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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT01037062
Other study ID # AI463-060
Secondary ID
Status Completed
Phase Phase 2
First received December 17, 2009
Last updated January 24, 2011
Start date December 2003
Est. completion date December 2006

Study information

Verified date December 2009
Source Bristol-Myers Squibb
Contact n/a
Is FDA regulated No
Health authority Japan: Pharmaceuticals and Medical Devices Agency
Study type Interventional

Clinical Trial Summary

To provide open-label entecavir to subjects who have completed previous blinded entecavir trials in Japan and are assessed by the investigator as likely to benefit from additional anti-hepatitis B therapy


Recruitment information / eligibility

Status Completed
Enrollment 282
Est. completion date December 2006
Est. primary completion date December 2006
Accepts healthy volunteers No
Gender Both
Age group 20 Years and older
Eligibility Inclusion Criteria:

- Subjects who completed a previous entecavir Phase II studies (AI463047, 052 or 053);

- ALT = 10 x upper limit of normal;

- Subjects must have well-compensated liver disease according to ALL of the following criteria;

1. Prothrombin time = 3 seconds prolonged compared to control value or INR = 1.5

2. Serum albumin = 3 g/dL (= 30 g/L)

3. Serum bilirubin = 2.5 mg/dL (= 42.75 µmol/L)

Exclusion Criteria:

- Sex and Reproductive Status Exceptions

- Target Disease Exceptions

- Medical History and Concurrent Diseases

Study Design

Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Treatment


Intervention

Drug:
Entecavir
Tablet, P.O. 0.5, 1 mg, once daily

Locations

Country Name City State
Japan Local Institution Aichi-Gun Aichi
Japan Local Institution Akashi-Shi Hyogo
Japan Local Institution Asahikawa-Shi Hokkaido
Japan Local Institution Chiba-Shi Chiba
Japan Local Institution Fukuoka-Shi Fukuoka
Japan Local Institution Fukuyama-Shi Hiroshima
Japan Local Institution Gifu-Shi Gifu
Japan Local Institution Hiroshima City Hiroshima
Japan Local Institution Hiroshima-Shi Hiroshima
Japan Local Institution Iruma-Gun Saitama
Japan Local Institution Kawachinagano-Shi Osaka
Japan Local Institution Kumamoto-Shi Kumamoto
Japan Local Institution Kurashiki-Shi Okayama
Japan Local Institution Kurume Fukuoka
Japan Local Institution Kyoto
Japan Local Institution Matsumoto City Nagano
Japan Local Institution Minato-Ku Tokyo
Japan Local Institution Mitoyo-Gun Kagawa
Japan Local Institution Miyazaki-Gun Miyazaki
Japan Local Institution Morioka-Shi Iwate
Japan Local Institution Musashino-Shi Tokyo
Japan Local Institution Nagasaki City Nagasaki
Japan Local Institution Nagoya Aichi
Japan Local Institution Nagoya-Shi Aichi
Japan Local Institution Nagoya-Shi Aichi
Japan Local Institution Nakakoma-Gun Yamanashi
Japan Local Institution Niigata
Japan Local Institution Ogaki-Shi Gifu
Japan Local Institution Oita-Gun Oita
Japan Local Institution Okayama-Shi Okayama
Japan Local Institution Okayama-Shi Okayama
Japan Local Institution Okayama-Shi Okayama
Japan Local Institution Omura-Shi Nagasaki
Japan Local Institution Onsen-Gun Ehime
Japan Local Institution Osaka
Japan Local Institution Osaka-Shi Osaka
Japan Local Institution Sakai-Shi Osaka
Japan Local Institution Sapporo-Shi Hokkaido
Japan Local Institution Sapporo-Shi Hokkaido
Japan Local Institution Sendai Miyagi
Japan Local Institution Shinjuku-Ku Tokyo
Japan Local Institution Shinjuku-Ku Tokyo
Japan Local Institution Shinjuku-Ku Tokyo
Japan Local Institution Suita-Shi Osaka
Japan Local Institution Takamatsu-City Kagawa
Japan Local Institution Tokyo
Japan Local Institution Tsuyama-Shi Okayama
Japan Local Institution Ube-Shi Yamaguchi

