TY - JOUR
T1 - Infant Antibody Repertoires during the First Two Years of Influenza Vaccination
AU - Kuraoka, Masayuki
AU - Curtis, Nicholas C.
AU - Watanabe, Akiko
AU - Tanno, Hidetaka
AU - Shin, Seungmin
AU - Ye, Kevin
AU - Macdonald, Elizabeth
AU - Lavidor, Olivia
AU - Kong, Susan
AU - Holle, Tarra Von
AU - Windsor, Ian
AU - Ippolito, Gregory C.
AU - Georgiou, George
AU - Walter, Emmanuel B.
AU - Kelsoe, Garnett
AU - Harrison, Stephen C.
AU - Anthony Moody, M.
AU - Bajic, Goran
AU - Lee, Jiwon
N1 - Funding Information:
The research was supported by NIAID grant number P01 AI089618. We also acknowledge support from NIH grant number P20 GM113132 (to J.L.), NSF graduate research fellowship grant number 1840344 (to N.C.C.), and NIAID CIVIC contract number 75N93019C00051 (to G.B., G.G., and G.C.I.). SCH is an Investigator in the Howard Hughes Medical Institute.
Publisher Copyright:
© 2022 American Society for Microbiology. All rights reserved.
PY - 2022/12
Y1 - 2022/12
N2 - The first encounter with influenza virus biases later immune responses. This “immune imprinting,” formerly from infection within a few years of birth, is in the United States now largely from immunization with a quadrivalent, split vaccine (IIV4 [quadrivalent inactivated influenza vaccine]). In a pilot study of IIV4 imprinting, we used single-cell cultures, next-generation sequencing, and plasma antibody proteomics to characterize the primary antibody responses to influenza in two infants during their first 2 years of seasonal influenza vaccination. One infant, who received only a single vaccination in year 1, contracted an influenza B virus (IBV) infection between the 2 years, allowing us to compare imprinting by infection and vaccination. That infant had a shift in hemagglutinin (HA)-reactive B cell specificity from largely influenza A virus (IAV) specific in year 1 to IBV specific in year 2, both before and after the year 2 vaccination. HA-reactive B cells from the other infant maintained a more evenly distributed specificity. In year 2, class-switched HA-specific B cell IGHV somatic hypermutation (SHM) levels reached the average levels seen in adults. The HA-reactive plasma antibody repertoires of both infants comprised a relatively small number of antibody clonotypes, with one or two very abundant clonotypes. Thus, after the year 2 boost, both infants had overall B cell profiles that resembled those of adult controls. IMPORTANCE Influenza virus is a moving target for the immune system. Variants emerge that escape protection from antibodies elicited by a previously circulating variant (“antigenic drift”). The immune system usually responds to a drifted influenza virus by mutating existing antibodies rather than by producing entirely new ones. Thus, immune memory of the earliest influenza virus exposure has a major influence on later responses to infection or vaccination (“immune imprinting”). In the many studies of influenza immunity in adult subjects, imprinting has been from an early infection, since only in the past 2 decades have infants received influenza immunizations. The work reported in this paper is a pilot study of imprinting by the flu vaccine in two infants, who received the vaccine before experiencing an influenza virus infection. The results suggest that a quadrivalent (four-subtype) vaccine may provide an immune imprint less dominated by one subtype than does a monovalent infection.
AB - The first encounter with influenza virus biases later immune responses. This “immune imprinting,” formerly from infection within a few years of birth, is in the United States now largely from immunization with a quadrivalent, split vaccine (IIV4 [quadrivalent inactivated influenza vaccine]). In a pilot study of IIV4 imprinting, we used single-cell cultures, next-generation sequencing, and plasma antibody proteomics to characterize the primary antibody responses to influenza in two infants during their first 2 years of seasonal influenza vaccination. One infant, who received only a single vaccination in year 1, contracted an influenza B virus (IBV) infection between the 2 years, allowing us to compare imprinting by infection and vaccination. That infant had a shift in hemagglutinin (HA)-reactive B cell specificity from largely influenza A virus (IAV) specific in year 1 to IBV specific in year 2, both before and after the year 2 vaccination. HA-reactive B cells from the other infant maintained a more evenly distributed specificity. In year 2, class-switched HA-specific B cell IGHV somatic hypermutation (SHM) levels reached the average levels seen in adults. The HA-reactive plasma antibody repertoires of both infants comprised a relatively small number of antibody clonotypes, with one or two very abundant clonotypes. Thus, after the year 2 boost, both infants had overall B cell profiles that resembled those of adult controls. IMPORTANCE Influenza virus is a moving target for the immune system. Variants emerge that escape protection from antibodies elicited by a previously circulating variant (“antigenic drift”). The immune system usually responds to a drifted influenza virus by mutating existing antibodies rather than by producing entirely new ones. Thus, immune memory of the earliest influenza virus exposure has a major influence on later responses to infection or vaccination (“immune imprinting”). In the many studies of influenza immunity in adult subjects, imprinting has been from an early infection, since only in the past 2 decades have infants received influenza immunizations. The work reported in this paper is a pilot study of imprinting by the flu vaccine in two infants, who received the vaccine before experiencing an influenza virus infection. The results suggest that a quadrivalent (four-subtype) vaccine may provide an immune imprint less dominated by one subtype than does a monovalent infection.
KW - B cell memory
KW - circulating antibodies
KW - immune imprinting
KW - influenza virus
KW - viral immunity
UR - http://www.scopus.com/inward/record.url?scp=85144346082&partnerID=8YFLogxK
U2 - 10.1128/mbio.02546-22
DO - 10.1128/mbio.02546-22
M3 - Article
C2 - 36314798
AN - SCOPUS:85144346082
SN - 2161-2129
VL - 13
JO - mBio
JF - mBio
IS - 6
ER -