18 mL/minute (SD 1444) for group 2; 9646 mL/minute (SD 2933) a

18 mL/minute (SD 14.44) for group 2; 96.46 mL/minute (SD 29.33) and 98.21 mL/minute (SD 25.86) for group 3; 87.35 mL/minute (SD 20.27) and 92.23 mL/minute (SD 24.79) for group 4; and 94.86 mL/minute (SD 21.23) and 96.85 mL/minute (29.67) for group 5, respectively. There were no significant differences in the CrCl between the values at baseline and week 12 in all the five groups (P > 0.05). The exact CrCl values at baseline, week 12 (end of LB80380 treatment), and week 36 (end of adefovir treatment) for all individual patients in the five groups are depicted in Fig. 4. Two patients in group 1 experienced selleck kinase inhibitor an increase in creatinine greater than the predetermined amount at week 28 and week 36, respectively.

The CrCl were 78.6 mL/minute and 101.1 mL/minute, respectively. According to our previous study of LB80380 given for 4 weeks in treatment-naïve CHB patients, there is a dose-proportional effect on HBV DNA

reduction with an increasing dose.12 The maximal HBV DNA suppression with 4 logs HBV DNA reduction after 4 weeks is achieved with the dose of equal or higher than 60 mg daily. In the current study, for lamivudine-resistant disease, a dose-proportional effect was also demonstrated with increasing doses of LB80380 up to 150 mg daily. This could be mathematically expressed by the dose-proportional constants for every single log unit increase in the dose for week 4 and this website 12 (Fig. 3). The maximal mean HBV DNA reduction was achieved at the dose of 150 mg daily (group 4) (Table 2, Fig. 2), with 4.16 logs copies/mL reduction after only 12 weeks of treatment. The mean HBV DNA suppression after 1-year treatment of adefovir and of entecavir (1 mg daily) in lamivudine-resistant patients are 4.0 logs copies/mL and 5.1 logs copies/mL, respectively.5, 14 This suggests that greater viral suppression may be achieved by LB80380. In the present study, there was an increase of median HBV DNA at 16 weeks (i.e., 4 weeks after Amino acid switching from

LB80380 to adefovir) in group 5 (Fig. 2). All 13 episodes of virologic rebound occurred after switching to adefovir. The highest dose of LB80380 (group 5) had earlier virologic rebound. This was presumably related to the greater suppression of HBV DNA with this dosage. However, it should be noted that the study was not empowered statistically to compare the efficacy between these two antiviral agents. The HBV DNA reduction achieved by LB80380 and tenofovir appears to be comparable. The mean HBV DNA reduction at week 12 was 4.16 logs copies/mL for LB80380 and 4.5 logs copies/mL for tenofovir.15 However, head-to-head comparative studies must be performed for more definite conclusions. It has been shown in in vitro studies that, of nine mutants resistant to lamivudine, adefovir, entecavir, or telbivudine tested, LB80380 is as potent against six of these as the wild-type virus.13 Two other mutants have a small decrease (<7-fold) in sensitivity to LB80380.

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