Functional Microbiomics Reveals Alterations of the Gut Microbiome and Host Co-Metabolism in Patients With Alcoholic Hepatitis.

Gao, Bei; Duan, Yi; Lang, Sonja; Barupal, Dinesh; Wu, Tsung-Chin; Valdiviez, Luis; Roberts, Bryan; Choy, Ying Yng; Shen, Tong; Byram, Gregory; Zhang, Ying; Fan, Sili; Wancewicz, Benjamin; Shao, Yan; Vervier, Kevin; Wang, Yanhan; Zhou, Rongrong; Jiang, Lu; Nath, Shilpa; Loomba, Rohit; Abraldes, Juan G; Bataller, Ramon; Tu, Xin M; Stärkel, Peter; Lawley, Trevor D; Fiehn, Oliver; Schnabl, Bernd

Gao, Bei; Duan, Yi; Lang, Sonja; Barupal, Dinesh; Wu, Tsung-Chin; Valdiviez, Luis; Roberts, Bryan; Choy, Ying Yng; Shen, Tong; Byram, Gregory; Zhang, Ying; Fan, Sili; Wancewicz, Benjamin; Shao, Yan; Vervier, Kevin; Wang, Yanhan; Zhou, Rongrong; Jiang, Lu; Nath, Shilpa; Loomba, Rohit; Abraldes, Juan G; Bataller, Ramon; Tu, Xin M; Stärkel, Peter; Lawley, Trevor D; Fiehn, Oliver; Schnabl, Bernd.

Afiliação

Gao B; Department of Medicine University of California San Diego La Jolla CA.
Duan Y; Department of Medicine University of California San Diego La Jolla CA.
Lang S; Department of Medicine VA San Diego Healthcare System San Diego CA.
Barupal D; Department of Medicine University of California San Diego La Jolla CA.
Wu TC; West Coast Metabolomics Center University of California Davis Davis CA.
Valdiviez L; Division of Mathematics University of California San Diego San Diego CA.
Roberts B; West Coast Metabolomics Center University of California Davis Davis CA.
Choy YY; West Coast Metabolomics Center University of California Davis Davis CA.
Shen T; West Coast Metabolomics Center University of California Davis Davis CA.
Byram G; West Coast Metabolomics Center University of California Davis Davis CA.
Zhang Y; West Coast Metabolomics Center University of California Davis Davis CA.
Fan S; West Coast Metabolomics Center University of California Davis Davis CA.
Wancewicz B; West Coast Metabolomics Center University of California Davis Davis CA.
Shao Y; Department of Cell and Regenerative Biology University of Wisconsin-Madison Madison WI.
Vervier K; Host-Microbiota Interactions Laboratory Wellcome Sanger Institute Wellcome Genome Campus Hinxton United Kingdom.
Wang Y; Host-Microbiota Interactions Laboratory Wellcome Sanger Institute Wellcome Genome Campus Hinxton United Kingdom.
Zhou R; Department of Medicine University of California San Diego La Jolla CA.
Jiang L; Department of Medicine VA San Diego Healthcare System San Diego CA.
Nath S; Department of Medicine University of California San Diego La Jolla CA.
Loomba R; Department of Medicine University of California San Diego La Jolla CA.
Abraldes JG; Department of Medicine University of California San Diego La Jolla CA.
Bataller R; Department of Medicine University of California San Diego La Jolla CA.
Tu XM; Department of Medicine University of Alberta Edmonton AB Canada.
Stärkel P; Division of Gastroenterology, Hepatology and Nutrition Department of Medicine Pittsburgh Liver Research Center University of Pittsburgh Medical Center Pittsburgh PA.
Lawley TD; Department of Biostatistics and Bioinformatics Department of Family Medicine and Public Health University of California San Diego San Diego CA.
Fiehn O; St. Luc University Hospital Université Catholique de Louvain Brussels Belgium.
Schnabl B; Host-Microbiota Interactions Laboratory Wellcome Sanger Institute Wellcome Genome Campus Hinxton United Kingdom.

Hepatol Commun ; 4(8): 1168-1182, 2020 Aug.

Article em En | MEDLINE | ID: mdl-32766476

ABSTRACT

ABSTRACT

Alcohol-related liver disease is a major public health burden, and the gut microbiota is an important contributor to disease pathogenesis. The aim of the present study is to characterize functional alterations of the gut microbiota and test their performance for short-term mortality prediction in patients with alcoholic hepatitis. We integrated shotgun metagenomics with untargeted metabolomics to investigate functional alterations of the gut microbiota and host co-metabolism in a multicenter cohort of patients with alcoholic hepatitis. Profound changes were found in the gut microbial composition, functional metagenome, serum, and fecal metabolomes in patients with alcoholic hepatitis compared with nonalcoholic controls. We demonstrate that in comparison with single omics alone, the performance to predict 30-day mortality was improved when combining microbial pathways with respective serum metabolites in patients with alcoholic hepatitis. The area under the receiver operating curve was higher than 0.85 for the tryptophan, isoleucine, and methionine pathways as predictors for 30-day mortality, but achieved 0.989 for using the urea cycle pathway in combination with serum urea, with a bias-corrected prediction error of 0.083 when using leave-one-out cross validation.

Conclusion:

Our study reveals changes in key microbial metabolic pathways associated with disease severity that predict short-term mortality in our cohort of patients with alcoholic hepatitis.

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Texto completo: 1 Bases de dados: MEDLINE Tipo de estudo: Clinical_trials Idioma: En Revista: Hepatol Commun Ano de publicação: 2020 Tipo de documento: Article