Clinical Trials Study
Copyright ©The Author(s) 2017.
World J Gastroenterol. Jan 14, 2017; 23(2): 306-317
Published online Jan 14, 2017. doi: 10.3748/wjg.v23.i2.306
Table 1 Characteristics of the modified intent-to-treat population
CharacteristicVacc. (n = 107)Ctr. (n = 115)P value
Demographics
Age, median (IQR)28.9 (23.1-37.1)29.3 (24.0-35.4)0.950
Male sex, n (%)86 (78.9)86 (74.1)0.400
Weight (kg), median (IQR)62.5 (56.0-70.0)63.0 (56.0-70.0)0.907
Genotype B, n (%)42/107 (39.3)39/115 (33.9)0.409
Week 0 laboratory results
ALT (IU/L), median (IQR)119.0 (94.0-167.5)136.0 (102.6-195.3)0.066
HBV DNA (log10 IU/mL), median (IQR)8.1 (7.7-8.3)8.1 (7.5-8.4)0.9532
HBeAg (COI), median (IQR)852.0 (223.5-1093.0)926.6 (508.5-1076.0)0.1972
HBsAg (IU/mL), median (IQR)10261.0 (3953.0-24089.0)8637.0 (2748.0-24436.0)0.7542
Week 12 laboratory results1
HBV DNA (log10 IU/mL), median (IQR)3.5 (2.6-4.5)3.4 (2.6-4.6)0.7542
HBeAg (COI), median (IQR)147.4 (15.6-650.0)45.9 (11.9-1011.0)0.6052
HBsAg (IU/mL) median (IQR)4072.0 (1608.0-8514.0)3023.5 (1167.0-11194.0)0.4602
1The time point when the injection of study agent started;
2Analyzed with Wilcoxon Rank Sum test. mITT: Modified intent-to-treat; LAM: Lamivudine; IQR: Interquartile ranges; ALT: Alanine aminotransferase; COI: Semi-quantification by S/CO [the signal value ratio of sample (S) to the control (CO)]; Vacc.: LAM + vaccine arm; Ctr.: LAM + placebo arm.
Table 2 Cumulative number of patients in the per-protocol set with adefovir add-on treatment due to lamivudine antiviral failure at each time point of the trial n (%)
WeekVacc. (n = 102)Ctr. (n = 113)
241 (0.98)0 (0.00)
362 (1.96)1 (0.88)
404 (3.92)5 (4.42)
487 (6.86)8 (7.08)
5211 (10.78)14 (12.39)
5617 (16.67)18 (15.93)
6027 (26.47)26 (23.01)
6434 (33.33)32 (28.32)
Vacc.: LAM + vaccine arm; Ctr.: LAM + placebo arm; ADV: Adefovir; LAM: Lamivudine.
Table 3 Virological responses after the end of treatment with DNA vaccination or placebo injection in contrast to the baseline at week 12 in different analysis populations
PopulationResponse12 wk after EOT (week 48)
28 wk after EOT (week 64)
36 wk after EOT (week 72)
Vacc.Ctr.P valueVacc.Ctr.P valueVacc.Ctr.P value
mITTNo. of patients107115107115107115
HBV DNA (log10 IU/mL), median (IQR)3.06 (0-4.63)3.05 (1.43-5.02)0.7422.18 (0-5.01)2.78 (1.41-4.86)0.1641.88 (0-4.36)2.37 (0-5.38)0.329
HBV DNA > 2 log10 IU/mL decrease, n (%)11 (10.3)4 (3.48)0.04413 (12.2)6 (5.2)0.06510 (9.4)7 (6.1)0.362
HBV DNA undetectable, n (%)27 (25.2)23 (20.0)0.35130 (28.0)20 (17.4)0.05824 (22.4)26 (22.6)0.975
HBeAg > 1 log10 IU/mL decrease, n (%)22 (20.6)22 (19.1)0.789NDND37 (34.6)27 (23.5)0.068
HBeAg seroconversion, n (%)16 (15.0)10 (8.7)0.147NDND18 (16.8)15 (13.0)0.429
dPPSNo. of patients9810875876881
HBV DNA (log10 IU/mL), median (IQR)2.99 (0-4.59)3.05 (1.43-5.02)0.5932.16 (0-4.66)2.78 (1.41-4.86)0.1041.85 (0-3.78)2.37 (0-5.38)0.262
