Abstract:
:Structure-guided approaches to HIV-1 vaccine design depend on knowledge of the presentation of neutralizing epitopes on gp120, such as the epitope for the broadly neutralizing mAb b12. Here, we characterized predicted three-dimensional structures of functionally diverse gp120 proteins in their b12-bound conformation, to better understand the gp120 determinants that expose or occlude the b12 epitope. Mapping the gp120-b12 binding interface identified amino acid polymorphisms within the C2, C3, C4 and V5 regions of gp120 associated with augmented b12 binding, and importantly, identified residues in the b12-exclusive binding domain of gp120 that are important for b12 neutralization resistance. Structural studies suggest that these b12 resistance variants promote reduced conformational flexibility in the b12 recognition site, which we show involves structural alterations within the gp120 CD4 binding loop and the V4 loop. Together, our studies provide new mechanistic insights into the gp120 determinants influencing sensitivity and resistance to HIV-1 neutralization by b12.
journal_name
Virologyjournal_title
Virologyauthors
Sterjovski J,Churchill MJ,Ellett A,Wesselingh SL,Ramsland PA,Gorry PRdoi
10.1016/j.virol.2012.06.024subject
Has Abstractpub_date
2012-10-25 00:00:00pages
394-404issue
2eissn
0042-6822issn
1096-0341pii
S0042-6822(12)00326-1journal_volume
432pub_type
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