Hepatitis C, Chronic Clinical Trial
Official title:
Hepatic Safety of Currently Used Antiretroviral Regimens in HIV-infected Patients With Chronic Hepatitis B and/or Hepatitis C Under Real Life Conditions: The HEPAVIR HEPATIC SAFETY Cohort.
The purpose of this study is to compare the liver toxicity in HIV-infected patients with chronic hepatitis B and/or hepatitis C, who start a new antiretroviral drug regimen, as well as the influence of the degree of pre-existing liver fibrosis on the incidence of liver toxicity.
In the last years, various clinical trials and studies have evaluated the incidence of
hepatic toxicity (HT) associated with the commonly used antiretroviral drugs in the
HIV/hepatitis C virus (HCV)-infected population. Unfortunately, clinical trials that
compared hepatic safety of these antiretrovirals include a low number of coinfected patients
(van Leth 2004, Molina 2010, Ortiz 2008, Rockstroh 2012). According to recent cohort
studies, rates of grade 3 or 4 transaminase elevations (TE) observed in patients receiving
ritonavir-boosted protease inhibitors PI/r as lopinavir (LPV/r), atazanavir (ATV/r),
fosamprenavir (FPV/r) and darunavir (DRV/r) are similar to those observed in individuals
that receive efavirenz (EFV) or raltegravir (RAL) (Pineda 2008, Palacios 2006, Macías 2011,
Neukam 2011). However, this conclusion may not be exact due to methodological problems. In
this context, currently available data on severe TE are derived from cohort studies that
were conducted in different populations, with distinct methods and/or data that was
collected retrospectively.
Little information is available on whether the stage of liver damage influences the
incidence of HT caused by antiretroviral drugs. Although two studies found an association
between advanced fibrosis and higher rates of TE (Aranzabal 2005, Mira 2006), data obtained
by further studies are contradictory (Pineda 2008, Palacios 2006, Macías 2011, Neukam 2011)
and there are still open questions. Thus, the number of cirrhotic patients is considerably
small in these cohorts, however, cirrhosis represents an important comorbidity in HIV. In
these individuals, plasmatic concentrations of antiretroviral drugs could reach toxic levels
which would be reflected in TE (Barreiro 2007).
Therefore, studies conducted in the same population and with the same methodology are
required in order to obtain precise and reliable information on hepatic safety of all
commonly used antiretroviral drugs in the clinical practice. These findings could contribute
to a better understanding of differences between antiretrovirals and could therefore improve
the individualization of antiretroviral therapy in individuals with chronic hepatitis B
and/or C. Therefore, the HEPAVIR group of the Andalusian Society of Infectious Diseases
(SAEI) has established a prospective cohort: The HEPAVIR Cohort.
Hypothesis: The incidence of severe TE associated with antiretroviral therapy in the
clinical practice in hepatitis B virus and/or hepatitis C virus-coinfected patients could be
different according to the administered drug.
Primary objective: To determine the incidence of grade 3 or 4 TE associated with
antiretroviral therapy in the clinical practice in patients with viral hepatitis.
Secondary objectives:
- Identification of factors associated with grade 3 or 4 TE
- Analysis of the association between TE and pre-existing hepatic damage
- Evaluate the incidence of serious symptoms, including hepatic decompensations, acute
fulminant hepatitis and death due to liver failure, associated with the antiretroviral
drug
- Determination of the incidence of grade 3 or 4 bilirubin elevations associated with the
antiretroviral drugs
- Evaluation of efficacy of the antiretroviral drugs used in the study
Scheduled visits: 0, 4, 12, 24, 36 and 48 weeks.
Definition of grade 3 or 4 laboratory abnormalities/data dictionary: Grade 3 transaminase
elevations (TE) are considered when elevations between 5 and 10 times above the upper level
of normality (ULN) are presented in patients with normal baseline levels of
alanine-aminotransferase (ALT) and aspartate-aminotransferase (AST). Grade 4 TE are defined
as ALT or AST values >10 times of the ULN. In patients with elevated baseline ALT or AST
levels, 3.5- to 5-fold increase from baseline levels are considered grade 3 TE and >5-fold
elevations grade 4 TE, respectively. Grade 4 total bilirubin elevations were defined as
increases of total bilirubin ≥5 mg/dl.
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: AST, ALT
- epidemiological variable: age, sex
- 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
- variables related to HIV-infection: Centers for Disease Control and Prevention (CDC)
category, HIV viral load, cluster of differentiation 4 (CD4) cell count, previous and
new antiretroviral drugs
- analytical variables: platelets, cholesterol, bilirubin, gamma-glutamyltransferase
(GGT), alkaline phosphatase
- clinical variables: alcohol intake
- time to TE
- percentage of patients who discontinued antiviral therapy due to TE
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 six
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 500 is planned for this study.
Statistical analysis:
The outcome variables of this study will be the development of grade 3 or 4 transaminase
elevations (TE) and grade 4 total bilirubin elevations (TBE) during follow-up. Comparative
analyses of TE and TBE will be carried out between the different drug groups. Additionally,
the relationship between the outcome variable and the following potential predictors will be
assessed: age, sex, previous intravenous drug use, alcohol consumption, baseline ALT levels,
baseline CD4 cell count, CDC category C, undetectable plasma HIV-RNA, HCV genotype, previous
ART, type of drug, as well as significant fibrosis and cirrhosis at initiation of the new
ART regimen. Continuous variables will be expressed as median [interquartile range (IQR)]
and categorical variables as number [percentage; 95% confidence interval (CI)]. The density
of incidence of grade 3-4 TE will be calculated as number of cases per 100 person-years of
the follow-up. Continuous variables will be compared using the Student's t-test for normal
distribution and the Mann-Whitney U-test otherwise, whereas the categorical variables will
be analyzed applying the χ2-test or the Fisher's test, when applicable. The Wilcoxon Signed
Rank test and the McNemar test will be applied to compare repeated measurements in
continuous and categorical variables, respectively. 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 into a logistic regression model in order to identify independent
risk factors for grade 3-4 TE and grade 4 TBE. 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 analysed using the SPSS statistical software package release 19.0
(SPSS Inc., Chicago, IL, USA) and STATA 9.0 (StataCorp LP, College Station, TX, USA).
;
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