Subclass and avidity of circumsporozoite protein specific antibodies associate with protection status against malaria infection
- PMID: 34462438
- PMCID: PMC8405700
- DOI: 10.1038/s41541-021-00372-x
Subclass and avidity of circumsporozoite protein specific antibodies associate with protection status against malaria infection
Abstract
RTS,S/AS01 is an advanced pre-erythrocytic malaria vaccine candidate with demonstrated vaccine efficacy up to 86.7% in controlled human malaria infection (CHMI) studies; however, reproducible immune correlates of protection (CoP) are elusive. To identify candidates of humoral correlates of vaccine mediated protection, we measured antibody magnitude, subclass, and avidity for Plasmodium falciparum (Pf) circumsporozoite protein (CSP) by multiplex assays in two CHMI studies with varying RTS,S/AS01B vaccine dose and timing regimens. Central repeat (NANP6) IgG1 magnitude correlated best with protection status in univariate analyses and was the most predictive for protection in a multivariate model. NANP6 IgG3 magnitude, CSP IgG1 magnitude, and total serum antibody dissociation phase area-under-the-curve for NANP6, CSP, NPNA3, and N-interface binding were also associated with protection status in the regimen adjusted univariate analysis. Identification of multiple immune response features that associate with protection status, such as antibody subclasses, fine specificity and avidity reported here may accelerate development of highly efficacious vaccines against P. falciparum.
© 2021. The Author(s).
Conflict of interest statement
E.J., F.U.M. and M.C. are employees of the GSK group of companies and hold shares or restricted shares in the GSK group of companies. G.D.T. was a recipient of a research subcontract through Duke University from GSK and Macrogenics for work unrelated to this study. U.W.R. became an employee of GSK group of companies during the review of this manuscript.
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