HUDDINGE, Sweden, April 1, 2011 /PRNewswire/ -- Medivir AB (OMX: MVIR), the emerging research-based specialty pharmaceutical company focused on infectious diseases, announces that their partner, Tibotec has presented the results of a planned Week 24 interim analysis of the phase 2b ASPIRE study for TMC435 in treatment experienced hepatitis C patients in a late-breaker session at the 46th Annual meeting of the European Association for the Study of the Liver (EASL), Berlin, Germany.

Treatment experienced patients are known to be the most difficult to treat hepatitis C patient group.

TMC435 is a potent, once-daily, oral hepatitis C virus protease inhibitor which recently entered clinical phase 3 studies. The study enrolled patients chronically infected with genotype-1 hepatitis C virus (HCV) that had previously failed treatment with standard of care therapy (peginterferon and ribavarin). TMC435 is being jointly developed by Medivir and its partner Tibotec.

In this Week 24 interim analysis, treatment-experienced patients who failed peginterferon and ribavarin treatment achieved significantly greater virologic response rates following treatment with TMC435-containing regimen at all doses, compared with placebo. Results demonstrated that the TMC435 150 mg dose group showed the highest response, particularly in prior null responders. In this 150 mg dose group, HCV RNA levels were undetectable at week 24 for between 82% and 91% of the patients. Results also showed that there was no statistically relevant difference in safety and tolerability between the TMC435 and placebo treated groups.

Ron Long, CEO of Medivir, commented: "We are delighted that these strong results are to be presented at such a prestigious scientific conference as EASL. TMC435 continues to demonstrate why Medivir are so confident that hepatitis C treatment can be significantly changed by a more convenient, once daily protease inhibitor especially for treatment experienced patients. These data and the recent start of phase 3 clinical studies for TMC435, represent an exciting stage in Medivir's development as a significant player in the infectious disease market."

On-treatment response rates are shown below.

TMC12/PR48 TMC24/PR48 TMC48/PR48 TMC12/PR48 100mg 100mg 100mg 150mg (N=66) (N=65) (N=66) (N=66) HCV RNA <25 IU/mL undetectable, % (u/N) Overall population 67,7 (44/65) 59,4 (38/64) 53,8 (35/65) 63,1 (41/65) Week 4 (RVR) *** *** *** *** Prior null responders 33,3 (5/15) 50,0 (8/16) 25,0 (4/16) 35,3 (6/17) Prior partial responders 65,2 (15/23) 40,9 (9/22) 60,9 (14/23) 65,2 (15/23) Prior relapser 88,9 (24/27) 80,8 (21/26) 65,4 (17/26) 80,0 (20/25) Overall population 87,1 (54/62) 84,5 (49/58) 85,2 (52/61) 85,7 (54/63) Week 24 *** *** *** *** Prior null responders 71,4 (10/14) 83,3 (10/12) 68,8 (11/16) 70,6 (12/17) Prior partial responders 86,6 (19/22) 80,0 (16/20) 85,7 (18/21) 86,4 (19/22) Prior relapser 96,2 (25/26) 88,5 (23/26) 95,8 (23/24) 95,8 (23/24) *** Statistically significant difference versus placebo, p<0,001 (table continued) TMC24/PR48 TMC48/PR48 Pbo48/PR48 150mg 150mg (N=68) (N=65) (N=66) HCV RNA <25 IU/mL undetectable, % (u/N) Overall population 70,8 (46/65) 66,2 (43/65) 1,5 (1/65) Week 4 (RVR) *** *** Prior null responders 41,2 (7/17) 41,2 (7/17) 0,0 (0/16) Prior partial responders 69,6 (16/23) 68,2 (15/22) 0,0 (0/23) Prior relapser 92,0 (23/25) 80,8 (21/26) 3,8 (1/26) Overall population 90,8 (59/65) 90,3 (56/62) 51,9 (28/54) Week 24 *** *** Prior null responders 81,3 (13/16) 93,3 (14/15) 44,4 (4/9) Prior partial responders 90,9 (20/22) 86,4 (19/22) 19,0 (4/21) Prior relapser 96,3 (26/27) 92,0 (23/25) 83,3 (20/24) *** Statistically significant difference versus placebo, p<0,001

The ASPIRE study evaluates the effect of TMC435 in combination with standard of care (SoC) in 462 patients infected with the difficult to treat genotype-1 hepatitis C virus who had undergone and failed prior treatment with (SoC). The study includes patients that have relapsed, achieved partial response, or achieved no response (null responders) to treatment with standard of care. TMC435 was administered once daily at a dose of either 100 mg or 150mg given for either 12, 24, or 48 weeks in combination with standard of care. Standard of care treatment was continued until the study completion at week 48.

As well as the late-breaker ASPIRE data presented, a further three presentations will be made at EASL on TMC435. These include:

Oral presentation: Impact of IL28b genotype and pretreatment serum IP-10 in treatment-naive genotype-1 HCV patients treated with TMC435 in combination with peginterferona-2a and ribavirin in PILLAR study, J. Aerssens, which found that during 24 weeks of treatment, IL28B genotype and serum IP-10 were predictive of response in patients receiving standard of care (peginterferon and ribavirin) but had limited predictive value in patients treated with both TMC435 and peginterferon and ribavirin, therefore suggesting that TMC435, a potent, once daily oral protease inhibitor, may overcome the negative consequences of unfavourable host genotype encountered with pegIFN/RBV.

Poster presentation No.472: Pharmacokinetics of TMC435 in subjects with moderate hepatic impairment, V. Sekar, which found that no TMC435 dose adjustment was necessary for patients with moderate liver impairment.

Poster presentation No.1221: Treatment outcome and resistance analysis in HCV genotype 1 patients previously exposed to TMC435 monotherapy and re-treated with TMC435 in combination with pegifna-2a/ribavirin, O. Lenz, which found that viral variants in patients who had received TMC435 as a monotherapy were no longer detected over time and successful treatment after prior exposure to TMC435 with emergence of resistance variants was possible in 3/5 patients who had failed interferon-based therapy.