Targeting the gut-liver-immune axis to treat cirrhosis

Targeting the gut-liver-immune axis to treat cirrhosis

Cirrhotic portal hypertension is characterised by development of the decompensating events of ascites, encephalopathy, portal hypertensive bleeding and hepatorenal syndrome, which arise in a setting of cirrhosis-associated immune dysfunction (CAID) and define morbidity and prognosis. CAID describes...

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Veröffentlicht in:Gut 2021-05, Vol.70 (5), p.982-994
Hauptverfasser: Tranah, Thomas Henry, Edwards, Lindsey A, Schnabl, Bernd, Shawcross, Debbie Lindsay
Format: Artikel
Sprache:eng
Schlagworte:
Antigens
Antimicrobial agents
Ascites
bacterial interactions
bacterial translocation
Bile
chronic liver disease
Cirrhosis
Digestive system
Dysbacteriosis
Encephalopathy
Fatty acids
Gastrointestinal tract
Genomes
gut immunology
Hemorrhage
Immune system
Immunoglobulins
Immunology
Inflammation
Intestinal microflora
Intestine
Liver cirrhosis
Liver diseases
Metabolism
Metabolites
Microbiomes
Microbiota
Morbidity
Mortality
Motility
Mucosal immunity
Pathogens
Peptides
Peritonitis
Phenotypes
Proteins
Recent advances in clinical practice
Roles
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creator Tranah, Thomas Henry
Edwards, Lindsey A
Schnabl, Bernd
Shawcross, Debbie Lindsay
description Cirrhotic portal hypertension is characterised by development of the decompensating events of ascites, encephalopathy, portal hypertensive bleeding and hepatorenal syndrome, which arise in a setting of cirrhosis-associated immune dysfunction (CAID) and define morbidity and prognosis. CAID describes the dichotomous observations that systemic immune cells are primed and display an inflammatory phenotype, while failing to mount robust responses to pathogen challenge. Bacterial infections including spontaneous bacterial peritonitis are common complications of advanced chronic liver disease and can precipitate variceal haemorrhage, hepatorenal syndrome and acute-on-chronic liver failure; they frequently arise from gut-derived organisms and are closely linked with dysbiosis of the commensal intestinal microbiota in advanced chronic liver disease.Here, we review the links between cirrhotic dysbiosis, intestinal barrier dysfunction and deficits of host-microbiome compartmentalisation and mucosal immune homoeostasis that occur in settings of advanced chronic liver disease. We discuss established and emerging therapeutic strategies targeted at restoring intestinal eubiosis, augmenting gut barrier function and ameliorating the mucosal and systemic immune deficits that characterise and define the course of decompensated cirrhosis.
doi_str_mv 10.1136/gutjnl-2020-320786
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CAID describes the dichotomous observations that systemic immune cells are primed and display an inflammatory phenotype, while failing to mount robust responses to pathogen challenge. Bacterial infections including spontaneous bacterial peritonitis are common complications of advanced chronic liver disease and can precipitate variceal haemorrhage, hepatorenal syndrome and acute-on-chronic liver failure; they frequently arise from gut-derived organisms and are closely linked with dysbiosis of the commensal intestinal microbiota in advanced chronic liver disease.Here, we review the links between cirrhotic dysbiosis, intestinal barrier dysfunction and deficits of host-microbiome compartmentalisation and mucosal immune homoeostasis that occur in settings of advanced chronic liver disease. 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subjects Antigens
Antimicrobial agents
Ascites
bacterial interactions
bacterial translocation
Bile
chronic liver disease
Cirrhosis
Digestive system
Dysbacteriosis
Encephalopathy
Fatty acids
Gastrointestinal tract
Genomes
gut immunology
Hemorrhage
Immune system
Immunoglobulins
Immunology
Inflammation
Intestinal microflora
Intestine
Liver cirrhosis
Liver diseases
Metabolism
Metabolites
Microbiomes
Microbiota
Morbidity
Mortality
Motility
Mucosal immunity
Pathogens
Peptides
Peritonitis
Phenotypes
Proteins
Recent advances in clinical practice
Roles
title Targeting the gut-liver-immune axis to treat cirrhosis
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