Chronic Hepatitis C Clinical Trial
Official title:
Prospective Randomized Pilot Study of Daily Consensus Interferon (CIFN) and Ribavirin for 52 Wks vs Extended Duration 72 Wks Based on Virologic Response for the Initial Treatment of Difficult-to-treat Patients With Chronic HCV Genotype 1
Data have suggested that consensus interferon (CIFN) has greater antiviral activity in vitro compared with interferon alfa-2a or alfa-2b. Several clinical studies also suggest that CIFN has greater antiviral activity in patients with genotype 1 hepatitis C infection, particularly if given as a daily injection. These data indicate that the use of a regimen of daily CIFN and ribavirin will lead to greater virologic response rates compared with pegylated interferon alfa-2b and ribavirin in patients with genotype 1 infection, with comparable adverse events. Emerging data indicate that HCV genotype 1 patients with a delayed virologic response to initial therapy may benefit from an extended duration of therapy. Therefore, the goals of this pilot study are to determine the tolerability and efficacy of daily CIFN plus ribavirin when given for 52 weeks or an extended duration of therapy. The target population will consist of "difficult-to-treat" patients, defined as having the following characteristics: genotype 1, a North American patient population, predominantly male gender, and no specific exclusions for pre-existing psychiatric or substance abuse co-morbidities.
Current treatment for hepatitis C is a pegylated interferon alfa plus ribavirin. This
treatment is inadequate for patients with HCV genotype 1, since the majority of patients do
not respond (termed non-responders) or respond but relapse (termed relapsers) following
termination of these treatments. Data from the Veterans Health Administration (VHA)
Hepatitis C Registry and community hospitals indicate that the large majority of patients
identified with hepatitis C have characteristics associated with a poor treatment response
and remain untreated at this time. Data have suggested that consensus interferon (CIFN, CIFN
or interferon alfacon-1) has greater antiviral activity in vitro compared with interferon
alfa-2a or alfa-2b. Preliminary data indicate that more patients with genotype 1 can respond
to CIFN and ribavirin than current standard treatments, due to the fact that approximately
25% of patients who are nonresponders to pegylated interferon and ribavirin may have a
sustained response to a regimen of daily CIFN and ribavirin. Furthermore, difficult to treat
patients may benefit from a longer duration of therapy than the standard 48 week regimen
based on when an initial virologic response to therapy occurs.
Aims: To determine the safety and efficacy of (A) daily CIFN (15 mcg/d sq) and ribavirin
(1-1.2 gm/d PO) given for 52 weeks, vs (B) daily CIFN (15 mcg/d sq) and ribavirin (1-1.2
gm/d PO) given for 52 to 72 weeks for treatment-naïve patients with hepatitis C genotype 1,
with treatment duration based on the virologic response during the initial 24 weeks.
Methods: Patients who meet eligibility criteria will be stratified by race and randomized to
one of two treatment arms, and all patients will have viral kinetics measured by
quantitative PCR at weeks 4,8,12,16,20 and 24. Patients in treatment arm A will follow
"standard" stopping rules, i.e., if there is not a 2-log drop in viremia by 12 weeks the
treatment will be discontinued, otherwise they will all receive 52 weeks of treatment if
they also are qualitative PCR negative by week 24. In treatment arm B the patients will be
monitored monthly until they have a virologic response (defined as >2 log drop in viral
levels from baseline) by quantitative PCR for up to 24 weeks. Once they have a virologic
response by quantitative PCR their treatment will be continued for an additional 48 weeks.
In both groups, treatment will be stopped if the patients do not become negative for HCV RNA
by qualitative PCR by 24 weeks on therapy. A total of 192 patients at up to 10-20 sites will
be recruited. The primary endpoint would be the number who achieve a sustained virologic
response; secondary endpoints are the percentage of patients who complete therapy, have
significant adverse events, and the relationship of early virologic response at each 4 week
period between 4 and 24 weeks and those who achieve a sustained virologic response.
Sample size determination: To detect an absolute difference of 20% or more in sustained
virologic response between treatment arms A and B; the Log-rank test is performed at the
alpha level of .05 and the test is maintained at least 80 percent statistical power; it is
estimated that a total of 96 patients in each treatment arm will be required.
Analysis: Univariate and multivariate analysis will be used to determine factors associated
with final endpoints. Subgroup analyses will be done based on time to early virologic
response and duration of therapy each stratification. The primary and secondary endpoints
will be determined on an intention-to-treat basis starting with all patients that receive at
least one dose of study medications. The primary and secondary endpoints will also be
determined in a per-protocol analysis on those patients who take 80% of the prescribed CIFN
and 80% of the prescribed ribavirin for 80% of the time.
Significance: The current initial treatment of pegylated interferon alfa and ribavirin for
patients with hepatitis C who are genotype 1 and have other "difficult-to-treat"
characteristics is inadequate. The results of this trial are needed to demonstrate the
safety and efficacy of two regimens of daily CIFN and ribavirin. Since the large majority of
hepatitis C patients in VA and other community hospitals fall into this category, the
results of this trial may influence the potential treatments recommended for these patients.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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