Hepatitis C Clinical Trial
Official title:
Tacrolimus Monotherapy in OLT Recipients With HCV Under Preemptive Treatment With Interferon and Ribavirin
After a liver transplant, the hepatitis C virus (which destroyed one's own liver) eventually
comes back. In many patients, this will eventually cause the loss of the new liver and can
also confuse the doctors taking care of them because it is hard to tell the difference
between one's body rejecting the new liver and hepatitis. This can cause serious treatment
errors that can lead to more severe hepatitis or to rejection of the liver. Some of the
drugs used to prevent rejection of one's new liver can cause the hepatitis to come back in a
more severe form. This is especially true for the drugs known as corticosteroids.
Right now, the only effective treatment against hepatitis C is a combination of two drugs
called interferon and ribavirin. These drugs act by strengthening one's immune system to
fight the virus and by directly reducing the reproduction of the virus. Because the
treatment with these drugs is associated with many side effects, there is little experience
with treating patients after liver transplantation with them.
In the investigators' transplant program, they have decided to treat all patients with
hepatitis C as early as possible after transplantation and to follow them closely for the
development of hepatitis and side effects of the treatment. The investigators treat one's
hepatitis as early as possible, before any actual damage has occurred in the new liver. This
approach has been tried before but it has been hard to tell if it has worked or not. The
main reason for failure was that many patients could not complete the treatment due to side
effects. The investigators' purpose is to treat those side effects aggressively so that most
patients can complete the treatment course.
The purpose of this study is to collect all the data regarding the investigators' treatment
protocol so that they will be able to learn if this form of treatment is beneficial.
The study includes performing liver biopsies at scheduled times after one's liver transplant
and for scheduled blood tests to see how much virus is still in the blood. If patients show
signs that they are not responding to treatment they will be removed from the study.
HCV recurs in the transplanted liver almost invariably. The clinical course is variable and
ranges from no hepatitis to severe aggressive hepatitis with cirrhosis. Factors that affect
outcome are high viral load prior to OLT, genotype, and immunosuppressive regimen. Recent
studies indicate that the severity of recurrence is increasing with longer follow up, and
longevity of both graft and patient is compromised by HCV. Viral load appears to be
particularly affected by corticosteroids. The impact of mycophenolate mofetil and tacrolimus
is not certain. The results of re-transplantation are generally poor and seem to be a
non-cost beneficial way to deal with recurrence HCV cirrhosis. Additionally,
re-transplantation deprives other patients from getting OLT in a timely fashion.
Recent studies have shown that with intensive alpha interferon and ribavirin treatment, up
to 40% of patients can be cleared of virus as measured by PCR. Thus, despite the cost and
side effects of this treatment, it appears justified to treat recurrence preemptively.
Due to the deleterious effects of high dose Corticosteroids it seems logical to attempt to
withdraw them as soon as possible from treatment. MMF is often incompatible with interferon
and ribavirin treatment due to leukopenia and anemia. The same is true for sirolimus. Thus,
most patients will eventually be treated with Tacrolimus monotherapy. Presently, numerous
patients end up being treated with Tacrolimus monotherapy as part of the reduction in immune
suppression, which occurs over time. There is, however, very little prospective data
regarding Tacrolimus monotherapy and almost no data on the specific issue of monotherapy in
HCV patients. Even less is known with respect to this type of treatment while using
interferon and ribavirin.
Our purpose in this protocol is to examine both the effect of preemptive antiviral treatment
on recurrent HCV and the effect of Tacrolimus monotherapy in this setting. This may be
important as more and more programs are turning to preemptive anti viral treatment and the
issue of appropriate immune suppression becomes seminal to this discussion.
Aims
1. To determine the safety and efficacy of PEG interferon and ribavirin in the treatment
of HCV recurrence after OLT.
2. To determine the effectiveness and safety of maintenance dose of PEG interferon to
delay progression of fibrosis and histologic damage, in non-responders to the initial
regimen of PEG interferon and ribavirin.
3. To determine the effect of early prednisone withdrawal in the rate of response to
treatment with PEG interferon and ribavirin.
4. To assess the feasibility of Tacrolimus monotherapy in patients undergoing treatment
for HCV recurrence post transplant.
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Allocation: Non-Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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