Breakthrough infections by SARS-CoV-2 variants boost cross-reactive hybrid immune responses in mRNA-vaccinated Golden Syrian hamsters

SARS-CoV-2 变种病毒的突破性感染可增强接种 mRNA 疫苗的金丝鼠体内的交叉反应性混合免疫应答。

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作者:Juan García-Bernalt Diego ,Gagandeep Singh ,Sonia Jangra ,Kim Handrejk ,Manon Laporte ,Lauren A Chang ,Sara S El Zahed ,Lars Pache ,Max W Chang ,Prajakta Warang ,Sadaf Aslam ,Ignacio Mena ,Brett T Webb ,Christopher Benner ,Adolfo García-Sastre ,Michael Schotsaert

Abstract

Hybrid immunity (vaccination + natural infection) to SARS-CoV-2 provides superior protection to re-infection. We performed immune profiling studies during breakthrough infections in mRNA-vaccinated hamsters to evaluate hybrid immunity induction. The mRNA vaccine, BNT162b2, was dosed to induce binding antibody titers against ancestral spike, but inefficient serum virus neutralization of ancestral SARS-CoV-2 or variants of concern (VoCs). Vaccination reduced morbidity and controlled lung virus titers for ancestral virus and Alpha but allowed breakthrough infections in Beta, Delta and Mu-challenged hamsters. Vaccination primed for T cell responses that were boosted by infection. Infection back-boosted neutralizing antibody responses against ancestral virus and VoCs. Hybrid immunity resulted in more cross-reactive sera, reflected by smaller antigenic cartography distances. Transcriptomics post-infection reflects both vaccination status and disease course and suggests a role for interstitial macrophages in vaccine-mediated protection. Therefore, protection by vaccination, even in the absence of high titers of neutralizing antibodies in the serum, correlates with recall of broadly reactive B- and T-cell responses.

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