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2 YEARS VERSUS 6 MONTHS OF INTERFERON THERAPY FOR CHRONIC
HEPATITIS C
Short-term (end-of-treatment) responses (ETR) to interferon
(IFN) therapy for chronic hepatitis C are encouraging; however, the
relapse rate is high, and long-term response is obtained in only
12- 25% of patients. The Australian Hepatitis C Study Group
conducted a trial of 230 patients that compared the standard 3 MU
three times a week six-month course of IFN-alpha(2b) with 5 MU
three times a week for six months (5 MU group) or 3 MU three times
a week for two years (two-year group). ETR (normalization of serum
aminotransferase level until the end of treatment) rates based on
an intent-to-treat analysis were 64% for the 5 MU group and 58% for
the combined 3 MU groups. After six months of treatment, the
overall relapse rate was 71%, and the long-term response (LTR;
continued normal aminotransferase until six month follow up) rate
did not differ significantly between the 3 MU (17% of all treated,
27% ETR) and 5 MU groups (20% of all treated, 31% ETR). In
contrast, among the 46 patients who exhibited an ETR in the
two-year group, 27 (59%) had a LTR to IFN, resulting in an overall
LTR rate of 33% for all patients treated for up to two years (P
< 0.001 compared with 3 MU group). Among these 46 subjects, Il
did not complete the full two-year course, including eight who
withdrew due to adverse effects. Nine of these 11 patients had
received at least 12 months of therapy. All 18 LTR subjects tested
(irrespective of treatment group) were serum HCV -RNA negative at
the 12-month follow-up evaluation. Improvement in hepatic
inflammation was significantly greater among those treated for two
years compared with six months, but there was no reduction in
fibrosis score in any group. Among the entire study group,
treatment duration, liver histology, and liver function (assessed
by antipyrine clearance test) were the only independent predictors
of ETR, although HCV genotype was closely related to histological
severity leg, cirrhosis was present in 60% of type 1 and 18% of
type 3). Viral load and duration of infection were additional
predictors of LTR; however, there were insufficient data to
determine whether prolonging treatment beyond six months overcomes
the negative impact of these predictors. Continuing IFN therapy for
at least 12 months decreases the relapse rate by 50% and thereby
improves the LTR rate compared with a six-month treatment course.
However, our experience of 24 months of treatment indicates that
initial IFN treatment courses of this duration are not well
tolerated by approximately 20% (8/46) of patients and are unlikely
to improve the results obtained with 12-18 months of treatment.
Author: FARRELL GC, UNIV SYDNEY, WESTMEAD HOSP, DEPT MED,
STORR LIVER UNIT, WESTMEAD NSW 2145
Source: DIGESTIVE DISEASES AND SCIENCES 1996 DEC;41(12):S 93-S
98
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