Immunogenicity and Safety of a Newly Developed Live Attenuated Varicella Vaccine in Healthy Children: A Multi-National, Randomized, Double-Blinded, Active-Controlled, Phase 3 Study
Ui Yoon Choi,
Ki Hwan Kim,
Hye-Kyung Cho,
Dong Ho Kim,
Sang Hyuk Ma,
Young Youn Choi,
Chun Soo Kim,
Maria Rosario Capeding,
Ilya Angelica Rochin Kobashi,
Hun Kim,
Ji Hwa Ryu,
Su Jeen Lee,
Ho Keun Park,
Jong-Hyun Kim
Affiliations
Ui Yoon Choi
Department of Pediatrics, Eunpyeong St. Mary’s Hospital, College of Medicine, The Catholic University of Korea, Seoul 03312, Republic of Korea
Ki Hwan Kim
Department of Pediatrics, Incheon St. Mary’s Hospital, College of Medicine, The Catholic University of Korea, Seoul 21431, Republic of Korea
Hye-Kyung Cho
Department of Pediatrics, Gachon University College of Medicine, Incheon 21936, Republic of Korea
Dong Ho Kim
Department of Pediatrics, Korea Cancer Center Hospital, Seoul 01812, Republic of Korea
Sang Hyuk Ma
Department of Pediatrics, Changwon Fatima Hospital, Changwon 51394, Republic of Korea
Young Youn Choi
Department of Pediatrics, Chonnam National University Medical School, Gwangju 61469, Republic of Korea
Chun Soo Kim
Department of Pediatrics, Keimyung University School of Medicine, Daegu 42601, Republic of Korea
Maria Rosario Capeding
Department of Microbiology, Research Institute for Tropical Medicine, Manila 1781, Philippines
Ilya Angelica Rochin Kobashi
Centro de Investigacion Clinica del Pacifico, Acapulco 39680, Mexico
Hun Kim
SK Bioscience, Seongnam 13494, Republic of Korea
Ji Hwa Ryu
SK Bioscience, Seongnam 13494, Republic of Korea
Su Jeen Lee
SK Bioscience, Seongnam 13494, Republic of Korea
Ho Keun Park
SK Bioscience, Seongnam 13494, Republic of Korea
Jong-Hyun Kim
Department of Pediatrics, St. Vincent’s Hospital, College of Medicine, The Catholic University of Korea, Suwon 16247, Republic of Korea
Korean manufacturers have developed a new varicella vaccine, NBP608. This phase 3, randomized, double-blind, multicenter study aimed to compare the immunogenicity and safety of NBP608 in healthy children to those of VarivaxTM (control). Children aged 12 months to 12 years were randomized in a ratio of 1:1 to receive either NBP608 or the control vaccine. Serum samples were obtained before vaccination and within six to eight weeks after vaccination. In total, 499 participants (NBP608, n = 251; control, n = 248) were enrolled. The seroconversion rate (SCR) measured using a FAMA assay was 99.53% in the NBP608 group, and the lower limit of the 95% confidence interval (95% LCL) for the SCR difference (NBP608 minus the control) was 0.52%. This 95% LCL for the difference was higher than the specified non-inferiority margin of −15%. In an assessment using gpELISA, the SCR was 99.53% in the NBP608 group, and the 95% LCL for the SCR difference was 6.5%, which was higher than the specified non-inferiority margin of −15%. There were no significant differences between the NBP608 and control group with respect to the proportions of participants who demonstrated local and systemic solicited AEs. This study indicated that NBP608 had a clinically acceptable safety profile and was not immunologically inferior to VarivaxTM.
