Influenza A Reinfection in Sequential Human Challenge: Implications for Protective Immunity and “Universal” Vaccine Development

Author:

Memoli Matthew J1,Han Alison1,Walters Kathie-Anne2,Czajkowski Lindsay1,Reed Susan1,Athota Rani1,Angela Rosas Luz1,Cervantes-Medina Adriana1,Park Jae-Keun3,Morens David M4,Kash John C3,Taubenberger Jeffery K3

Affiliation:

1. Clinical Studies Unit, Laboratory of Infectious Diseases, Division of Intramural Research, National Institute of Allergy and Infectious Diseases (NIAID), National Institutes of Health (NIH), Bethesda, Maryland

2. Institute for Systems Biology, Seattle, Washington

3. Viral Pathogenesis and Evolution Section, Laboratory of Infectious Diseases, Division of Intramural Research, Bethesda, Maryland

4. Office of the Director, NIAID, NIH, Bethesda, Maryland

Abstract

Abstract Background Identification of correlates of protection against human influenza A virus infection is important in development of broadly protective (“universal”) influenza vaccines. Certain assumptions underlie current vaccine developmental strategies, including that infection with a particular influenza A virus should offer long-term or lifelong protection against that strain, preventing reinfection. In this study we report observations made when 7 volunteers participated in sequential influenza challenge studies where they were challenged intranasally using the identical influenza A(H1N1)pdm09 virus approximately 1 year apart. We evaluate and describe the outcomes of these 7 rechallenge participants and discuss what these results may suggest about correlates of protection and development of more broadly protective influenza vaccines. Methods Seven participants were enrolled in 2 viral challenge studies at 7.5- to 18.5-month intervals. Both challenge studies used the identical lot of influenza A (H1N1)pdm09 virus administered intranasally. We evaluated pre- and postchallenge hemagglutination inhibition, neuraminidase inhibition, and stalk antibody titers; peripheral blood leukocyte host gene expression response profiles; daily viral detection via nasal wash; and clinical signs and symptoms. Results At least 3 of 7 participants demonstrated confirmed laboratory evidence of sequential infection, with 5 of 7 demonstrating clinical evidence. Conclusions The data presented in this report demonstrate that sequential infection with the identical influenza A virus can occur and suggest it may not be rare. These data raise questions about immune memory responses in an acute superficial respiratory mucosal infection and their implications in development of broadly protective influenza vaccines. Further investigation of these observations is warranted. Clinical Trials Registration NCT01646138; NCT01971255.

Funder

National Institutes of Health

National Institute of Allergy and Infectious Diseases

Biomedical Advanced Research and Development Authority

Publisher

Oxford University Press (OUP)

Subject

Infectious Diseases,Microbiology (medical)

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