Hepatitis C, Chronic Clinical Trial
Official title:
Security and Efficacy of Triple Therapy Including Direct-Acting Antivirals Against Chronic Hepatitis C Infection In HIV-Coinfected Patients In Real-Life Conditions: The Prospective HEPAVIR Cohort.
The purpose of this study is to evaluate the efficacy and tolerability of DAA-based regimens
in the clinical practice in HIV/HCV-coinfected patients.
Hypothesis: The efficacy and tolerability of DAA-based regimens in the clinical practice is
different to what is observed in clinical trials in HIV/HCV-coinfected patients.
Treatment strategies aimed to achieve sustained virologic response (SVR) are of highest
priority in patients with chronic hepatitis C and HIV coinfection, since SVR leads to a
dramatic reduction in the incidence of hepatic decompensations and mortality in this
setting. Until recently, therapy against hepatitis C virus (HCV) was based on pegylated
interferon (peg-IFN) plus ribavirin (RBV). This combination prompt SVR only in approximately
50% of the HCV genotype 1 (HCV-1)-infected patients. Furthermore, it is costly and
associated with multiple and sometimes serious side effects. In the setting of
HIV/HCV-1-coinfection, rates of SVR are even lower and do not exceed 25% in the clinical
practice.
Considerable increases of SVR have been achieved recently with the arrival of direct acting
antivirals (DAA) against HCV. Among the first of these new agents are the protease
inhibitors telaprevir (TVR) and boceprevir (BOC), which are approved for HCV-1 infection.
Data obtained from clinical trials have demonstrated that the combination of peg-IFN/RBV
with TVR or BOC significantly augments SVR rates as compared to what is observed with
peg-IFN plus RBV only. As a consequence, triple therapy including peg-IFN, RBV plus TVR or
BOC has become the standard therapy for HCV-1-infected patients in our setting. In addition,
a number of further DAAs are currently in the final phases of development, as it is the case
for the protease inhibitors faldaprevir and simeprevir, the polymerase NS5B inhibitor
sofosbuvir and the NS5A inhibitor daclatasvir.
Although the considerable improvement of therapy outcome with DAA-including regimens is
giving a positive prospective, there are a number of questions that have to be solved as
soon as possible. On the one hand, the information on response to DAA in the coinfected
population is derived from clinical trials, which often do not reflect patient management in
the clinical practice. Also, the populations included in clinical trials are highly
selective and may lack the high proportion of difficult-to-treat individuals expected among
the candidate population, i.e., those who failed previous treatment and who bear compensated
cirrhosis. In fact, data derived from the French cohort CUPIC including HCV-monoinfected,
cirrhotic patients, show that tolerability and efficacy of TVR and BOC-based treatment is
lower than observed in pivotal trials. On the other hand, similar to dual therapy including
Peg-IFN/RBV, it is possible that both response rates and safety profiles of DAAs are not
comparable between HCV-monoinfected and HIV/HCV-coinfected patients. In this context, the
coinfected population has singularities as the coadministration of antiretroviral therapy,
that may cause drug-drug-interactions and decreased tolerability, thus resulting in
diminished efficacy. Finally, it is of highest relevance to identify predictive factors for
treatment response in the new DAA-based regimens in order to individualize treatment
decision and duration of therapy.
Due to the above mentioned, studies on safety and efficacy of DAA-based therapy under real
life conditions in HIV/HCV-coinfected patients are urgently needed.
Primary objectives:
- To determine the efficacy of DAA-based therapy in the clinical in patients with chronic
hepatitis C and HIV coinfection.
- To determine the security of DAA-based therapy in the clinical in patients with chronic
hepatitis C and HIV coinfection.
Secondary objectives:
- Identification of predictive factors for response to DAA-based treatment in the studied
population.
- Compare security and efficacy of the different DAAs used.
- Evaluate the on-treatment HCV kinetics for the different regimens.
Scheduled visits: 0, 1, 2, 4, 8, 12, 24, 36 and 48 weeks, as well as 12 and 24 weeks
post-treatment.
Definition SVR: Undetectable HCV-RNA 24 weeks after scheduled end of treatment.
Definition of hepatic fibrosis:
- advanced fibrosis: F3 as determined by liver biopsy or 11 kilopascals as determined by
transient elastometry
- cirrhosis: F4 as determined by liver biopsy or 14.6 kilopascals as determined by
transient elastometry
Variables collected within in the cohort:
- primary outcome variable: SVR (efficacy study) and % of patients who discontinued
therapy due to adverse events (safety study)
- epidemiological variable: age, sex, interleukin 28B rs12979860 genotype
- variables related to hepatitis C virus-infection: infection route, genotype, grade of
hepatic fibrosis and method used for its determination, baseline Child-Pough-Index,
previous hepatic decompensations
- treatment-related variables: previous response to treatment, doses and dose
reductions/discontinuations of peg-IFN, RBV and the DAA(s), overall severe adverse
events, adverse events that occur in more than 5% of the patients, hepatic
decompensations, deaths, HCV viral load at baseline and at each visit
- variables related to HIV-infection: Centers for Disease Control and Prevention (CDC)
category, HIV viral load, cluster of differentiation 4 (CD4) cell count, antiretroviral
regimen
- analytical variables: aspartate aminotransferase (AST), alanine aminotransferase (ALT),
platelets, leucocytes, low-density lipoprotein cholesterol, bilirubin,
gamma-glutamyltransferase (GGT), alkaline phosphatase,
- clinical variables: alcohol intake Quality assurance and data checks: Data will be
obtained from controlled databases at the participating centers. Databases will be
monitored and controlled by queries every three months. Descriptive statistics will be
be applied in order to detect transcription errors.
Source data verification: not planned.
All grade 3 or 4 adverse events, as well as all unexpected events, will be reported to the
Andalusian Center for Pharmacovigilance (Centro Andaluz de Farmacovigilancia, www.cafv.es).
A sample size of 230 is planned for this study.
Statistical analysis: The outcome variables of this study will be the achievement of SVR, as
well as the development of severe adverse events during follow-up. Descriptive statistical
analysis will be performed in order to describe the cohort. Continuous variables will be
expressed as median [interquartile range (IQR)] and categorical variables as number
[percentage; 95% confidence interval (CI)]. The association of continuous variables with SVR
or the frequency of patients who discontinue therapy will be analyzed using the Student's
t-test for normal distribution and the Mann-Whitney U-test otherwise whereas the
relationship with categorical variables will be determined applying the χ2-test or the
Fisher's test, when applicable. Those factors that show an association in the univariate
analysis with a p<0.2, as well as those with a biologically possible influence, will be
entered logistic regression in order to identify independent predictors for SVR. The
adjusted odds ratio (AOR) and the respective 95% CI will be calculated. All p values <0.05
will be considered statistically significant. Data will be analyzed using the SPSS
statistical software package release 19.0 (SPSS Inc., Chicago, Illinois, USA) and STATA 9.0
(StataCorp, College Station, Texas, USA).
Sample size calculations: Estimating a SVR rate of 55%, with a confidence interval of 95%
and a lost-to-follow-up rate of 5%, a minimum of 230 patients should be included in order to
obtain a precision of 5%.
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Observational Model: Cohort, Time Perspective: Prospective
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