After the 28-day study clinic visit, participants were visited or telephoned monthly by trained physicians until the end of the study to identify only SAEs. SAEs were graded for severity using the generic grading scale for unsolicited events. The study was designed to estimate simultaneously seropositivity for JE and measles antibodies 28 days post-vaccination. The primary analysis of immunogenicity was based on the per-protocol subject population. Seropositivity rates and corresponding exact 95% confidence intervals (CIs) were calculated based on the binomial distributions of
study outcomes. GMTs and corresponding 95% confidence intervals were calculated based on the normal distributions. For calculations of JE GMTs, titers less than the limit of detection were assigned a value of 1:5. We assumed the Day 28 post-co-administration selleck chemical seropositivity would be 90% [5] for JE and 95% [6] for measles. RG7204 in vitro Under these assumptions, a sample size of 249 evaluable subjects was required to demonstrate with at least 80% power that the observed seropositivity rate for JE antibodies is greater than 80% and that the observed seropositivity rate for measles antibodies is greater than 90%, using one-sided significance
levels of 0.025. We planned to consent up to 312 infants to allow for up to 10% exclusion during screening and 10% loss to follow-up. At the end of the study, any child who had not successfully seroconverted for JE and/or measles was offered revaccination Rolziracetam free of cost. The study was approved by the University Of Colombo Faculty Of Medicine Ethical Review Committee and PATH’s Research Ethics Committee, USA. Written informed consent was obtained from parents or guardians of all participants. The study was conducted in accordance with the principles of the Declaration of Helsinki and in compliance with the International Conference on Harmonization’s (ICH) Good Clinical Practice (GCP) guidelines [7]. The trial was registered with ClinicaTrials.gov as NCT00463684. Of 299 infants screened at enrollment, 278 were determined
to be eligible for participation, provided a pre-vaccination blood specimen, and received LJEV and measles vaccine (16 did not meet study inclusion criteria and 5 did not provide pre-vaccination blood specimens). All vaccinated subjects were included in safety analyses. Of those vaccinated, 53.2% were female and 93.9% were of Sinhalese ethnicity; their average age was 9.2 months (standard deviation, 0.3 months). After completion of the study, 257 participants were determined to meet criteria for entry into the per-protocol analysis of immunogenicity at 28 days weeks post-co-administration with study vaccines (13 were found to have been out of range for age at inclusion, 4 did not have the Day 28 blood specimen collected within range, and 4 were not able to provide sera at Day 28). A total of 274 subjects (98.