Paradoxical clade- and age-specific vaccine effectiveness during the 2018/19 influenza A(H3N2) epidemic in Canada: potential imprint-regulated effect of vaccine (I-REV)

Author:

Skowronski Danuta M12,Sabaiduc Suzana2,Leir Siobhan2,Rose Caren12,Zou Macy2,Murti Michelle34,Dickinson James A5,Olsha Romy4,Gubbay Jonathan B34,Croxen Matthew A67,Charest Hugues8,Bastien Nathalie9,Li Yan9,Jassem Agatha12,Krajden Mel12,De Serres Gaston10118

Affiliation:

1. University of British Columbia, Vancouver, Canada

2. British Columbia Centre for Disease Control, Vancouver, Canada

3. University of Toronto, Toronto, Canada

4. Public Health Ontario, Toronto, Canada

5. University of Calgary, Calgary, Canada

6. University of Alberta, Edmonton, Canada

7. Alberta Precision Laboratories, Edmonton, Alberta

8. Institut National de Santé Publique du Québec, Québec, Canada

9. National Microbiology Laboratory, Public Health Agency of Canada, Winnipeg, Canada

10. Centre Hospitalier Universitaire de Québec, Québec, Canada

11. Laval University, Quebec, Canada

Abstract

Introduction The Canadian Sentinel Practitioner Surveillance Network reports vaccine effectiveness (VE) for the 2018/19 influenza A(H3N2) epidemic. Aim To explain a paradoxical signal of increased clade 3C.3a risk among 35–54-year-old vaccinees, we hypothesise childhood immunological imprinting and a cohort effect following the 1968 influenza A(H3N2) pandemic. Methods We assessed VE by test-negative design for influenza A(H3N2) overall and for co-circulating clades 3C.2a1b and 3C.3a. VE variation by age in 2018/19 was compared with amino acid variation in the haemagglutinin glycoprotein by year since 1968. Results Influenza A(H3N2) VE was 17% (95% CI: −13 to 39) overall: 27% (95% CI: −7 to 50) for 3C.2a1b and −32% (95% CI: −119 to 21) for 3C.3a. Among 20–64-year-olds, VE was −7% (95% CI: −56 to 26): 6% (95% CI: −49 to 41) for 3C.2a1b and −96% (95% CI: −277 to −2) for 3C.3a. Clade 3C.3a VE showed a pronounced negative dip among 35–54-year-olds in whom the odds of medically attended illness were > 4-fold increased for vaccinated vs unvaccinated participants (p < 0.005). This age group was primed in childhood to influenza A(H3N2) viruses that for two decades following the 1968 pandemic bore a serine at haemagglutinin position 159, in common with contemporary 3C.3a viruses but mismatched to 3C.2a vaccine strains instead bearing tyrosine. Discussion Imprinting by the first childhood influenza infection is known to confer long-lasting immunity focused toward priming epitopes. Our findings suggest vaccine mismatch may negatively interact with imprinted immunity. The immunological mechanisms for imprint-regulated effect of vaccine (I-REV) warrant investigation.

Publisher

European Centre for Disease Control and Prevention (ECDC)

Subject

Virology,Public Health, Environmental and Occupational Health,Epidemiology

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