HBV DNA > 2 log10 IU/mL decrease, n (%)11 (11.2)4 (3.8)0.03813 (17.3)6 (7.1)0.04010 (14.7)7 (8.9)0.246
HBV DNA undetectable, n (%)27 (27.6)23 (21.3)0.29629 (38.7)20 (23.0)0.03024 (35.3)26 (32.1)0.681
HBeAg > 1 log10 IU/mL decrease, n (%)20 (20.4)21 (19.4)0.863NDND29 (42.7)25 (30.9)0.136
HBeAg seroconversion, n (%)16 (16.3)10 (9.3)0.127NDND18 (26.5)15 (18.5)0.244
Subgroup1No. of patients111911191119
HBV DNA (log10 IU/mL), median (IQR)0 (0-1.16)1.43 (0-2.64)0.2680 (0-0)1.73 (0-3.6)0.0530 (0-0)0 (0-4.32)0.172
HBV DNA undetectable, n (%)8 (72.7)7 (36.8)0.1288 (72.7)8 (44.1)0.1427 (63.6)9 (47.4)0.466
HBeAg seroconversion, n (%)5 (45.5)2 (10.5)0.068NDND6 (54.6)3 (15.8)0.042
dPPS of subgroup2No. of patients1119918917
HBV DNA (log10 IU/mL), median (IQR)0 (0-1.16)1.43 (0-2.64)0.2680 (0-0)1.73 (0-3.6)0.0530 (0-0)0 (0-4.32)0.172
HBV DNA undetectable, n (%)8 (72.7)7 (36.8)0.1288 (88.9)8 (44.4)0.0427 (77.8)9 (52.9)0.399
HBeAg seroconversion, n (%)5 (45.5)2 (10.5)0.068NDND6 (66.7)3 (17.7)0.028
1Subgroup, 30 patients with HBV DNA < 1000 copies/mL (1.79 × 102 IU/mL) at week 12;
2dPPS of subgroup, population for analysist of the 30 patients with HBV DNA < 1000 copies/mL (1.79 × 102 IU/mL) at week 12 by ruling out the ADV add-on cases at each time point instantly after ADV administration due to lamivudine (LAM) antiviral failure. Data were analyzed with Fisher’s exact test. mITT: Modified intent to treat; dPPS: Dynamic per-protocol set by ruling out the adefovir (ADV) add-on cases at each time point instantly after ADV administration due to lamivudine (LAM) antiviral failure; ND: Not detected; Vacc.: LAM + DNA vaccine arm; Ctr.: LAM + placebo arm.
Table 4 Hepatitis B virus antigen-specific T-cell responses in 45 patients from week 50 to 70 after the trial n (%)
Positive responseVacc. (n = 22)Ctr. (n = 23)P value
1IFN-γ secretion19 (86.4)13 (56.5)0.047
2CD3 + CD8 + IFN-γ17 (77.3)10 (43.5)0.021
1A positive T-cell response was defined as an increase in interferon-γ (IFN-γ) secretion by two times compared to the control level, tested by ELISA, that in itself was no less than 100 pg/mL upon 9 d cultivation of PBMCs stimulated by HBsAg;
2A positive T-cell response was defined as no less than 0.1 percentage frequency of CD8 cells showing positive IFN-γ intracellular staining, tested by FACS, upon stimulation by various HBV envelope antigens. Vacc.: LAM + DNA vaccine arm; Ctr.: LAM + placebo arm.
  • Citation: Yang FQ, Rao GR, Wang GQ, Li YQ, Xie Y, Zhang ZQ, Deng CL, Mao Q, Li J, Zhao W, Wang MR, Han T, Chen SJ, Pan C, Tan DM, Shang J, Zhang MX, Zhang YX, Yang JM, Chen GM. Phase IIb trial of in vivo electroporation mediated dual-plasmid hepatitis B virus DNA vaccine in chronic hepatitis B patients under lamivudine therapy. World J Gastroenterol 2017; 23(2): 306-317
  • URL: https://www.wjgnet.com/1007-9327/full/v23/i2/306.htm
  • DOI: https://dx.doi.org/10.3748/wjg.v23.i2.306