The Effect of Gut Sterilisation on Macrophage Activation in Patients With Alcoholic Hepatitis.
NCT ID: NCT03157388
Last Updated: 2019-05-23
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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COMPLETED
NA
15 participants
INTERVENTIONAL
2017-06-01
2018-12-01
Brief Summary
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This project investigates the effects of gut sterilisation with broad spectrum antibiotics in patients with AH
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Detailed Description
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The current perception of the pathogenesis of alcohol-induced liver injury mainly derives from animal models, and the resident hepatic macrophages, the Kupffer cells, seem to play an important role. Activation of these cells may give rise to most of the hallmark clinical findings of AH: The cytokines released initiate hepatic inflammation and an acute phase response, recruit neutrophils, and activate stellate cells, contributing to the acute portal hypertension. Jaundice is due to intrahepatic cholestasis caused by down regulation of the bilirubin transporters on the basolateral hepatocyte membrane. Hepatic macrophages are thought to be activated by the bacterial derived endotoxins/lipopolysaccharides (LPS) present in the portal blood because of an alcohol-induced increase in gut-blood permeability with translocation of bacteria, as found in patients with alcoholic liver injury. LPS is recognized by the hepatic macrophages via a membrane complex including the pathogen recognition receptor molecule Toll-like receptor 4 (TLR-4). LPS Binding Proteins (LBP) produced by hepatocytes then bind and present LPS to the membrane glycoprotein CD14 that in turn activates TLR-4. In support of these mechanisms, alcohol-induced liver injury is reduced in knockout mice missing LBP, CD14, and TLR-4. Likewise, chemical destruction of hepatic macrophages in rats prevents alcohol-induced liver injury, as does cleansing the gut flora with antibiotics.
Human hepatic macrophages when activated, express their surface receptor CD163. We and others have previously shown that sCD163 is released from the liver in alcoholic liver disease, that its plasma concentration predicts mortality in patients with acute liver failure and is as a marker of portal hypertension and a predictor of clinical decompensation in patients with liver cirrhosis. Very recently we have directly demonstrated hepatic macrophage activation in human AH paralleling the disease severity, and to suggest this to be elicited by LPS.
The line of evidence presented above provides rationale for testing whether intervention toward bacterial translocation may result in a diminished immune response in human AH. Consequently, in this study the investigators seek to perform total gut microbiota eradication by combining 3 different orally administered antibiotics. The investigators have chosen antibiotics that are not absorbed into the systemic circulation, because the investigators want to limit the effects to the gastrointestinal tract.
Conditions
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Study Design
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NA
SINGLE_GROUP
BASIC_SCIENCE
NONE
Study Groups
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Intervention
Combined Vancomycin and Gentamycin and Meropenem
Combined Vancomycin and Gentamycin and Meropenem
The following combined antibiotic regime will be administered for eradication of gut bacteria.
7 days combined antibiotic treatment, per oral route, once daily: vancomycin 500 mg (Vancomycin "Hospira"), powder for concentrate and gentamycin 40 mg ("Hexamycin®"), solution and meropenem 500 mg (Meropenem "Hospira"), powder for concentrate; The three drugs are dissolved and combined in approximately 100 ml of apple juice.
Interventions
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Combined Vancomycin and Gentamycin and Meropenem
The following combined antibiotic regime will be administered for eradication of gut bacteria.
7 days combined antibiotic treatment, per oral route, once daily: vancomycin 500 mg (Vancomycin "Hospira"), powder for concentrate and gentamycin 40 mg ("Hexamycin®"), solution and meropenem 500 mg (Meropenem "Hospira"), powder for concentrate; The three drugs are dissolved and combined in approximately 100 ml of apple juice.
Eligibility Criteria
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Inclusion Criteria
1. A history of excessive alcohol ingestion (10 units or more per day) until at least three weeks before admission
2. Acute jaundice (developed over at most 2 weeks, serum bilirubin \> 80 μmol/l).
3. liverbiopsy will be performed in case of doubt regarding the diagnosis.
Exclusion Criteria
2. Viral hepatitis,
3. Autoimmune liver disease,
4. Bile duct obstruction,
5. Liver tumours or any other cancer,
6. Presence of an infectious focus (either clinically assessed or based on chest x-ray, urine samples or ascites puncture),
7. On-going gastrointestinal bleeding or bleeding within the previous three months
8. Any prior immune-modulating therapy.
9. Any known gastrointestinal disease
10. Contraindications against/allergy towards the used antibiotics
18 Years
75 Years
ALL
No
Sponsors
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University of Aarhus
OTHER
Responsible Party
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Principal Investigators
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Hendrik D Vilstrup, Professor
Role: STUDY_DIRECTOR
Aarhus University Hospital
Locations
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Aarhus University Hospital
Aarhus, , Denmark
Countries
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Other Identifiers
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1-10-72-1-15
Identifier Type: -
Identifier Source: org_study_id
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