Convergent Structures Illuminate Features for Germline Antibody Binding and Pan-Lassa Virus Neutralization
Author(s) -
Kathryn M. Hastie,
Robert W. Cross,
Stephanie Harkins,
Michelle Zandonatti,
Anatoliy Koval,
Megan L. Heinrich,
Megan M. Rowland,
James E. Robinson,
Thomas W. Geisbert,
Robert F. Garry,
Luis M. Branco,
Erica Ollmann Saphire
Publication year - 2019
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2019.07.020
Subject(s) - neutralization , biology , lassa virus , antibody , virology , epitope , arenavirus , neutralizing antibody , potency , antigenicity , glycoprotein , virus , microbiology and biotechnology , immune system , immunology , biochemistry , in vitro , lymphocytic choriomeningitis , cd8
Lassa virus (LASV) causes hemorrhagic fever and is endemic in West Africa. Protective antibody responses primarily target the LASV surface glycoprotein (GPC), and GPC-B competition group antibodies often show potent neutralizing activity in humans. However, which features confer potent and broadly neutralizing antibody responses is unclear. Here, we compared three crystal structures of LASV GPC complexed with GPC-B antibodies of varying neutralization potency. Each GPC-B antibody recognized an overlapping epitope involved in binding of two adjacent GPC monomers and preserved the prefusion trimeric conformation. Differences among GPC-antibody interactions highlighted specific residues that enhance neutralization. Using structure-guided amino acid substitutions, we increased the neutralization potency and breadth of these antibodies to include all major LASV lineages. The ability to define antibody residues that allow potent and broad neutralizing activity, together with findings from analyses of inferred germline precursors, is critical to develop potent therapeutics and for vaccine design and assessment.
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