Hepatitis C Clinical Trial
Official title:
Insulin Resistance Associated With Chronic Hepatitis C (CHC) and the Effect of Anti-Viral Therapy
The literature suggests that there may be an association between hepatitis C and type 2
diabetes mellitus independent of the presence of cirrhosis, the likely mechanism for which
is insulin resistance. The prevalence of insulin resistance in patients with hepatitis C is
unknown. Furthermore, there are no studies that indicate an increased prevalence of insulin
resistance in patients with hepatitis C compared to other etiologies of liver disease. The
role that hepatitis C may have in the development of insulin resistance is unclear. The
effect of antiviral therapy for hepatitis C virus on insulin resistance has not been
addressed. The long-term consequence of insulin resistance is type 2 diabetes mellitus.
There is significant morbidity and mortality from type 2 diabetes mellitus in the general
population, and similar complications would be expected in patients with hepatitis C and
insulin resistance particularly if they develop type 2 diabetes mellitus.
Our hypothesis: The prevalence of insulin resistance is increased in patients with chronic
hepatitis C compared to chronic hepatitis B. Secondarily, insulin resistance when present in
patients with chronic hepatitis C improves with successful antiviral therapy.
This study has two phases. The first phase of our study will be to estimate the prevalence
of insulin resistance in individuals with chronic hepatitis C without cirrhosis compared to
patients with chronic hepatitis B without cirrhosis. The second phase of the study will be
restricted to those patients with hepatitis C found to be insulin resistant from phase 1, in
the absence of known risk factors for insulin resistance (cirrhosis, diabetes). The effect
on insulin resistance of anti-viral therapy to eradicate hepatitis C will be assessed.
The first phase will include patients with hepatitis C who are candidates for anti-viral
treatment, and patients with chronic hepatitis B who have undergone a recent liver biopsy
showing hepatitis without cirrhosis, with equal numbers in each group (100/ group).
Phase 2 (40 patients)- Patients with hepatitis C found in phase 1 by the HOMA test to have
increased insulin resistance will be recruited to phase 2 (interventional phase). Patients
with HBV infection will not be studied further.
The study will be conducted at a single center using an open-label design. All patients will
be treatment naïve. Up to 40 patients will be treated per current standard of care with
combination pegylated interferon alfa and ribavirin (Phase 2). Patients with genotype 2 or 3
will be treated with combination weekly Pegasys with a daily Copegus dose of 800 mg given
for 24 weeks (Group A). Patients with genotype non-2 or 3 will be treated with combination
weekly Pegasys with a daily Copegus dose of 1000-1200 mg given for 48 weeks (Group B). Both
groups will have an untreated follow-up period of 24 weeks. Pegasys will be administered sc
once weekly (180 microg in 0.5 or 1 mL solution) and Copegus will be taken po daily in split
doses of 400 mg in the morning and 400 mg in the evening (i.e., 2 tablets of 200 mg bid).
For doses of 1000 mg (genotype non- 2 or 3 patients whose body weight < 75 kg) Copegus will
be administered po daily: 400 mg (i.e. 2 tablets of 200 mg) in the morning and 600 mg (i.e.
3 tablets of 200 mg) in the evening. For genotype non-2 or 3 patients whose body weight is
75 kg, 600 mg (i.e. 3 tablets of 200 mg) in the morning and 600 mg (i.e. 3 tablets of 200
mg) in the evening is recommended. All patients in this study will receive Copegus treatment
with food. By definition, Copegus “with food” means taking their doses within 1 hour before
or 2 hours after a meal. The meal should be considered “regular” as opposed to
“fat-restricted”.
All 40 patients who meet inclusion criteria will also have indices of body fat assessed
through calculation of their BMI, DEXA scanning, and waist-to-hip circumference
measurements. Prior to therapy all patients will undergo the OGTT , which is a dynamic test
for insulin resistance providing accurate information on the relationship between insulin
and glucose.
At week 12 of treatment patients will have a quantitative assessment of HCV viral load and a
second OGTT . The current standard of therapy is to discontinue anti-viral therapy in
patients with genotype 1 or 4 without a ≥ 2-log fall in HCV RNA. Those who have a ≥ 2-log
fall in HCV RNA are expected to have a SVR. Patients to be continued on anti-viral therapy
will then be followed to SVR.
Twenty-four weeks after completion of anti-viral therapy, a OGTT will be repeated (SVR
OGTT). The effect of viral clearance on insulin resistance will be assessed by comparing the
OGTT at SVR (SVR OGTT) to pre-treatment OGTT.
Patients who are Non-Responders should also be assessed for safety 4-8 weeks after their
last dose of test medication following premature discontinuation from the study.
Non-Responders are defined as patients without a 2-log drop in PCR between baseline and week
12 or a positive PCR at their last visit. Responders should be followed for until Week 48
(Group A patients) or Week 72 (Group B patients). Responders are defined as patients who
have a 2-log drop in PCR between baseline and week 12 and a negative PCR at their last
visit. Female patients receiving Copegus should continue to do the home-based pregnancy test
every 4 weeks for the 6-month period after the last dose of study drug.
Efficacy assessments consist of serum HCV-RNA via PCR. Quantitative viral titers (AMPLICOR
HCV MONITOR Test, v2.0) will be obtained at Weeks 0 and 12 from all patients. Qualitative
HCV-RNA results (AMPLICORÒ HCV Test, v2.0) will be obtained at treatment period Week 24 for
all patients and Week 48 for group B; in addition during follow-up at week 24 for all
patients.
Insulin resistance as determined by the OGTT method will be assessed prior to initiation of
therapy, at 12 weeks of therapy, and during follow-up at week 24 for all patients.
Study Outcome:
Phase 1 - To evaluate the prevalence of insulin resistance in patients with hepatitis C
without cirrhosis and compare it to that observed in patients with hepatitis B also without
cirrhosis.
Phase 2 - Interventional phase - To evaluate the effect of anti-viral therapy on insulin
resistance, determined by the OGTT method, in patients with hepatitis C found to have
insulin resistance pre-treatment.
- To evaluate the safety, efficacy and tolerability of Pegasys (peginterferon alfa-2a) given
in combination with Copegus (ribavirin) given for 24 weeks or 48 weeks in treatment naïve
patients with chronic hepatitis C (CHC).
;
Allocation: Non-Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment
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