Continued Alcohol Misuse in Human Cirrhosis is Associated with an Impaired Gut-Liver Axis.

Bajaj, Jasmohan S; Kakiyama, Genta; Zhao, Derrick; Takei, Hajime; Fagan, Andrew; Hylemon, Phillip; Zhou, Huiping; Pandak, William M; Nittono, Hiroshi; Fiehn, Oliver; Salzman, Nita; Holtz, Mary; Simpson, Pippa; Gavis, Edith A; Heuman, Douglas M; Liu, Runping; Kang, Dae Joong; Sikaroodi, Masoumeh; Gillevet, Patrick M

Bajaj, Jasmohan S; Kakiyama, Genta; Zhao, Derrick; Takei, Hajime; Fagan, Andrew; Hylemon, Phillip; Zhou, Huiping; Pandak, William M; Nittono, Hiroshi; Fiehn, Oliver; Salzman, Nita; Holtz, Mary; Simpson, Pippa; Gavis, Edith A; Heuman, Douglas M; Liu, Runping; Kang, Dae Joong; Sikaroodi, Masoumeh; Gillevet, Patrick M.

Afiliación

Bajaj JS; Virginia Commonwealth University and McGuire VA Medical Center, Richmond, Virginia.
Kakiyama G; Virginia Commonwealth University and McGuire VA Medical Center, Richmond, Virginia.
Zhao D; Virginia Commonwealth University and McGuire VA Medical Center, Richmond, Virginia.
Takei H; Junshin Clinic Bile Acid Institute, Tokyo, Japan.
Fagan A; Virginia Commonwealth University and McGuire VA Medical Center, Richmond, Virginia.
Hylemon P; Virginia Commonwealth University and McGuire VA Medical Center, Richmond, Virginia.
Zhou H; Virginia Commonwealth University and McGuire VA Medical Center, Richmond, Virginia.
Pandak WM; Virginia Commonwealth University and McGuire VA Medical Center, Richmond, Virginia.
Nittono H; Junshin Clinic Bile Acid Institute, Tokyo, Japan.
Fiehn O; West Coast Metabolomics Center, Davis, California.
Salzman N; Medical College of Wisconsin, Milwaukee, Wisconsin.
Holtz M; Medical College of Wisconsin, Milwaukee, Wisconsin.
Simpson P; Medical College of Wisconsin, Milwaukee, Wisconsin.
Gavis EA; Virginia Commonwealth University and McGuire VA Medical Center, Richmond, Virginia.
Heuman DM; Virginia Commonwealth University and McGuire VA Medical Center, Richmond, Virginia.
Liu R; Virginia Commonwealth University and McGuire VA Medical Center, Richmond, Virginia.
Kang DJ; Virginia Commonwealth University and McGuire VA Medical Center, Richmond, Virginia.
Sikaroodi M; George Mason University, Manassas, Virginia.
Gillevet PM; George Mason University, Manassas, Virginia.

Alcohol Clin Exp Res ; 41(11): 1857-1865, 2017 Nov.

Article en En | MEDLINE | ID: mdl-28925102

RESUMEN

BACKGROUND: Cirrhosis and alcohol can independently affect the gut-liver axis with systemic inflammation. However, their concurrent impact in humans is unclear. METHODS: Our aim was to determine the effect of continued alcohol misuse on the gut-liver axis in cirrhotic patients. Age- and MELD-balanced cirrhotic patients who were currently drinking (Alc) or abstinent (NAlc) and healthy controls underwent serum and stool collection. A subset underwent upper endoscopy and colonoscopy for biopsies and duodenal fluid collection. The groups were compared regarding (i) inflammation/intestinal barrier: systemic tumor necrosis factor levels, intestinal inflammatory cytokine (duodenum, ileum, sigmoid), and ileal antimicrobial peptide expression; (ii) microbiota composition: 16SrRNA sequencing of duodenal, ileal, and colonic mucosal and fecal microbiota; and (iii) microbial functionality: duodenal fluid and fecal bile acid (BA) profile (conjugation and dehydroxylation status), intestinal BA transporter (ASBT, FXR, FGF-19, SHP) expression, and stool metabolomics using gas chromatography/mass spectrometry. RESULTS: Alc patients demonstrated a significant duodenal, ileal, and colonic mucosal and fecal dysbiosis, compared to NAlc and controls with lower autochthonous bacterial taxa. BA profile skewed toward a potentially toxic profile (higher secondary and glycine-conjugated BAs) in duodenal fluid and stool in Alc patients. Duodenal fluid demonstrated conjugated secondary BAs only in the Alc group. There was a greater expression of all ileal BA transporters in Alc patients. This group also showed higher endotoxemia, systemic and ileal inflammatory expression, and lower amino acid and bioenergetic-associated metabolites, without change in antimicrobial peptide expression. CONCLUSIONS: Despite cirrhosis, continued alcohol misuse predisposes patients to widespread dysbiosis with alterations in microbial functionality such as a toxic BA profile, which can lead to intestinal and systemic inflammation.

Asunto(s)

Alcoholismo/fisiopatología; Disbiosis/fisiopatología; Tracto Gastrointestinal/fisiopatología; Cirrosis Hepática/fisiopatología; Alcoholismo/diagnóstico; Alcoholismo/epidemiología; Disbiosis/diagnóstico; Disbiosis/epidemiología; Endoscopía del Sistema Digestivo/métodos; Femenino; Humanos; Cirrosis Hepática/diagnóstico; Cirrosis Hepática/epidemiología; Masculino; Microbiota/fisiología; Persona de Mediana Edad

Palabras clave

Bile Acids; Functionality; Inflammation; Metabolomics; Microbiota

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Texto completo: 1 Banco de datos: MEDLINE Asunto principal: Tracto Gastrointestinal / Alcoholismo / Disbiosis / Cirrosis Hepática Tipo de estudio: Diagnostic_studies / Risk_factors_studies Límite: Female / Humans / Male / Middle aged Idioma: En Revista: Alcohol Clin Exp Res Año: 2017 Tipo del documento: Article

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