Beta-variant recombinant SARS CoV-2 vaccine induces durable cross-reactive antibodies against Omicron BA variants

Odile Launay; Rachna Gupta; Tifany Machabert; Eleine Konate; Alexandra Rousseau; Claire Vigne; Francois Beckers; Louis Devlin; Elisabeth Botelho-Nevers; Marine Cachanado; Christian Chidiac; Dominique Deplanque; Bertrand Dussol; Inès Ben Ghezala; Marie Lachatre; Karine Lacombe; Fabrice Laine; Liem Binh Luong Nguyen; Patricia Pavese; Catherine Schmidt-Mutter; Marie-Pierre Tavolacci; Roman M. Chicz; Bogdana Coudsy; Saranya Sridhar; Amel Touati; Eric Tartour; Tabassome Simon

doi:10.1038/s43856-024-00675-9

Communications Medicine (Jan 2025)

Beta-variant recombinant SARS CoV-2 vaccine induces durable cross-reactive antibodies against Omicron BA variants

Odile Launay,
Rachna Gupta,
Tifany Machabert,
Eleine Konate,
Alexandra Rousseau,
Claire Vigne,
Francois Beckers,
Louis Devlin,
Elisabeth Botelho-Nevers,
Marine Cachanado,
Christian Chidiac,
Dominique Deplanque,
Bertrand Dussol,
Inès Ben Ghezala,
Marie Lachatre,
Karine Lacombe,
Fabrice Laine,
Liem Binh Luong Nguyen,
Patricia Pavese,
Catherine Schmidt-Mutter,
Marie-Pierre Tavolacci,
Roman M. Chicz,
Bogdana Coudsy,
Saranya Sridhar,
Amel Touati,
Eric Tartour,
Tabassome Simon

Affiliations

Odile Launay: Assistance Publique Hôpitaux Paris (APHP), Hôpital Cochin; Université Paris Cité; Inserm CIC 1417 Cochin Pasteur
Rachna Gupta: Sanofi
Tifany Machabert: Sanofi
Eleine Konate: Assistance Publique Hôpitaux Paris (APHP), Hôpital Cochin; Université Paris Cité; Inserm CIC 1417 Cochin Pasteur
Alexandra Rousseau: APHP, Hôpital Saint Antoine, Unité de Recherche Clinique (URCEST), Centre de Ressources Biologiques (CRB)
Claire Vigne: Sanofi
Francois Beckers: Sanofi
Louis Devlin: Sanofi
Elisabeth Botelho-Nevers: Service d’infectiologie, CIC1408, Inserm, CHU de Saint-Etienne
Marine Cachanado: APHP, Hôpital Saint Antoine, Unité de Recherche Clinique (URCEST), Centre de Ressources Biologiques (CRB)
Christian Chidiac: Maladies Infectieuses, GHN Croix Rousse, Hospices Civils de Lyon
Dominique Deplanque: Univ. Lille, Inserm, CHU Lille, CIC 1403 - Centre d’Investigation Clinique
Bertrand Dussol: CIC 14-09, INSERM - Aix Marseille Université – Hôpitaux Universitaires de Marseille
Inès Ben Ghezala: Inserm, CIC 1432, Clinical Investigation Center, Clinical Epidemiology/Clinical Trials Unit, University Hospital
Marie Lachatre: Assistance Publique Hôpitaux Paris (APHP), Hôpital Cochin; Université Paris Cité; Inserm CIC 1417 Cochin Pasteur
Karine Lacombe: Sorbonne Université, IPLESP Inserm UMR-S1136, Hôpital St Antoine AP-HP
Fabrice Laine: INSERM, CIC 1414, CHU Rennes
Liem Binh Luong Nguyen: Assistance Publique Hôpitaux Paris (APHP), Hôpital Cochin; Université Paris Cité; Inserm CIC 1417 Cochin Pasteur
Patricia Pavese: Maladies Infectieuses et Tropicales, CHU de Grenoble Alpes
Catherine Schmidt-Mutter: Inserm CIC 1434, CHU Strasbourg
Marie-Pierre Tavolacci: Université Rouen, Inserm 1073, CHU Rouen, CIC 1404 - Centre d’investigation clinique
Roman M. Chicz: Sanofi
Bogdana Coudsy: Sanofi
Saranya Sridhar: Sanofi
Amel Touati: APHP, Hôpital Saint Antoine, Unité de Recherche Clinique (URCEST), Centre de Ressources Biologiques (CRB)
Eric Tartour: APHP, Hôpital Européen Georges Pompidou; PARCC, INSERM U970 Université de Paris
Tabassome Simon: URC EST, Sorbonne Université

DOI: https://doi.org/10.1038/s43856-024-00675-9
Journal volume & issue: Vol. 5, no. 1
pp. 1 – 7

Abstract

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Abstract Background We previously reported the safety and immunogenicity data from a randomized trial comparing the booster responses of vaccinees who received monovalent (MV) recombinant protein Beta-variant (MVB.1.351) and MV ancestral protein (MVD614) vaccines with AS03 adjuvant (Sanofi/GSK) to booster response of vaccinees who received mRNA MV ancestral strain BNT162b2 vaccine (Pfizer-BioNTech). Methods First booster of the vaccines was administered in adult participants previously primed with 2 doses of MV ancestral strain BNT162b2. A subset of these participants with available blood samples collected at Day 0 (D0), at 28 days (D28), and 3 months (M3) post-booster were contacted for additional testing (195/208 participants). The persistence of cross-neutralizing antibodies, including against Omicron BA.1 and BA.4/5, up to 3 months after boosting was evaluated using a validated pseudovirus neutralization assay. Results Across the whole population, MVB.1.351 vaccine induces highest NAbs titers against Omicron BA.1 and BA.4/5 variants at D28 and M3 post-booster. In participants with SARS-CoV-2 infection between D28 and M3, both MVB.1.351 and BNT162b2 vaccine groups show an increase in GMTs against Omicron BA.1 and Omicron BA.4/5 following infection. Among uninfected participants, the ratio of M3 to D28 GMTs was higher for the MVB.1.351 group than the BNT162b2 group against Omicron BA.1 (0.64 [0.53;0.77] versus 0.43 [0.35;0.53]), Omicron BA.4/5 (0.61 [0.50; 0.75] versus 0.44 [0.34; 0.56]), and D614 (0.68 [0.58,0.81] versus 0.46 [0.39,0.55]). Conclusions The MVB.1.351 vaccine induces higher and durable cross-neutralizing antibodies against Omicron subvariants up to 3 months after boosting compared to an MV ancestral and mRNA BNT162b2 booster vaccine.

Published in Communications Medicine

ISSN: 2730-664X (Online)
Publisher: Nature Portfolio
Country of publisher: United Kingdom
LCC subjects: Medicine
Website: https://www.nature.com/commsmed/

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