The effect of BCG revaccination on the response to unrelated vaccines in urban Ugandan adolescents (POPVAC C): an open-label, randomised controlled trial

Immune responses induced by several important vaccines differ between populations, with reduced responses in low-income and rural settings compared with high-income and urban settings. BCG immunisation boosts immune responses to some unrelated vaccines in high-income populations. We aimed to test th...

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Veröffentlicht in:The Lancet global health 2024-11, Vol.12 (11), p.e1849-e1859
Hauptverfasser: Nassuuna, Jacent, Zirimenya, Ludoviko, Nkurunungi, Gyaviira, Natukunda, Agnes, Zziwa, Christopher, Ninsiima, Caroline, Apule, Barbara, Onen, Caroline, Amongi, Susan, Serubanja, Joel, Tumwesige, Pius, Nsubuga, Denis, Amongin, Rebecca, van Dam, Govert J, Corstjens, Paul L A M, Kayiwa, John, Kabagenyi, Joyce, Cose, Stephen, Wajja, Anne, Kaleebu, Pontiano, Webb, Emily L, Elliott, Alison M, Akello, Mirriam, Akello, Florence A, Akurut, Hellen, Driciru, Emmanuella, Kabali, Joel, Kabami, Grace, Kabuubi, Prossy N, Kakande, Ayoub, Katushabe, Charity, Kiwanuka, Samuel, Kiwudhu, Fred, Kizindo, Robert, Kizza, Moses, Kukundakwe, Christine, Mutebe, Alex, Nakazibwe, Esther, Namusobya, Loyce, Namutebi, Milly, Nankabirwa, Christine, Nassanga, Beatrice, Nayebare, Doreen, Nkangi, Ronald, Nyanzi, Ruth, Oduru, Gloria, Sewankambo, Moses, Tumusiime, Josephine, Walusimbi, Bridgious
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Zusammenfassung:Immune responses induced by several important vaccines differ between populations, with reduced responses in low-income and rural settings compared with high-income and urban settings. BCG immunisation boosts immune responses to some unrelated vaccines in high-income populations. We aimed to test the hypothesis that BCG revaccination can enhance responses to unrelated vaccines in Ugandan schoolchildren. We conducted an open-label, randomised controlled trial to compare the effects of BCG revaccination versus no BCG revaccination on the immunogenicity of subsequent unrelated vaccines among adolescents aged 13–17 years who are participants in an urban Ugandan birth cohort study, in which BCG vaccination was documented at birth. Participants were excluded if they had received any of the trial vaccines or related agents when aged 5 years or older. Computer-generated 1:1 randomisation was implemented in REDCap. Participants were excluded if they were concurrently enrolled in other trials; had a clinically significant history of immunodeficiency, or serious psychiatric conditions or moderate to severe acute illnesses; were taking immunosuppressive medications; had allergies to vaccine components, a predisposition towards developing keloid scarring; positive HIV tests or pregnancy tests; were female participants who were lactating; or if they planned to use investigational drugs, vaccines, blood products, or any combination thereof. Trial participants assigned to the BCG revaccination group received the live parenteral BCG-Russia vaccine (Serum Institute of India, Pune, India; 0·1 mL intradermally, right upper arm) at week 0. All participants received yellow fever vaccine (YF-17D; Sanofi Pasteur, Lyon, France; 0·5 mL intramuscularly, left upper arm), live oral typhoid vaccine (Ty21a; PaxVax, London, UK; one capsule per day taken for three alternate days), and quadrivalent virus-like particle human papillomavirus (HPV) vaccine (Merck, Rahway, NJ, USA; 0·5 mL intramuscularly, left upper arm) at week 4; and toxoid vaccines (tetanus–diphtheria; Serum Institute of India; 0·5 mL intramuscularly, left upper arm) and an HPV booster at week 28. An additional HPV vaccination at week 8 was provided to female participants older than 14 years who had not previously been vaccinated. The primary outcomes were yellow fever neutralising antibody titres at 4 weeks post-YF-17D vaccination, Salmonella enterica serovar Typhi (henceforth S Typhi) O-lipopolysaccharide (O:LPS)-specific
ISSN:2214-109X
2214-109X
DOI:10.1016/S2214-109X(24)00282-1