Emergence of the B.1.214.2 SARS-CoV-2 lineage with an Omicron-like spike insertion and a unique upper airway immune signature

Author:

Holtz Andrew1,Weyenbergh Johan2,Hong Samuel L.2,Cuypers Lize2,O’Toole Áine3,Dudas Gytis4,Gerdol Marco5,Potter Barney I.2,Ntoumi Francine6,Mapanguy Claujens Chastel Mfoutou6,Vanmechelen Bert2,Wawina-Bokalanga Tony2,Bram Van Holm2,Menezes Soraya Maria2,Katja Soubotko2,Pottelbergh Gijs Van2,Wollants Elke2,Vermeersch Pieter2,Jacob Ann-Sophie2,Maes Brigitte7,Obbels Dagmar8,Matheeussen Veerle9,Martens Geert10,Gras Jérémie11,Verhasselt Bruno8,Laffut Wim2,Vael Carl12,Goegebuer Truus13,Kant Rob van der2,Rousseau Frederic2,Schymkotwitz Joost2,Serrano Luis14,Delgado Javier15,Wenseleers Tom2,Bours Vincent16,André Emmanuel2,Suchard Marc A.17,Rambaut Andrew3,Dellicour Simon2,Maes Piet2,Durkin Keith18,Baele Guy2

Affiliation:

1. Institut Pasteur, Université Paris Cité

2. Rega Institute, KU Leuven

3. University of Edinburgh

4. Vilnius University

5. University of Trieste

6. Fondation Congolaise Pour La Recherche Médicale

7. Jessa Hospital

8. University of Ghent

9. Antwerp University Hospital (UZA)

10. AZ Delta General Hospital

11. Institut de Pathologie et de Génétique

12. AZ KLINA General Hospital

13. AZ Sint-Maarten

14. Barcelona Institute for Science and Technology

15. Institució Catalana de Recerca i Estudis Avançats

16. CHU Liege

17. University of California, Los Angeles

18. GIGA Research Institute

Abstract

Abstract

We investigate the emergence, mutation profile, and dissemination of SARS-CoV-2 lineage B.1.214.2, first identified in Belgium in January 2021. This variant, featuring a 3-amino acid insertion in the spike protein similar to the Omicron variant, was speculated to enhance transmissibility or immune evasion. Initially detected in international travelers, it substantially transmitted in Central Africa, Belgium, Switzerland, and France, peaking in April 2021. Our travel-aware phylogeographic analysis, incorporating travel history, estimated the origin to the Republic of the Congo, with primary European entry through France and Belgium, and multiple smaller introductions during the epidemic. We correlate its spread with human travel patterns and air passenger data. Further, upon reviewing national reports of SARS-CoV-2 outbreaks in Belgian nursing homes, we found this strain caused moderately severe outcomes (8.7% case fatality ratio). A distinct nasopharyngeal immune response was observed in elderly patients, characterized by 80% unique signatures, higher B- and T-cell activation, increased type I IFN signaling, and reduced NK, Th17, and complement system activation, compared to similar outbreaks. This unique immune response may explain the variant's epidemiological behavior and underscores the need for nasal vaccine strategies against emerging variants.

Publisher

Research Square Platform LLC

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