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Induction of HIV Neutralizing Antibody Lineages in Mice with Diverse Precursor Repertoires
Author(s) -
Ming Tian,
Cheng Cheng,
Xuejun Chen,
Hongying Duan,
Hwei-Ling Cheng,
Mai N. Dao,
Zizhang Sheng,
Michael T. Kimble,
Lingshu Wang,
Sherry Lin,
Stephen D. Schmidt,
Zhou Du,
Michael Joyce,
Yiwei Chen,
Brandon J. DeKosky,
Yimin Chen,
Erica Normandin,
Elizabeth Cantor,
Rita E. Chen,
Nicole A. DoriaRose,
Yi Zhang,
Wei Shi,
WingPui Kong,
Misook Choe,
Amy R. Henry,
Farida Laboune,
Ivelin S. Georgiev,
Pei-Yi Huang,
Suvi Jain,
Andrew T. McGuire,
Eric Georgeson,
Sergey Menis,
Daniel C. Douek,
William R. Schief,
Leonidas Stamatatos,
Peter D. Kwong,
Lawrence Shapiro,
Barton F. Haynes,
John R. Mascola,
Frederick W. Alt
Publication year - 2016
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.2016.07.029
Subject(s) - biology , antibody , antibody repertoire , virology , germline , glycoprotein , hiv vaccine , gp41 , neutralizing antibody , immunology , genetics , epitope , gene , vaccine trial
The design of immunogens that elicit broadly reactive neutralizing antibodies (bnAbs) has been a major obstacle to HIV-1 vaccine development. One approach to assess potential immunogens is to use mice expressing precursors of human bnAbs as vaccination models. The bnAbs of the VRC01-class derive from the IGHV1-2 immunoglobulin heavy chain and neutralize a wide spectrum of HIV-1 strains via targeting the CD4 binding site of the envelope glycoprotein gp120. We now describe a mouse vaccination model that allows a germline human IGHV1-2(∗)02 segment to undergo normal V(D)J recombination and, thereby, leads to the generation of peripheral B cells that express a highly diverse repertoire of VRC01-related receptors. When sequentially immunized with modified gp120 glycoproteins designed to engage VRC01 germline and intermediate antibodies, IGHV1-2(∗)02-rearranging mice, which also express a VRC01-antibody precursor light chain, can support the affinity maturation of VRC01 precursor antibodies into HIV-neutralizing antibody lineages.

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