The secondary objective was met as the HI antibody responses foll

The secondary objective was met as the HI antibody responses following the second vaccine dose fulfilled the CHMP criteria in all treatment groups at Day 42 and persisted through Day 182. At Day 42, in subjects who were seronegative at baseline, the seroconversion rates were 95% for those who received a single primary dose of AS03B-adjuvanted 1.9 μg HA vaccine or the non-adjuvanted vaccine, and 100% for those who received two primary doses of the AS03B-adjuvanted 1.9 μg HA vaccine or a single Ruxolitinib solubility dmso primary dose of the 3.75 μg HA AS03A-adjuvanted vaccine.

In subjects who were seropositive at baseline, seroconversion rates ranged from 73.3% for those who received a single primary dose of AS03B-adjuvanted 1.9 μg HA vaccine to 95.5% buy Ulixertinib for those who received a single primary dose of

the 3.75 μg HA AS03A-adjuvanted vaccine (Supplementary Table 1). As observed from the HI antibody GMTs, the highest HI antibody response at Day 182 (pre-booster) was observed for children who received two primary doses of the AS03B-adjuvanted 1.9 μg HA vaccine (GMT [95% CI]: 318.4 [257.8–393.1]), followed by those who received a single primary dose of the 3.75 μg HA AS03A-adjuvanted vaccine (GMT [95% CI]: 240.2 [188.1–306.6]). The HI antibody GMTs (95% CI) in groups that received a single primary dose of AS03B-adjuvanted 1.9 μg HA vaccine or a single primary non-adjuvanted vaccine dose were 176.1 (137.1–226.0) and 177.2 (140.1–224.0). Seven days after booster vaccination (Day 189), with Day 0 as the reference point, SPR, SCR, and GMFR were ≥97.2%, ≥74.6% and ≥12.1, respectively,

in all treatment groups, meeting the CHMP criteria. Using the pre-booster time point as the reference point for computation, the SCR ranged from 10.2% in the non-adjuvanted vaccine group to 28.6% in the group receiving a single primary dose of AS03B-adjuvanted 1.9 μg HA vaccine. GMFR ranged from 1.5 in the non-adjuvanted vaccine group to 2.5 in the AS03A-adjuvanted 3.75 μg HA vaccine group (Table 3). An anamnestic response in all treatment groups was suggested based on the rapid increase in HI antibody Rebamipide GMTs (1.5–2.5-fold increase), 7 days after booster vaccination (Day 189) compared with the pre-booster time point (Day 182) (Table 2). Of all subjects included in the per protocol cohort for immunogenicity, 33 from 5 study centers had not reached seroconversion (either post-vaccination HI antibody titers against the A/California H1N1/2009 strain were <1:40 for subjects who were seronegative at baseline, or post-vaccination HI antibody titers against the A/California H1N1/2009 had increased by less than 4-fold for subjects who were seropositive at baseline) and thus were considered as non-responders to the study vaccine. Of these, 15 subjects were enrolled and vaccinated in four centers in Slovakia and 18 in the center located in Estonia. The distribution of these subjects per study group and center is presented in Supplementary Table 2.

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