HIV Clinical Trial
Official title:
Determination of Hepatitis C Prevalence, Genetic Diversity and Treatment Eligibility in an HIV Patient Cohort in Phnom Penh, Cambodia
Hepatitis C (HCV) is an important global public health problem, disproportionately affecting
HIV positive populations. Asia and Africa account for most of the co-infection burden, but
access to HCV screening and treatment is still very limited. It is expected though, with the
recent therapeutic advances and increasing global advocacy efforts, that HCV treatment
should become a feasible option in the near future.
Sihanouk Hospital Center of HOPE (Phnom Penh, Cambodia) is catering for one of the largest
HIV cohorts of the country, followed in an ambulatory settings. In this cohort, the
prevalence of HCV co-infection will be determined, as well as HCV genotype diversity and the
severity of liver disease. The researcher will also explore the performance of simple blood
tests/panels as predictors of significant fibrosis and/or cirrhosis.
Patients will attend two study-visits. All adult patients of the HIV patient cohort of SHCH
will be proposed HCV testing during their next HIV follow-up consultation, following the
latest algorithm of the Centre for Disease Control (CDC) (May 2013). Anamnesis and clinical
examination will focus, additionally to routine practice, on presence of general and HCV
liver-disease related features. Laboratory analyses will include basic HIV tests (CD4), and
tests for liver function such as Hepatitis B surface antigen (HbsAg) .
During the following routine HIV follow-up consultation, the results of HCV testing will be
explained to the patient. If the patient is HCV negative, his/her study participation ends
here. If currently infected with HCV, the clinician will repeat the HCV liver-disease
(extra-hepatic & hepatic) related anamnesis and clinical examination, and prescribe
additional blood tests for the non-invasive liver fibrosis/cirrhosis blood panel tests,
liver and kidney function. Patients will moreover be asked to undergo a liver ultrasound and
liver stiffness measurements.
Hepatitis C (HCV) is an important global public health problem, disproportionally affecting
HIV positive populations. Asia and Africa account for most of the co-infection burden, but
access to HCV screening and treatment is still very limited. The high cost and complexity of
current diagnostic and treatment algorithms are major bottlenecks and the linked lack of
accurate HCV prevalence estimates and treatment-need data do not allow for robust treatment
advocacy and program planning. Cambodia is not an exception.
It is expected though, with the recent therapeutic advances and increasing global advocacy
efforts, that HCV treatment should become a feasible option in the near future. Sihanouk
Hospital Center of HOPE (Phnom Penh, Cambodia) is catering for one of the largest HIV
cohorts of the country, and it is planning to engage in HCV treatment from 2014 2015
onwards, with a double objective of direct patient benefit and catalyst role at national
level, as in the past when starting its antiretroviral (ARV) program.
Within this specific setting, the researchers plan to determine the prevalence of HCV
co-infection, HCV genotype diversity and severity of liver disease in this HIV patient
cohort, followed in an ambulatory setting. The researchers will also explore the performance
of simple blood tests/panels as predictors of significant fibrosis and/or cirrhosis .
The current HCV diagnostic procedures (and tools), as applied in this study, are too
expensive and resource-demanding to allow for scalability in resource limited settings.
Thus, the researchers plan to set up during this study a biobank with samples of a
clinically well described HIV patient population. These samples should allow constituting a
well-balanced panel for evaluation of future 'more scalable' HCV diagnostic tools.
Patients will attend two study-visits. All adult patients of the HIV cohort will be proposed
HCV testing during their next regular HIV follow-up consultation. HCV testing will follow
the latest algorithm of the Centre for Disease Control (CDC) (May 2013). During this same
consultation, anamnesis and clinical examination will focus, additionally to routine
practice ,on presence of general and HCV liver-disease related features. Laboratory analyses
will also include basic HIV (CD4), and tests for liver function such as Hepatitis B surface
antigen (HbsAg).
During the following routine HIV follow-up consultation (2-3 months later), the results of
HCV testing will be explained to the patient. If the patient is HCV negative, his/her study
participation ends here. If currently infected with Hepatitis C, the clinician will repeat
the HCV liver-disease (extra-hepatic & hepatic) related anamnesis and clinical examination
and prescribe additional blood tests for the non-invasive liver fibrosis/cirrhosis blood
panel tests, liver and kidney function. Patients will moreover be asked to undergo a liver
ultrasound and liver stiffness measurements.
The biobank will be set up with left over biological samples (whole blood plasma and serum)
and comprehensive clinical information of all patients who give additional consent for this
scope. Both biological samples and clinical information will be coded, to ensure
confidentiality.
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Observational Model: Cohort, Time Perspective: Cross-Sectional
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