Sponsors (1)

Lead Sponsor Collaborator
Bristol-Myers Squibb

Country where clinical trial is conducted

Japan, 

References & Publications (2)

Karino Y, Toyota J, Kumada H, Katano Y, Izumi N, Kobashi H, Sata M, Moriyama M, Imazeki F, Kage M, Ishikawa H, Masaki N, Seriu T, Omata M. Efficacy and resistance of entecavir following 3 years of treatment of Japanese patients with lamivudine-refractory chronic hepatitis B. Hepatol Int. 2010 Feb 6;4(1):414-22. doi: 10.1007/s12072-009-9162-x. Erratum in: Hepatol Int. 2010;4(4):789-90. — View Citation

Yokosuka O, Takaguchi K, Fujioka S, Shindo M, Chayama K, Kobashi H, Hayashi N, Sato C, Kiyosawa K, Tanikawa K, Ishikawa H, Masaki N, Seriu T, Omata M. Long-term use of entecavir in nucleoside-naïve Japanese patients with chronic hepatitis B infection. J Hepatol. 2010 Jun;52(6):791-9. doi: 10.1016/j.jhep.2009.12.036. Epub 2010 Mar 24. — View Citation

Outcome

Type Measure Description Time frame Safety issue
Primary To provide open-label entecavir to subjects who have completed previous blinded entecavir trials in Japan and are assessed by the investigator as likely to benefit from additional anti-hepatitis B therapy 24 weeks No
Secondary Incidence of clinical adverse events and discontinuations due to adverse events of entecavir for each cohort Week 2, 4, 6, 8, 10, 12, 16, 20 and 24 post dosing Yes
Secondary Incidence of laboratory abnormalities of of entecavir for each cohort Week 2, 4, 6, 8, 10, 12, 16, 20 and 24 post dosing Yes
Secondary Proportion of subjects HBeAg-positive at baseline who have loss of HBeAg from serum Day 1, Week 12, Week 24 and every subsequent 24 week during dosing No
Secondary Proportion of subjects HBeAg-positive at baseline who achieve seroconversion (loss of HBeAg and appearance of HBeAb) Day 1, Week 12, Week 24 and every subsequent 24 week during dosing No
Secondary Proportion of subjects with abnormal ALT at baseline who achieve normalization of serum ALT at Week 48 Day 1, Week 48 No
Secondary Proportion of subjects who achieve HBV DNA levels by PCR assay less than the limit of quantification (LOQ) Day 1, Week 12, 24, and subsequent 24 week during dosing No
Secondary Proportion of subjects positive for HBeAg at baseline who achieve HBV DNA levels by PCR assay less than LOQ, normal serum ALT, and seroconversion Week 8, 16, 24 post dosing No
Secondary Proportion of subjects negative for HBeAg at baseline who achieve HBV DNA levels by PCR assay less than LOQ and normal ALT and remain negative for HBeAg Day 1, Week 12, Week 24 and every subsequent 24 weeks during dosing No
Secondary Proportion of subjects who achieved Complete Response during therapy, who have sustained Complete Response for 24 weeks after stopping drug 24 Week post dosing No
Secondary Proportion of subjects with histological improvement in the liver at Wks 48 & 96 [improvement in necroinflammatory score and no worsening of fibrosis at Wks 48 & 96 liver biopsy compared to baseline & to baseline in previous study] Week 48, 96 No
Secondary NChanges in liver histology as assessed by the New Inuyama Classification for histological assessment of chronic hepatitis Week 48 & Week 96 No
Secondary Incidence of genotypic changes in HBV DNA polymerase conferring resistance to entecavir in subjects with confirmed =1 log10 increase in HBV DNA from nadir on treatment Week 2, 4, ± days, Week 8 every 4 weeks ± 7 days No
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