Prior infection with SARS-CoV-2 boosts and broadens Ad26.COV2.S immunogenicity in a variant-dependent manner

既往感染SARS-CoV-2可增强并拓宽Ad26.COV2.S的免疫原性,且这种增强和拓宽作用取决于病毒株类型。

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作者:Roanne Keeton,Simone I Richardson,Thandeka Moyo-Gwete,Tandile Hermanus,Marius B Tincho,Ntombi Benede,Nelia P Manamela,Richard Baguma,Zanele Makhado,Amkele Ngomti,Thopisang Motlou,Mathilda Mennen,Lionel Chinhoyi,Sango Skelem,Hazel Maboreke,Deelan Doolabh,Arash Iranzadeh,Ashley D Otter,Tim Brooks,Mahdad Noursadeghi,James C Moon,Alba Grifoni,Daniela Weiskopf,Alessandro Sette,Jonathan Blackburn,Nei-Yuan Hsiao,Carolyn Williamson,Catherine Riou,Ameena Goga,Nigel Garrett,Linda-Gail Bekker,Glenda Gray,Ntobeko A B Ntusi,Penny L Moore,Wendy A Burgers

Abstract

The Johnson and Johnson Ad26.COV2.S single-dose vaccine represents an attractive option for coronavirus disease 2019 (COVID-19) vaccination in countries with limited resources. We examined the effect of prior infection with different SARS-CoV-2 variants on Ad26.COV2.S immunogenicity. We compared participants who were SARS-CoV-2 naive with those either infected with the ancestral D614G virus or infected in the second wave when Beta predominated. Prior infection significantly boosts spike-binding antibodies, antibody-dependent cellular cytotoxicity, and neutralizing antibodies against D614G, Beta, and Delta; however, neutralization cross-reactivity varied by wave. Robust CD4 and CD8 T cell responses are induced after vaccination, regardless of prior infection. T cell recognition of variants is largely preserved, apart from some reduction in CD8 recognition of Delta. Thus, Ad26.COV2.S vaccination after infection could result in enhanced protection against COVID-19. The impact of the infecting variant on neutralization breadth after vaccination has implications for the design of second-generation vaccines based on variants of concern.

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