Comparison of two schedules of two-dose priming with the ten-valent pneumococcal conjugate vaccine in Nepalese children: an open-label, randomised non-inferiority controlled trial

Nepalese infants receive ten-valent pneumococcal conjugate vaccine (PCV10) with a 1 month interval between priming doses for programmatic reasons. We aimed to investigate whether immune responses to PCV10 serotypes were non-inferior if the second priming dose of PCV10 was delivered at a 1 month inte...

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Bibliographic Details
Published in:The Lancet infectious diseases 2019-02, Vol.19 (2), p.156-164
Main Authors: Kandasamy, Rama, Gurung, Meeru, Thorson, Stephen, Yu, Ly-Mee, Galal, Ushma, Voysey, Merryn, Kelly, Sarah, Wahl, Brian, Berbers, Guy, Finnegan, Kier, Ansari, Imran, Paudel, Krishna, Murdoch, David R, O'Brien, Katherine L, Kelly, Dominic F, Goldblatt, David, Shrestha, Shrijana, Pollard, Andrew J
Format: Article
Language:English
Subjects:
Age
Antibodies
Antibodies, Bacterial - blood
Bacillus Calmette-Guerin vaccine
BCG
Children
Conjugates
Disease
Enzyme-linked immunosorbent assay
Family medical history
Female
Gestation
Herd immunity
Hospitals
Humans
Immune response
Immunity
Immunity, Herd
Immunization
Immunization Schedule
Immunization, Secondary - methods
Immunogenicity
Immunogenicity, Vaccine
Immunoglobulin G
Immunoglobulin G - blood
Infant
Infants
Infectious diseases
Male
Nepal - epidemiology
Pneumococcal Infections - epidemiology
Pneumococcal Infections - microbiology
Pneumococcal Infections - prevention & control
Pneumococcal Vaccines - immunology
Pneumococcal Vaccines - therapeutic use
Poliomyelitis
Priming
Randomization
Schedules
Serogroup
Serotypes
Streptococcus infections
Streptococcus pneumoniae - immunology
Studies
Systematic review
Treatment Outcome
Vaccines
Vaccines, Conjugate - immunology
Vaccines, Conjugate - therapeutic use
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Summary:Nepalese infants receive ten-valent pneumococcal conjugate vaccine (PCV10) with a 1 month interval between priming doses for programmatic reasons. We aimed to investigate whether immune responses to PCV10 serotypes were non-inferior if the second priming dose of PCV10 was delivered at a 1 month interval as opposed to a 2 month interval. We did an open-label, randomised, parallel group trial in healthy Nepalese infants aged 40–60 days at Patan Hospital, Kathmandu, Nepal. Children were eligible for inclusion if they were healthy, were born at more than or equal to 37 weeks' gestation, were residing in Kathmandu, and had not had any previous vaccinations other than BCG, and oral polio vaccine. Participants were randomly assigned (1:1) by means of a computer-generated list with randomly varying permuted block sizes accessed through a validated web-based interface, to receive PCV10 either at 6 weeks and 10 weeks of age (6 + 10 group) or at 6 weeks and 14 weeks of age (6 + 14 group), with both groups receiving a booster at 9 months of age. Laboratory staff, masked to study intervention, analysed serum samples for antibodies against PCV10 serotypes by ELISA. The primary outcome was to determine whether the 6 + 10 schedule was non-inferior to the 6 + 14 schedule at 9 months of age, on the basis of the proportion of infants with serotype-specific IgG greater than or equal to 0·35 μg/mL. Non-inferiority was established with a 10% margin, and the primary endpoint was measured in a modified intention-to-treat population, which included only participants who successfully had a blood sample collected. This trial is registered at ClinicalTrials.gov, number NCT02385513. Between Aug 21, 2015, and April 4, 2016, 304 Nepalese children were randomly assigned to either the 6 + 10 group (n=152) or the 6 + 14 group (n=152). At 9 months of age, the 6 + 10 schedule was non-inferior for serotype 5 (79 [55·2%] of 143 vs 78 [53·4%] of 146, difference 1·82% [95% CI −9·6 to 13·25], p=0·021), serotype 9V (66 [46·1%] of 143 vs 55 [37·6%] of 146, difference 8·48% [−2·84 to 19·8], p=0·001), serotype 14 (110 [77·4%] of 142 vs 110 [74·8%] of 147, difference 2·63% [−7·27 to 12·54], p=0·006), and serotype 19F (135 [95%] of 142 vs 146 [100%] of 146, difference −4·92% [−9·86 to 0], p=0·022). At the same timepoint, non-inferiority was not shown for serotype 1 (36 [25·1%] of 143 vs 42 [28·5%] of 147, difference −3·39% [95% CI −13·56 to 6·77], p=0·102), serotype 4 (70 [48·9%] of 143 vs 87 [59·1%] o
ISSN:1473-3099
1474-4457
DOI:10.1016/S1473-3099(18)30568-1