TY - JOUR
T1 - Broad hemagglutinin-specific memory B cell expansion by seasonal influenza virus infection reflects early-life imprinting and adaptation to the infecting virus
AU - Tesini, Brenda L.
AU - Kanagaiah, Preshetha
AU - Wang, Jiong
AU - Hahn, Megan
AU - Halliley, Jessica L.
AU - Chaves, Francisco A.
AU - Nguyen, Phuong Q.T.
AU - Nogales, Aitor
AU - DeDiego, Marta L.
AU - Anderson, Christopher S.
AU - Ellebedy, Ali H.
AU - Strohmeier, Shirin
AU - Krammer, Florian
AU - Yang, Hongmei
AU - Bandyopadhyay, Sanjukta
AU - Ahmed, Rafi
AU - Treanor, John J.
AU - Martinez-Sobrido, Luis
AU - Golding, Hana
AU - Khurana, Surender
AU - Zand, Martin S.
AU - Topham, David J.
AU - Sangster, Mark Y.
N1 - Funding Information:
We thank the staff of the University of Rochester Vaccine Research Center for subject enrollment and sample collection and BEI Resources and IRR for providing some of the viruses used in this study. This study was supported with Federal funds from the National Institute of Allergy and Infectious Diseases, National Institutes of Health, Department of Health and Human Services, through awards to the New York Influenza Center of Excellence (NYICE; contract HHSN272201400005C), a member of the NIAID Centers of Excellence for Influenza Research and Surveillance (CEIRS), and to the Respiratory Pathogens Research Center (RPRC; contract HHSN272201200005C). Additional funding was provided through the CRIP (Center for Research on Influenza Pathogenesis) CEIRS center (HHSN272201400008C), U19 AI109946, and R01 AI128821.
Funding Information:
This study was supported with Federal funds from the National Institute of Allergy and Infectious Diseases, National Institutes of Health, Department of Health and Human Services, through awards to the New York Influenza Center of Excellence (NYICE; contract HHSN272201400005C), a member of the NIAID Centers of Excellence for Influenza Research and Surveillance (CEIRS), and to the Respiratory Pathogens Research Center (RPRC; contract HHSN272201200005C). Additional funding was provided through the CRIP (Center for Research on Influenza Pathogenesis) CEIRS center (HHSN272201400008C), U19 AI109946, and R01 AI128821.
Publisher Copyright:
© 2019 American Society for Microbiology. All Rights Reserved.
PY - 2019
Y1 - 2019
N2 - Memory B cells (MBCs) are key determinants of the B cell response to influenza virus infection and vaccination, but the effect of different forms of influenza antigen exposure on MBC populations has received little attention. We analyzed peripheral blood mononuclear cells and plasma collected following human H3N2 influenza infection to investigate the relationship between hemagglutinin-specific antibody production and changes in the size and character of hemagglutinin-reactive MBC populations. Infection produced increased concentrations of plasma IgG reactive to the H3 head of the infecting virus, to the conserved stalk, and to a broad chronological range of H3s consistent with original antigenic sin responses. H3-reactive IgG MBC expansion after infection included reactivity to head and stalk domains. Notably, expansion of H3 head-reactive MBC populations was particularly broad and reflected original antigenic sin patterns of IgG production. Findings also suggest that early-life H3N2 infection “imprints” for strong H3 stalk-specific MBC expansion. Despite the breadth of MBC expansion, the MBC response included an increase in affinity for the H3 head of the infecting virus. Overall, our findings indicate that H3-reactive MBC expansion following H3N2 infection is consistent with maintenance of response patterns established early in life, but nevertheless includes MBC adaptation to the infecting virus. IMPORTANCE Rapid and vigorous virus-specific antibody responses to influenza virus infection and vaccination result from activation of preexisting virus-specific memory B cells (MBCs). Understanding the effects of different forms of influenza virus exposure on MBC populations is therefore an important guide to the development of effective immunization strategies. We demonstrate that exposure to the influenza hemagglutinin via natural infection enhances broad protection through expansion of hemagglutinin-reactive MBC populations that recognize head and stalk regions of the molecule. Notably, we show that hemagglutinin-reactive MBC expansion reflects imprinting by early-life infection and that this might apply to stalk-reactive, as well as to head-reactive, MBCs. Our findings provide experimental support for the role of MBCs in maintaining imprinting effects and suggest a mechanism by which imprinting might confer heterosubtypic protection against avian influenza viruses. It will be important to compare our findings to the situation after influenza vaccination.
AB - Memory B cells (MBCs) are key determinants of the B cell response to influenza virus infection and vaccination, but the effect of different forms of influenza antigen exposure on MBC populations has received little attention. We analyzed peripheral blood mononuclear cells and plasma collected following human H3N2 influenza infection to investigate the relationship between hemagglutinin-specific antibody production and changes in the size and character of hemagglutinin-reactive MBC populations. Infection produced increased concentrations of plasma IgG reactive to the H3 head of the infecting virus, to the conserved stalk, and to a broad chronological range of H3s consistent with original antigenic sin responses. H3-reactive IgG MBC expansion after infection included reactivity to head and stalk domains. Notably, expansion of H3 head-reactive MBC populations was particularly broad and reflected original antigenic sin patterns of IgG production. Findings also suggest that early-life H3N2 infection “imprints” for strong H3 stalk-specific MBC expansion. Despite the breadth of MBC expansion, the MBC response included an increase in affinity for the H3 head of the infecting virus. Overall, our findings indicate that H3-reactive MBC expansion following H3N2 infection is consistent with maintenance of response patterns established early in life, but nevertheless includes MBC adaptation to the infecting virus. IMPORTANCE Rapid and vigorous virus-specific antibody responses to influenza virus infection and vaccination result from activation of preexisting virus-specific memory B cells (MBCs). Understanding the effects of different forms of influenza virus exposure on MBC populations is therefore an important guide to the development of effective immunization strategies. We demonstrate that exposure to the influenza hemagglutinin via natural infection enhances broad protection through expansion of hemagglutinin-reactive MBC populations that recognize head and stalk regions of the molecule. Notably, we show that hemagglutinin-reactive MBC expansion reflects imprinting by early-life infection and that this might apply to stalk-reactive, as well as to head-reactive, MBCs. Our findings provide experimental support for the role of MBCs in maintaining imprinting effects and suggest a mechanism by which imprinting might confer heterosubtypic protection against avian influenza viruses. It will be important to compare our findings to the situation after influenza vaccination.
KW - Hemagglutinin
KW - Imprinting
KW - Influenza virus
KW - Memory B cells
KW - Original antigenic sin
UR - http://www.scopus.com/inward/record.url?scp=85064239750&partnerID=8YFLogxK
U2 - 10.1128/JVI.00169-19
DO - 10.1128/JVI.00169-19
M3 - Article
C2 - 30728266
AN - SCOPUS:85064239750
SN - 0022-538X
VL - 93
JO - Journal of Virology
JF - Journal of Virology
IS - 8
M1 - Y
ER -