Skip to main content

Lund University Publications

LUND UNIVERSITY LIBRARIES

Relationship between antibody avidity, Fc-mediated functional activity and longevity of malaria vaccine responses in clinical trials

Horton, Jessica L. ; Chan, Jo Anne ; Kurtovic, Liriye ; Reiling, Linda ; Feng, Gaoqian ; Persson, Kristina E.M. LU orcid ; Sacarlal, Jahit ; Anders, Robin F. ; McCarthy, James S. and Dobaño, Carlota , et al. (2026) In Frontiers in Immunology 17.
Abstract

Background – Advancing the development of highly efficacious and long-lasting malaria vaccines is hampered by incomplete knowledge of protective immune mechanisms and an absence of established correlates of immunity. Antibody avidity is frequently evaluated as an indicator of a high-quality or protective antibody response to vaccination. However, the importance of avidity in vaccine-induced immunity to malaria remains unclear. Methods/approach – We investigated the association between antibody avidity, Fc-mediated functional activities, and antibody longevity in two different Plasmodium falciparum vaccine trials; a phase 1 trial of merozoite surface protein 2 in malaria-naïve adults, and a phase 2b trial of the RTS, S vaccine in African... (More)

Background – Advancing the development of highly efficacious and long-lasting malaria vaccines is hampered by incomplete knowledge of protective immune mechanisms and an absence of established correlates of immunity. Antibody avidity is frequently evaluated as an indicator of a high-quality or protective antibody response to vaccination. However, the importance of avidity in vaccine-induced immunity to malaria remains unclear. Methods/approach – We investigated the association between antibody avidity, Fc-mediated functional activities, and antibody longevity in two different Plasmodium falciparum vaccine trials; a phase 1 trial of merozoite surface protein 2 in malaria-naïve adults, and a phase 2b trial of the RTS, S vaccine in African children. Results – In both trials, we found that the magnitude of IgG induced by vaccination correlated strongly with antibody avidity indicating the two vaccine immunogenicity outcomes are related. Antibody avidity was not a major determinant of Fc-mediated functional activity, including complement fixation, binding of Fcγ-receptors, or opsonic phagocytosis. In analysis models, IgG magnitude was a stronger determinant of function than IgG avidity. Although avidity positively correlated with antibody functional activities, this was largely due to the confounding effect of the correlation between IgG magnitude and Fc functional activity. Additionally, we found that antibody avidity showed only a weak and antigen-specific association with antibody longevity. Similar findings in the two vaccine trials, which differed by vaccine antigen, adjuvant, and age group, suggests that these observations are likely to be generalisable and not specific to a vaccine type. Conclusion – Antibody avidity was not a better predictor of Fc-mediated functional activity than antibody magnitude and avidity was not a strong correlate of antibody longevity. These findings suggest that vaccine approaches that focus on increasing antibody avidity per se may not be sufficient to achieve more efficacious or long-lasting vaccines.

(Less)
Please use this url to cite or link to this publication:
author
; ; ; ; ; ; ; ; and , et al. (More)
; ; ; ; ; ; ; ; ; ; and (Less)
organization
publishing date
type
Contribution to journal
publication status
published
subject
keywords
affinity, children, complement, Fc-mediated antibody functions, malaria, phagocytosis, vaccines
in
Frontiers in Immunology
volume
17
article number
1808822
publisher
Frontiers Media S. A.
external identifiers
  • pmid:42023224
  • scopus:105036608084
ISSN
1664-3224
DOI
10.3389/fimmu.2026.1808822
language
English
LU publication?
yes
id
0dafc0cd-146d-440a-a295-6b781a3aa281
date added to LUP
2026-06-24 09:26:20
date last changed
2026-06-25 03:00:08
@article{0dafc0cd-146d-440a-a295-6b781a3aa281,
  abstract     = {{<p>Background – Advancing the development of highly efficacious and long-lasting malaria vaccines is hampered by incomplete knowledge of protective immune mechanisms and an absence of established correlates of immunity. Antibody avidity is frequently evaluated as an indicator of a high-quality or protective antibody response to vaccination. However, the importance of avidity in vaccine-induced immunity to malaria remains unclear. Methods/approach – We investigated the association between antibody avidity, Fc-mediated functional activities, and antibody longevity in two different Plasmodium falciparum vaccine trials; a phase 1 trial of merozoite surface protein 2 in malaria-naïve adults, and a phase 2b trial of the RTS, S vaccine in African children. Results – In both trials, we found that the magnitude of IgG induced by vaccination correlated strongly with antibody avidity indicating the two vaccine immunogenicity outcomes are related. Antibody avidity was not a major determinant of Fc-mediated functional activity, including complement fixation, binding of Fcγ-receptors, or opsonic phagocytosis. In analysis models, IgG magnitude was a stronger determinant of function than IgG avidity. Although avidity positively correlated with antibody functional activities, this was largely due to the confounding effect of the correlation between IgG magnitude and Fc functional activity. Additionally, we found that antibody avidity showed only a weak and antigen-specific association with antibody longevity. Similar findings in the two vaccine trials, which differed by vaccine antigen, adjuvant, and age group, suggests that these observations are likely to be generalisable and not specific to a vaccine type. Conclusion – Antibody avidity was not a better predictor of Fc-mediated functional activity than antibody magnitude and avidity was not a strong correlate of antibody longevity. These findings suggest that vaccine approaches that focus on increasing antibody avidity per se may not be sufficient to achieve more efficacious or long-lasting vaccines.</p>}},
  author       = {{Horton, Jessica L. and Chan, Jo Anne and Kurtovic, Liriye and Reiling, Linda and Feng, Gaoqian and Persson, Kristina E.M. and Sacarlal, Jahit and Anders, Robin F. and McCarthy, James S. and Dobaño, Carlota and Boyle, Michelle J. and Beeson, James G.}},
  issn         = {{1664-3224}},
  keywords     = {{affinity; children; complement; Fc-mediated antibody functions; malaria; phagocytosis; vaccines}},
  language     = {{eng}},
  publisher    = {{Frontiers Media S. A.}},
  series       = {{Frontiers in Immunology}},
  title        = {{Relationship between antibody avidity, Fc-mediated functional activity and longevity of malaria vaccine responses in clinical trials}},
  url          = {{http://dx.doi.org/10.3389/fimmu.2026.1808822}},
  doi          = {{10.3389/fimmu.2026.1808822}},
  volume       = {{17}},
  year         = {{2026}},
}