of chronic liver disease worldwide, and changes in the microbiome associated with alcohol use contribute to patients' risk for liver disease progression. Less is known about the effects of alcohol use on the intestinal viral microbiome (virome) and interactions between bacteriophages and their target bacteria. We studied changes in the intestinal virome of 62 clinically well-characterized patients with alcohol use disorder (AUD) during active alcohol use and after 2 weeks of alcohol abstinence, by extracting virus-like particles and performing metagenomic sequencing. We observed decreased abundance of Propionibacterium, Lactobacillus, and Leuconostoc phages in patients with active AUD when compared with controls, whereas after 2 weeks of alcohol abstinence, patients with AUD demonstrated an increase in the abundance of Propionibacterium, Lactobacillus, and Leuconostoc phages. The intestinal virome signature was also significantly different in patients with AUD with progressive liver disease, with increased abundance of phages targeting Enterobacteria and Lactococcus species phages compared with patients with AUD with nonprogressive liver disease. By performing moderation analyses, we found that progressive liver disease is associated with changes in interactions between some bacteriophages and their respective target bacteria. In summary, active alcohol use and alcohol-associated progressive liver disease are associated with changes in the fecal virome, some of which are partially reversible after a short period of abstinence. Progression of alcohol-associated liver disease is associated with changes in bacteriophage-bacteria interactions.

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