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Immunogenicity and safety of a 10-valent pneumococcal conjugate vaccine administered as a 2 + 1 schedule to healthy infants in The Gambia: a single-centre, double-blind, active-controlled, randomised, phase 3 trial - 20/04/23

Doi : 10.1016/S1473-3099(22)00734-4 
Ikechukwu Adigweme, MBBS a, Ahmed Futa, MD a, Ebrima Saidy-Jah, MBChB a, Bassey Edem, MBBCh a, Edem Akpalu, MD a, Tida Dibbasey, MBChB a, Vistasp Sethna, MBBS c, Rajeev Dhere, PhD c, Beate Kampmann, ProfPhD a, b, Christopher Bengt d, Jake Sirr, BSc d, Nancy Hosken, PhD e, David Goldblatt, ProfMBChB d, Kalpana Antony, BSc e, Mark R Alderson, PhD e, Steve Lamola, MD e, , Ed Clarke, MBChB a, b, ,
a Medical Research Council Unit The Gambia at the London School of Hygiene & Tropical Medicine, Banjul, The Gambia 
b The Vaccine Centre, London School of Hygiene & Tropical Medicine, London, UK 
c Serum Institute of India, Pune, India 
d Great Ormond Street Institute of Child Health Biomedical Research Centre, University College London, London, UK 
e PATH, Seattle, WA, USA 

* Correspondence to: Dr Ed Clarke, Medical Research Council Unit The Gambia at the London School of Hygiene & Tropical Medicine, PO Box 273, Banjul, The Gambia Medical Research Council Unit The Gambia at the London School of Hygiene & Tropical Medicine Banjul PO Box 273 The Gambia

Summary

Background

Three pneumococcal conjugate vaccines (PCVs) are currently licensed and WHO prequalified for supply by UN agencies. Here, we aimed to investigate the safety and immunogenicity of SIIPL-PCV compared with PHiD-CV and PCV13, when administered to infants according to a 2 + 1 schedule.

Methods

This single-centre, double-blind, active-controlled, randomised, phase 3 trial was done in Medical Research Council Unit The Gambia at the London School of Hygiene & Tropical Medicine clinical trial facilities within two government health centres in the western region of The Gambia. Healthy, PCV-naive infants aged 6–8 weeks were enrolled if they weighed at least 3·5 kg and had no clinically significant health complaints, as determined by history and clinical examination. Eligible infants were randomly assigned (1:1:1) to receive either SIIPL-PCV, PHiD-CV, or PCV13 using permuted blocks of variable size. Parents and the trial staff assessing all study outcomes were masked to vaccine group. The first PCV vaccine was given with other routine Expanded Programme on Immunization vaccines when infants were aged 6–8 weeks (visit 1). At visit 2, routine vaccines alone (without a PCV) were administered. At visit 3, the second dose of the PCV was administered alongside other routine vaccines. At visit 4, a blood sample was collected. Visits 1–4 took place at intervals of 4 weeks. The booster PCV was administered at age 9–18 months (visit 5), with final follow-up 4 weeks after the booster (visit 6). The primary immunogenicity outcome compared the serotype-specific IgG geometric mean concentrations (GMCs) generated by SIIPL-PCV with those generated by PHiD-CV and PCV13, 4 weeks after the booster. We used descriptive 95% CIs without adjustment for multiplicity. Immunogenicity analyses were done in the per protocol population (defined as all children who received all the assigned study vaccines, who had an immunogenicity measurement available, and who had no protocol deviations that might interfere with the immunogenicity assessment). This trial was registered with the Pan African Clinical Trials Registry, PACTR201907754270299, and ClinicalTrials.gov, NCT03896477.

Findings

Between July 18 and Nov 14, 2019, 745 infants were assessed for study eligibility. Of these, 85 infants (11%) were ineligible and 660 (89%) were enrolled and randomly assigned to receive SIIPL-PCV (n=220), PHiD-CV (n=220), or PCV13 (n=220). 602 infants (91%) were included in the per protocol immunogenicity population. The median age at vaccination was 46 days (range 42–56). 342 infants (52%) were female and 318 (48%) were male. Post-booster serotype-specific IgG GMCs generated by SIIPL-PCV ranged from 1·54 μg/mL (95% CI 1·38–1·73) for serotype 5 to 12·46 μg/mL (11·07–14·01) for serotype 6B. Post-booster GMCs against shared serotypes generated by PHiD-CV ranged from 0·80 μg/mL (0·72–0·88) for serotype 5 to 17·31 μg/mL (14·83–20·20) for serotype 19F. Post-booster GMCs generated by PCV13 ranged from 2·04 μg/mL (1·86–2·24) for serotype 5 to 15·54 μg/mL (13·71–17·60) for serotype 6B. Post-booster IgG GMCs generated by SIIPL-PCV were higher than those generated by PHiD-CV for seven of the eight shared serotypes (1, 5, 6B, 7F, 9V, 14, and 23F). The GMC generated by serotype 19F was higher after PHiD-CV. The SIIPL-PCV to PHiD-CV GMC ratios for shared serotypes ranged from 0·64 (95% CI 0·52–0·79) for serotype 19F to 2·91 (2·47–3·44) for serotype 1. The serotype 1 GMC generated by SIIPL-PCV was higher than that generated by PCV13, whereas serotype 5, 6A, 19A, and 19F GMCs were higher after PCV13. The SIIPL-PCV to PCV13 GMC ratios ranged from 0·72 (0·60–0·87) for serotype 19A to 1·44 (1·23–1·69) for serotype 1.

Interpretation

SIIPL-PCV was safe and immunogenic when given to infants in The Gambia according to a 2 + 1 schedule. This PCV is expected to provide similar protection against invasive and mucosal pneumococcal disease to the protection provided by PCV13 and PHiD-CV, for which effectiveness data are available. Generating post-implementation data on the impact of SIIPL-PCV on pneumococcal disease endpoints remains important.

Funding

Bill & Melinda Gates Foundation.

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© 2023  The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license. Publié par Elsevier Masson SAS. Tous droits réservés.
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P. 609-620 - mai 2023 Retour au numéro
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