Background: Two new formulations of an investigational 15-valent pneumococcal conjugate vaccine (PCV15-A and PCV15-B) were developed using 2 different protein-polysaccharide conjugation processes and evaluated in separate phase I/II studies (NCT02037984 [V114-004] and NCT02531373 [V114-005]) to assess optimal concentrations of pneumococcal polysaccharide (PnPs) and Aluminum Phosphate Adjuvant. Methods: Various lots of PCV15-A and PCV15-B containing different concentrations of PnPs and/or adjuvant were compared to PCV13 in young adults and infants. Adults received single dose and infants received 4 doses at 2, 4, 6, and 12-15 months of age. Adverse events (AEs) were collected after each dose. Serotype-specific immunoglobulin G (IgG) concentrations and opsonophagocytic activity (OPA) were measured prior and 30 days postvaccination in adults, at 1 month postdose 3 (PD3), pre-dose4, and postdose 4 (PD4) in infants. Results: Safety profiles were comparable across vaccination groups. At PD3, serotype-specific IgG GMCs were generally lower for either PCV15 formulation than PCV13 for most shared serotypes. PCV15 consistently elicited higher antibody responses to the 2 serotypes unique to the vaccine (22F and 33F) and serotype 3 for which PCV13 was shown to be ineffective. Except for serotypes 6A and 6B, no dose-response effect was observed with increasing concentrations of PnPs and/or adjuvant. Conclusion: PCV15 is safe and induces IgG and OPA responses to all 15 serotypes in the vaccine. No significant differences in antibody responses were observed with increases in PnPs and/or Aluminum Phosphate Adjuvant.
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Univ Witwatersrand, Perinatal HIV Res Unit, Johannesburg, South AfricaUniv Witwatersrand, Perinatal HIV Res Unit, Johannesburg, South Africa
Mohapi, L.
Osiyemi, O.
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Triple O Res Inst, Infect Dis, W Palm Beach, FL USAUniv Witwatersrand, Perinatal HIV Res Unit, Johannesburg, South Africa
Osiyemi, O.
Supparatpinyo, K.
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Chiang Mai Univ, Dept Internal Med, Chiang Mai, ThailandUniv Witwatersrand, Perinatal HIV Res Unit, Johannesburg, South Africa
Supparatpinyo, K.
Ratanasuwan, W.
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Mahidol Univ, Dept Prevent & Social Med, Siriraj Hosp, Nakhon Pathom, ThailandUniv Witwatersrand, Perinatal HIV Res Unit, Johannesburg, South Africa
Ratanasuwan, W.
Molina, J.
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Assistance Publ Hop Paris, Infect Dis, Paris, FranceUniv Witwatersrand, Perinatal HIV Res Unit, Johannesburg, South Africa
Molina, J.
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Dagan, R.
Tamms, G.
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Merck & Co Inc, Clin Res, Kenilworth, NJ USAUniv Witwatersrand, Perinatal HIV Res Unit, Johannesburg, South Africa
Tamms, G.
Sterling, T.
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Merck & Co Inc, Clin Res, Kenilworth, NJ USAUniv Witwatersrand, Perinatal HIV Res Unit, Johannesburg, South Africa
Sterling, T.
Zhang, Y.
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Merck & Co Inc, Clin Res, Kenilworth, NJ USAUniv Witwatersrand, Perinatal HIV Res Unit, Johannesburg, South Africa
Zhang, Y.
Hartzel, J.
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Merck & Co Inc, Clin Res, Kenilworth, NJ USAUniv Witwatersrand, Perinatal HIV Res Unit, Johannesburg, South Africa
Hartzel, J.
Pedley, A.
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Merck & Co Inc, Clin Res, Kenilworth, NJ USAUniv Witwatersrand, Perinatal HIV Res Unit, Johannesburg, South Africa
Pedley, A.
Kan, Y.
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Merck & Co Inc, Clin Res, Kenilworth, NJ USAUniv Witwatersrand, Perinatal HIV Res Unit, Johannesburg, South Africa
Kan, Y.
Hurtado, K.
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Merck & Co Inc, Clin Res, Kenilworth, NJ USAUniv Witwatersrand, Perinatal HIV Res Unit, Johannesburg, South Africa
Hurtado, K.
Buchwald, U.
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Merck & Co Inc, Clin Res, Kenilworth, NJ USAUniv Witwatersrand, Perinatal HIV Res Unit, Johannesburg, South Africa
Buchwald, U.
Musey, L.
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Merck & Co Inc, Clin Res, Kenilworth, NJ USAUniv Witwatersrand, Perinatal HIV Res Unit, Johannesburg, South Africa
Musey, L.
Simon, J.
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Merck & Co Inc, Clin Res, Kenilworth, NJ USAUniv Witwatersrand, Perinatal HIV Res Unit, Johannesburg, South Africa