Hepatitis C Clinical Trial
Official title:
A Randomized Trial of Telaprevir, Peginterferon, and Ribavirin Versus Peginterferon and Ribavirin for Treatment of Genotype 1 Hepatitis C Virus With Host Interleukin 28B CC Polymorphism
Chronic hepatitis C is a major cause of liver disease and is thus an important public health
problem. Although some strains (genotypes) of the hepatitis C virus are highly responsive to
treatment with a combination of peginterferon and ribavirin, the most common form of the
virus (genotype 1) is relatively resistant to this treatment. Recently, telaprevir has been
approved by the Food and Drug Administration to be given in combination with peginterferon
and ribavirin. This 3-drug combination boosts the remission rate for genotype 1 hepatitis C
to that seen with other more responsive hepatitis C genotypes treated with only
peginterferon and ribavirin. However, telaprevir has additional side affects such as rash
and anemia that may limit its usefulness. Intriguingly, about one third of patients infected
with genotype 1 hepatitis C, who have a specific variation (polymorphism) in the DNA
sequence (CC) near an immune response gene (IL28B), in fact are highly responsive to 2-drug
treatment with peginterferon and ribavirin. This raises the possibility that individuals who
have the IL28B CC polymorphism may not need to be treated with the addition of telaprevir
and could therefore be spared unnecessary side effects. Thus, the purpose of this study is
to determine among genotype 1 hepatitis C patients with the IL28B CC polymorphism the
success rate and side effects of 3-drug treatment compared with 2-drug treatment.
In this study, patients with genotype 1 chronic hepatitis C who have the IL28B CC
polymorphism will be randomly assigned to be treated with telaprevir, peginterferon, and
ribavirin or with only peginterferon with ribavirin. These medications and the procedures
involved, including patient history, physical examination, and obtaining small volume blood
specimens (less than 4 teaspoons) for laboratory testing, are within the scope of standard
management of hepatitis C treatment. All patients will be monitored during treatment with
periodic blood testing (weeks 2, 4, and every 4 weeks thereafter while on treatment, and 24
weeks after stopping treatment) and office visits (weeks 5, 12, 25, 49 while on treatment
and 25 weeks after stopping treatment). The success of treatment will be judged by the
presence or absence of detectable virus in blood, as measured by a sensitive diagnostic test
(PCR). The data to be generated will include measurement by PCR of hepatitis C viral loads
before, during, and after treatment, as well as reporting of adverse drug effects.
Chronic infection with the hepatitis C virus (HCV), which affects 1-2% of adults in the
United States, is a major risk factor for liver failure due to cirrhosis and/or
hepatocellular carcinoma (Davis 2010). Epidemiological information suggests that the
frequency of these HCV-related sequelae is likely to continue to increase over the next
10-15 years unless effective and well-tolerated treatments become available. Development of
improved antiviral therapy is thus an important public health priority.
Until recently, the most effective treatment for chronic HCV infection has been a
combination of peginterferon and ribavirin, given for up to 48 weeks. With this regimen, the
sustained virological response (SVR), defined as undetectable HCV RNA 24 weeks after
completion of antiviral treatment, is approximately 50-60% (Hoofnagle 2006). Not all
patients are able to complete therapy however; up to 10% will discontinue this prematurely
as a result of intolerable side effects, predominantly depression and/or fatigue (Seeff
2010). The major determinants of responsiveness to antiviral therapy are viral genotype and
selected host characteristics. Hepatitis C genotype 1 (HCV-1), which accounts for
approximately 70% of chronic infections in North America, and is relatively resistant to
treatment with peginterferon and ribavirin. SVR with treatment for HCV-1 is approximately
40% (Hoofnagle 2006). That said, among HCV-1-infected individuals, there is diversity in
SVR, which is correlated with a dinucleotide polymorphism at a locus upstream of the
interleukin 28B (IL28B) gene. Specifically, with 48 weeks of peginterferon and ribavirin
therapy, 70% of individuals with the IL28B CC polymorphism achieve SVR, compared with only
30% of individuals with other IL28B polymorphisms (Thompson 2010).
New treatments for chronic HCV-1 infection are now available. In May 2011, the Food and Drug
Administration (FDA) approved telaprevir, an orally available small molecule inhibitor of
the HCV-1 protease, for treatment of chronic HCV-1, to be given in combination with
peginterferon and ribavirin. In HCV-1-infected patients, this three-drug regimen has been
shown to confer an SVR of 75% (Jacobson 2011). However, this regimen appears to be
associated with up to a nearly 1.5-fold increase in premature drug discontinuation, in
comparison with a regimen of peginterferon, and ribavirin alone, largely influenced by the
development of telaprevir-associated rash. Given the high responsiveness to conventional
peginterferon and ribavirin among HCV-1-infected individuals with the IL28B CC polymorphism,
we hypothesize SVR will not be enhanced in such individuals by the addition of telaprevir to
peginterferon and ribavirin therapy. If this is correct, HCV-1-infected patients with the
IL28B CC polymorphism can then be treated with comparable success with peginterferon and
ribavirin alone and will therefore be spared telaprevir-associated adverse affects.
The proposed study, which is a prospective randomized open label trial (in HCV-1-infected
subjects with the IL28B CC polymorphism) of treatment with telaprevir (T), peginterferon
(P), and ribavirin (R) versus PR alone, will test the working hypothesis. The study design
takes advantage of the concept of response-guided treatment, a strategy in which the
duration of antiviral treatment is based upon the presence or absence of a rapid virological
response (RVR), defined as loss of detectable serum HCV RNA within the first 4 weeks of
therapy. In particular, it has been shown that HCV-1 patients who achieve RVR (and maintain
undetectable HCV RNA at 12 weeks (defined as eRVR), with either PR-containing or
TPR-containing regimens have comparable SVR with 24 weeks, compared with 48 weeks, of total
treatment (Mangia 2008, Jacobson 2011).
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