A combination of TMC435
– also known as simeprevir
– plus pegylated interferon and
ribavirin raised cure rates for genotype 1 hepatitis C patients who did not
respond to previous treatment, according to a study presented at the 47th
International Liver Congress last week in Barcelona.
Last year's approval of the first direct-acting
antiviral agents has changed the face of treatment for chronic hepatitis C, but
several potentially more effective and better tolerated next-generation drugs
are under development. Those expected to be next in line for approval will be
used with pegylated interferon/ribavirin until trials of all-oral therapy are
completed.
TMC435 is a potent once-daily hepatitis C virus (HCV)
NS3/4A protease inhibitor. Early studies showed potent activity against HCV
genotype 1, lesser activity against genotypes 2, 4, 5 and 6, and a favourable
safety profile.
Glossary
- IL28B
An inherited gene which all individuals have. There are three genotypes of IL28B; these influence response to hepatitis C and its treatment. People with CC genotype are more likely to spontaneously clear acute infection or (during chronic infection) respond well to interferon-based treatment. The other two genotypes are known as CT and TT.
- rapid virological response (RVR)
An undetectable hepatitis C RNA viral load within 4 weeks of starting treatment. An extended rapid virological response (eRVR) is when viral load is undetectable within 4 weeks and remains undetectable until at least week 12.
In the ASPIRE trial, Stefan Zeuzem from JW Goethe
University Hospital and an international team of investigators evaluated TMC435
added to the previous standard-of-care treatment for chronic hepatitis C.
This phase IIb trial included 462 treatment-experienced patients with
difficult-to-treat HCV genotype 1. Forty per cent were prior relapsers (undetectable HCV
RNA at the end of prior therapy but viral rebound during 24 weeks of
post-treatment follow-up), 35% were prior partial responders (at least a 2 log10
viral load reduction at week 12 of prior therapy but still detectable at the
end of treatment) and 25% were prior null responders (less than a 2 log10
decrease in HCV RNA by week 12 of prior therapy).
About two-thirds of participants were men, almost all were white, and
the median age was 50 years. Just over 40% had HCV subtype 1a, the rest 1b;
most had high HCV viral load at baseline. Seventeen per cent had the favourable IL28B 'CC'
genotype associated with good response to interferon. Nearly 20% had
advanced liver fibrosis (stage F3) and a similar proportion had cirrhosis
(stage F4) at baseline. Patients with liver cancer, transplant recipients and
HIV or hepatitis B co-infected people were excluded.
Participants were randomly allocated to receive 100mg or 150mg
once-daily TMC435 for either 12, 24 or 48 weeks in combination with pegylated
interferon alfa-2a (Pegasys) and
1000 to 1200mg/day weight-adjusted ribavirin. In the 12- and 24-week arms,
pegylated interferon/ribavirin were continued alone through week 48. The
control arm received pegylated interferon/ribavirin plus placebo.
At week 4 of treatment, rapid virological response (RVR) rates among
patients receiving 100mg TMC435 were 67%, 59% and 53%, respectively, in the
12-, 24- and 48-week groups. Among people receiving 150mg TMC435, the
corresponding rates were 62%, 68% and 66%, respectively. Only 2% of this
difficult-to-treat population saw a rapid response with pegylated interferon/ribavirin
alone.
RVR was a good predictor of sustained virological response 24 weeks
after completion of therapy (SVR24). Sustained response rates were 70%, 66% and
61% for people taking 100mg TMC435 for 12, 24 or 48 weeks, and 67%, 72% and 80%
for those receiving 150mg. The SVR rate in the control group was just 23%.
Looking at type of prior response, the SVR24 rates for relapsers were
85% with either 100mg or 150mg TMC435 compared with 37% in the control group.
For prior partial relapsers, the corresponding rates were 57%, 75% and 9%,
respectively. Rates for prior null responders were 46%, 51% and 19%,
respectively.
Among prior relapsers, those with HCV subtype 1a and 1b had similar cure
rates, but among prior partial and null responders those with subtype 1b did
better. People with minimal fibrosis responded better overall than those with
advanced fibrosis or cirrhosis.
Few TMC435 recipients met the stopping rule for discontinuing treatment
early due to likely futility, compared with up to 75% of patients taking
pegylated interferon/ribavirin alone. Viral breakthrough during treatment
occurred in 1% to 24% of TMC435 recipients in the various arms, while viral
relapse after completing treatment was seen in 3% to 16%.
As described in another presentation at the conference by Oliver Lenz
from Tibotec, viral breakthrough and relapse were usually associated with
signature resistance mutations at NS3 positions 80, 122, 155 and/or 168, but
the distribution of mutations varied significantly between genotype 1a and 1b.
TMC435 was generally well tolerated. Rates of serious adverse events
were 6% in the 100mg TMC435 arm, 10% in the 150mg arm and 6% in the control
arm. Rates of discontinuation due to adverse events were 7%, 9% and 5%,
respectively.
The most common side-effects across all groups were headache, fatigue and
flu-like symptoms. TMC435 recipients were more likely to experience pruritis
(itching) or skin rash than those in the control group, but severe rashes were
rare (0.5%). Changes in blood cell levels were similar in the TMC435 and
control arms. People taking TMC435 were more likely to develop elevated
bilirubin, which Zeuzem explained was related to the drug's effect on two
transporters.
"In HCV genotype 1 patients who previously failed pegylated
interferon/ribavirin treatment, once-daily TMC435 administered with pegylated
interferon/ribavirin was significantly more effective than pegylated
interferon/ribavirin/placebo", the researchers concluded. "Once-daily
TMC435 was well tolerated in this population".
Based on the
finding of somewhat better response rates in the higher-dose TMC435 arm –
especially for prior partial or null responders
– the 150mg dose is currently
undergoing testing in phase III clinical trials.
Zeuzem noted
that while all arms were treated for a total of 48 weeks in this study, data
"clearly indicate that a treatment duration of 12 weeks
achieves optimal SVR rates", suggesting that TMC435 will be suitable for
response-guided therapy.