Liver Cirrhosis Clinical Trial
Official title:
A Placebo Controlled Single Centre Double Blind Randomised Trial to Investigate the Efficacy of Rifaximin Versus Placebo in Improving Systemic Inflammation and Neutrophil Malfunction in Patients With Cirrhosis and Chronic Hepatic Encephalopathy
Patients with cirrhosis are particularly prone to infection which is frequently a
precipitant of hepatic encephalopathy, renal failure and circulatory collapse. Bacterial
infections are of particular concern in patients with cirrhosis because they are poorly
tolerated. Sepsis and associated endotoxaemia whereby bacteria produce inflammatory
particles occur in approximately 40% of hospitalized patients with cirrhosis and is a major
cause of death.
Gut-derived and blood-borne pathogens can induce an inflammatory response within the liver
and spleen, which are the major organs that remove bacteria and their endotoxin (such as
lipopolysaccharide - LPS and bacterial DNA itself) from the bloodstream. Several mechanisms
have been identified and proposed in this process which depends upon a balance between the
barrier functions of the gut and the 'detoxifying' capacity of the liver. People with
established liver cirrhosis have been shown to have escape of endotoxin into the bloodstream
produced by bacteria that reside in their intestines, which becomes more permeable or
'leaky'.
Gut dysfunction is defined by changes in the types of bacteria within the gut and in overall
permeability allowing bacterial products which would otherwise be contained within the gut
to travel into the bloodstream and lymphatic system with detrimental effects elsewhere in
the body. This passage of bacterial products is termed bacterial translocation, and it's
effects on the liver and general immune system can be then be measured.
It has now become recognised that certain types of white blood cells such as neutrophils and
monocytes become dysfunctional and this predisposes to infection and may also have a more
direct pathogenic role in hepatic encephalopathy. Thus neutrophil and monocytes may be a
novel pharmacotherapeutic target in a condition where current therapies such as bowel
aperients (e.g. lactulose) are inadequate. A therapeutic strategy utilising Rifaximin, a
non-absorbable antibiotic, to modulate gut bacterial which produce ammonia, a chemical known
to be important in the cause of hepatic encephalopathy, could potentially lower gut-derived
systemic inflammation, endotoxaemia, infection and organ dysfunction in this population
improving outcomes and prolonging transplant-free survival.
We therefore plan to test if Rifaximin positively affects markers of immune dysfunction in
patients with liver cirrhosis experiencing chronic hepatic encephalopathy after 30 days of
treatment, as our primary research question.
Positive results from this study would support further trials into the potential benefit of
using Rifaximin to improve immune function, as well as reduce the recurrence of hepatic
encephalopathy, in patients with liver cirrhosis.
Overview
The study will be designed and conducted as a double blind placebo controlled randomised
controlled trial - Clinical Trial of an Investigational Medicinal Product.
This study will be performed on patients referred to King's Liver Unit for further
assessment and management of chronic overt hepatic encephalopathy (≥ Grade 1) or with ≥2
episodes of overt hepatic encephalopathy in the previous 6 months.
The study will be performed on 50 patients with cirrhosis and chronic hepatic encephalopathy
[25 Rifaximin and 25 placebo] aged between 18 and 75 years managed within the Liver Unit at
King's College Hospital which is the largest tertiary Liver Transplant Centre within the UK.
For the purposes of this study a patient will be considered to have cirrhosis if they fulfil
2 out of 3 diagnostic criteria of confirmatory liver histology, biochemistry and/or
radiologic findings consistent with cirrhosis/portal hypertension, and are presenting with
chronic persistent overt hepatic encephalopathy (≥ grade 1) or with ≥2 episodes of overt
hepatic encephalopathy in the previous 6 months.
Patient demographics, clinical details (including Westhaven hepatic encephalopathy grade)
and blood haematology, biochemistry (including venous ammonia), microbiology data and
neutrophil function will be assessed and collated at baseline and following 30 and 90 days
of Rifaximin therapy or placebo. Intestinal permeability will be assessed using the
intestinal disaccharide test. Faecal microbiota analysis will be performed by deep
pyrosequencing techniques and plasma endotoxemia will be measured (lipopolysaccharide
levels) with bacterial DNA quantification as a marker of bacterial translocation. These will
all be measured at 3 time points: baseline and at 30 and 90 days after initiation of
Rifaximin therapy or matching placebo.
Investigations
Patients will undergo intestinal functional tests within 7 days of recruitment, whereby they
will be administered a test solution of not more than a cupful (150mls) of different types
of non-absorbable sugars, which are drunk in liquid form by the participants. Prior to
ingestion, baseline samples will be obtained as follows:
i) blood samples - for analysis of intestinal & immune (dys)function, and metabonomic
analysis ii) urine sample - for intestinal (dys)function & metabonomic analysis iii) stool
sample - for faecal biomarker and microbiota analysis
1v) ascitic sample (if clinically indicated) - surplus fluid will be analysed for bacterial
translocation and immune (dys)function
Once the test solution has been ingested, blood samples will be obtained via a cannula which
is placed in a vein, usually in the arm, prior to the start of the test, to allow further
sampling without causing discomfort to the patient. A total of 15 samples will be obtained
over a 5 hour period, with intervals ranging between 20-30mins, of not more than 6mls per
sample. At the end of the test, at a 5 hour interval, a further urine sample will be
collected to allow for intestinal functional testing. This is exactly the same procedure as
that specified in the approved 'The Gut-Liver Axis in Liver Disease & Liver Transplantation'
study (REC ref: 12/LO/1417).
Where participants are undergoing sampling of ascitic fluid for clinical reasons any fluid
in excess of pathology's requirements will be analysed along with peripheral blood samples.
Ascitic samples will only be taken from patients in whom a decision has been made to take
these samples for clinical reasons (this decision will not be that of the investigator). No
increased volume of such sample would be required.
Clinical outcomes (development of recurrent overt hepatic encephalopathy, organ failure and
infection) will be recorded for a total of 90 days.
Analysis of samples - sites
Blood, urine and ascitic samples will be analysed in the Institute of Liver Studies and
King's College Hospital laboratories where various tests to determine intestinal and immune
function will be undertaken. Stool samples will be analysed both at laboratories at King's
College Hospital and at the Franklin-Wilkins Building, King's College London, where faecal
biomarkers and faecal microbiota analyses will be performed, respectively. Metabolic
analyses for metabonomic profiling will be carried out at Imperial College London (both at
St Mary's Hospital and at the South Kensington Campus).
Protocol
A more detailed list of the tests and analyses to be performed is to be found in the
protocol. Study-specific flow charts have also been provided for a step-by-step
representation of the study, visually representing the study process including participant
recruitment, randomisation, sampling protocols and analyses at the three time points and
follow-up visits.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator), Primary Purpose: Basic Science
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