Below is the text of Medivir's press release describing the
research and its findings to date.
Medivir
Announces Phase 2b 24-week Interim Results
of TMC435 in Treatment-naive Patients
Chronically Infected with Genotype-1 Hepatitis C Virus
Potent
and consistent antiviral efficacy was demonstrated at 24-week
end-of-treatment and in interim SVR4 and SVR12 results. There
were no clinically relevant differences between TMC435 treatment
groups and placebo for adverse events.
July 12, 2010 -- Medivir announced today 24-week end-of-treatment
interim results from the 5-arm phase 2b response guided PILLAR
study in 386 treatment-naive patients with hepatitis C virus
(HCV) genotype-1 (TMC435-C205).
TMC435
is a protease inhibitor jointly developed by Medivir and Tibotec
Pharmaceuticals, dosed as one pill once daily (q.d.) to treat
hepatitis C virus infections (HCV).
In
the PILLAR study, 75 mg or 150 mg TMC435 was given for either
12 weeks or 24 weeks in combination with 24 weeks of ribavirin
[RBV] and pegIFNalpha-2A [pegylated interferon alpha-2a, or
Pegasys], the current standard of care (SoC). Patients stopped
all treatment at week 24 when HCV RNA levels at week 4 were
< 25 log10 IU/mL detectable or undetectable and HCV RNA levels
at week 12, week 16 and week 20 were < 25 log10 IU/mL undetectable.
Patients who did not meet the above response-guided criteria
continued with SOC until week 48. The results showed that in
the TMC435 treatment groups 83% of patients were able to stop
all therapy at Week 24.
Potent
and consistent antiviral efficacy was demonstrated at 24-week
end-of-treatment and in interim SVR4 and SVR12 rates with no
major differences between TMC435 doses or length of triple therapy.
92% of patients taking TMC435 and Peg-IFN/RBV (SoC) achieved
undetectable HCV RNA levels at week 4 and 92% at week 12 after
cessation of treatment, i.e. SVR4 and SVR12. SVR4 and SVR12
data were available for 82% and 42% of the TMC435-treated patients
respectively who had stopped all therapy before or at Week 24
and had completed the follow-up visits. Both the viral breakthrough
rate (4.9%) and relapse rate (1.6%) were low in the TMC435 treatment
groups.
TMC435
was generally safe and well tolerated with no relevant differences
in adverse events (AEs) between placebo and TMC435 treatment
groups. Most AEs were mild to moderate in severity and the discontinuation
rate due to AEs was low and not different from placebo.
When
looking at particular adverse events of interest, the incidence
of rash, pruritis, GI side effects and anemia were similar in
TMC435 groups and placebo and were generally mild to moderate
in nature. Use of erythropoetin-stimulating agents (ESAs) was
not allowed during the trial.
In
laboratory parameters, there were no clinically relevant differences
between any TMC435 groups and placebo except for mild bilirubin
elevations. Significant decreases in transaminases (ALT and
AST) were observed in all treatment groups.
Further
safety and efficacy data will be presented at future scientific
meetings later in 2010.
"We
are extremely encouraged and excited by the efficacy and safety
demonstrating that TMC435 is truly a second-generation HCV protease
inhibitor," stated Bertil Samuelsson, CSO of Medivir. "We
also are looking forward to the top-line data coming up from
the phase 2b trial C206 (ASPIRE) in treatment-experienced patients
later this year as well as start of phase 3 clinical trials
in treatment-naive patients early next year."
|
Frequency
of Undetectable* HCV RNA Levels During and After Treatment
|
|
Treatment
week
|
TMC12
PR24
|
TMC2
PR24
|
TMC1
PR24
|
TMC2
PR24
|
SoC
|
|
|
75mg
q.d.
|
75mg
q.d.
|
150mg
q.d.
|
150mg
q.d.
|
|
|
N
(%)
|
N=78
|
N=75
|
N=77
|
N=79
|
N=77
|
|
Week
24, EoT***
|
67/73
(92%)
|
65/67
(97%)
|
68/74
(92%)
|
73/78
(94%)
|
4/18
(22%)**
|
| Follow-up
at Week 4 and Week 12 after EoT |
|
SVR4
|
59/65
(91%)
|
56/60
(93%)
|
57/61
(93%)
|
63/68
(93%)
|
NA****
|
|
SVR12
|
32/33
(97%)
|
27/29
(93%)
|
32/36
(89%)
|
29/32
(91%)
|
NA
|
*
< 25 log10 IU/mL undetectable
** End of treatment
***EoT: End of Treatment
****Patients in the control arm continue SoC till
Week 48 and SVR data are not available
q.d.: once daily; PR: pegylated interferon alpha-2a
and ribavirin; SVR4: undetectable HCV RNA at EoT &
undetectable HCV RNA 4 weeks after planned EoT; SVR12:
undetectable HCV RNA at EoT & undetectable HCV
RNA 12 weeks after planned EoT |
|
About
TMC435 clinical trial programs
TMC435 is a protease inhibitor jointly developed by Medivir
and Tibotec Pharmaceuticals to treat hepatitis C virus infections
(HCV).
TMC435 is currently being developed in three phase 2b clinical
trials (TMC435-C205, TMC435-C206 and TMC435-C215) in G1 treatment-naive
and in G1 patients that failed previous IFN-based treatment.
Safety and efficacy data from the phase 2b trials will be presented
at scientific meetings later in 2010.
TMC435-C205
is a global phase 2b study in 386 genotype-1 treatment-naive
patients. It is a once daily treatment of TMC435 with different
doses and durations given in addition to standard of care treatment,
consisting of ribavirin and pegIFNalpha-2A.
TMC435-C215
is a Japan phase 2b study in 92 genotype-1 treatment-naive patients.
It is a once daily treatment of TMC435 with different doses
and durations given in addition to standard of care treatment,
consisting of ribavirin and pegIFNalpha-2A.
TMC435-C206
is a global phase 2b study in 463 genotype-1 treatment-experienced
patients. It is a once daily treatment of TMC435 in with different
doses of given in addition to standard of care treatment, consisting
of ribavirin and pegIFNalpha-2A.
About
Hepatitis C
Hepatitis C is a blood-borne infectious disease of the liver
and is a leading cause of chronic liver disease and liver transplants.
The WHO estimates that nearly 180 million people worldwide,
or approximately 3% of the world's population, are infected
with hepatitis C virus (HCV). The CDC has reported that almost
three million people in the United States are chronically infected
with HCV.
For
more information on Medivir, please see the company website:
www.medivir.se.
8/24/10
Source
Medivir.
Medivir Announces Phase 2b 24-week Interim Results of TMC435
in Treatment-naïve Patients Chronically Infected with Genotype-1
Hepatitis C Virus. Press release. July 12, 2010.
