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Completeness of HIV-1 Envelope Glycan Shield at Transmission Determines Neutralization Breadth
Author(s) -
Kshitij Wagh,
Edward F. Kreider,
Yingying Li,
Hannah J. Barbian,
Gerald H. Learn,
Elena E. Giorgi,
Peter Hraber,
Timothy Decker,
Andrew G. Smith,
Marcos V. P. Gondim,
Lindsey Gillis,
Jamie M. Wandzilak,
GwoYu Chuang,
Reda Rawi,
Fangping Cai,
Pierre Pellegrino,
Ian Williams,
Julie Overbaugh,
Feng Gao,
Peter D. Kwong,
Barton F. Haynes,
George M. Shaw,
Persephone Borrow,
Michael S. Seaman,
Beatrice H. Hahn,
Bette Korber
Publication year - 2018
Publication title -
cell reports
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 6.264
H-Index - 154
eISSN - 2639-1856
pISSN - 2211-1247
DOI - 10.1016/j.celrep.2018.09.087
Subject(s) - neutralization , glycan , virology , antibody , neutralizing antibody , biology , glycoprotein , immunology , virus , genetics
Densely arranged N-linked glycans shield the HIV-1 envelope (Env) trimer from antibody recognition. Strain-specific breaches in this shield (glycan holes) can be targets of vaccine-induced neutralizing antibodies that lack breadth. To understand the interplay between glycan holes and neutralization breadth in HIV-1 infection, we developed a sequence- and structure-based approach to identify glycan holes for individual Env sequences that are shielded in most M-group viruses. Applying this approach to 12 longitudinally followed individuals, we found that transmitted viruses with more intact glycan shields correlated with development of greater neutralization breadth. Within 2 years, glycan acquisition filled most glycan holes present at transmission, indicating escape from hole-targeting neutralizing antibodies. Glycan hole filling generally preceded the time to first detectable breadth, although time intervals varied across hosts. Thus, completely glycan-shielded viruses were associated with accelerated neutralization breadth development, suggesting that Env immunogens with intact glycan shields may be preferred components of AIDS vaccines.

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