Vaccine-Induced Antibodies that Neutralize Group 1 and Group 2 Influenza A Viruses
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Date
2016-07-28Author
Joyce, M. GordonWheatley, Adam K.
Thomas, Paul V.
Chuang, Gwo-Yu
Soto, Cinque
Bailer, Robert T.
Druz, Aliaksandr
Georgiev, Ivelin S.
Gillespie, Rebecca A.
Kanekiyo, Masaru
Kong, Wing-Pui
Leung, Kwanyee
Narpala, Sandeep N.
Prabhakaran, Madhu S.
Yang, Eun Sung
Zhang, Baoshan
Zhang, Yi
Asokan, Mangaiarkarasi
Boyington, Jeffrey C.
Bylund, Tatsiana
Darko, Sam
Lees, Christopher R.
Ransier, Amy
Shen, Chen-Hsiang
Wang, Lingshu
Whittle, James R.
Wu, Xueling
Yassine, Hadi M.
Santos, Celia
Matsuoka, Yumiko
Tsybovsky, Yaroslav
Baxa, Ulrich
Mullikin, James C.
Subbarao, Kanta
Douek, Daniel C.
Graham, Barney S.
Koup, Richard A.
Ledgerwood, Julie E.
Roederer, Mario
Shapiro, Lawrence
Kwong, Peter D.
Mascola, John R.
McDermott, Adrian B.
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Show full item recordAbstract
Antibodies capable of neutralizing divergent influenza A viruses could form the basis of a universal vaccine. Here, from subjects enrolled in an H5N1 DNA/MIV-prime-boost influenza vaccine trial, we sorted hemagglutinin cross-reactive memory B cells and identified three antibody classes, each capable of neutralizing diverse subtypes of group 1 and group 2 influenza A viruses. Co-crystal structures with hemagglutinin revealed that each class utilized characteristic germline genes and convergent sequence motifs to recognize overlapping epitopes in the hemagglutinin stem. All six analyzed subjects had sequences from at least one multidonor class, and—in half the subjects—multidonor-class sequences were recovered from >40% of cross-reactive B cells. By contrast, these multidonor-class sequences were rare in published antibody datasets. Vaccination with a divergent hemagglutinin can thus increase the frequency of B cells encoding broad influenza A-neutralizing antibodies. We propose the sequence signature-quantified prevalence of these B cells as a metric to guide universal influenza A immunization strategies.
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