Induction of HIV neutralizing antibody lineages in mice with diverse precursor repertoires

M Tian, C Cheng, X Chen, H Duan, HL Cheng, M Dao… - Cell, 2016 - cell.com
M Tian, C Cheng, X Chen, H Duan, HL Cheng, M Dao, Z Sheng, M Kimble, L Wang, S Lin
Cell, 2016cell.com
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 …
Summary
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 IGHV1-202 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, IGHV1-202-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.
cell.com
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