Nature Communications (Jul 2023)

Correlates of protection for booster doses of the SARS-CoV-2 vaccine BNT162b2

  • Tomer Hertz,
  • Shlomia Levy,
  • Daniel Ostrovsky,
  • Hanna Oppenheimer,
  • Shosh Zismanov,
  • Alona Kuzmina,
  • Lilach M. Friedman,
  • Sanja Trifkovic,
  • David Brice,
  • Lin Chun-Yang,
  • Liel Cohen-Lavi,
  • Yonat Shemer-Avni,
  • Merav Cohen-Lahav,
  • Doron Amichay,
  • Ayelet Keren-Naus,
  • Olga Voloshin,
  • Gabriel Weber,
  • Ronza Najjar-Debbiny,
  • Bibiana Chazan,
  • Maureen A. McGargill,
  • Richard Webby,
  • Michal Chowers,
  • Lena Novack,
  • Victor Novack,
  • Ran Taube,
  • Lior Nesher,
  • Orly Weinstein

DOI
https://doi.org/10.1038/s41467-023-39816-4
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 16

Abstract

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Abstract Vaccination, especially with multiple doses, provides substantial population-level protection against COVID-19, but emerging variants of concern (VOC) and waning immunity represent significant risks at the individual level. Here we identify correlates of protection (COP) in a multicenter prospective study following 607 healthy individuals who received three doses of the Pfizer-BNT162b2 vaccine approximately six months prior to enrollment. We compared 242 individuals who received a fourth dose to 365 who did not. Within 90 days of enrollment, 239 individuals contracted COVID-19, 45% of the 3-dose group and 30% of the four-dose group. The fourth dose elicited a significant rise in antibody binding and neutralizing titers against multiple VOCs reducing the risk of symptomatic infection by 37% [95%CI, 15%-54%]. However, a group of individuals, characterized by low baseline titers of binding antibodies, remained susceptible to infection despite significantly increased neutralizing antibody titers upon boosting. A combination of reduced IgG levels to RBD mutants and reduced VOC-recognizing IgA antibodies represented the strongest COP in both the 3-dose group (HR = 6.34, p = 0.008) and four-dose group (HR = 8.14, p = 0.018). We validated our findings in an independent second cohort. In summary combination IgA and IgG baseline binding antibody levels may identify individuals most at risk from future infections.