Structure and function of broadly reactive antibody PG16 reveal an H3 subdomain that mediates potent neutralization of HIV-1

Pejchal, Robert; Walker, Laura M; Stanfield, Robyn L; Phogat, Sanjay K; Koff, Wayne C; Poignard, Pascal; Burton, Dennis R; Wilson, Ian A

doi:10.1073/pnas.1004600107

Title: Structure and function of broadly reactive antibody PG16 reveal an H3 subdomain that mediates potent neutralization of HIV-1

Journal Article · Mon Nov 15 00:00:00 EST 2010 · Proc. Natl. Acad. Sci. USA

DOI:https://doi.org/10.1073/pnas.1004600107· OSTI ID:1002842

Pejchal, Robert; Walker, Laura M; Stanfield, Robyn L; Phogat, Sanjay K; Koff, Wayne C; Poignard, Pascal; Burton, Dennis R; Wilson, Ian A ^[1]

Scripps

Development of an effective vaccine against HIV-1 will likely require elicitation of broad and potent neutralizing antibodies against the trimeric surface envelope glycoprotein (Env). Monoclonal antibodies (mAbs) PG9 and PG16 neutralize {approx}80% of HIV-1 isolates across all clades with extraordinary potency and target novel epitopes preferentially expressed on Env trimers. As these neutralization properties are ideal for a vaccine-elicited antibody response to HIV-1, their structural basis was investigated. The crystal structure of the antigen-binding fragment (Fab) of PG16 at 2.5 {angstrom} resolution revealed its unusually long, 28-residue, complementarity determining region (CDR) H3 forms a unique, stable subdomain that towers above the antibody surface. A 7-residue 'specificity loop' on the 'hammerhead' subdomain was identified that, when transplanted from PG16 to PG9 and vice versa, accounted for differences in the fine specificity and neutralization of these two mAbs. The PG16 electron density maps also revealed that a CDR H3 tyrosine was sulfated, which was confirmed for both PG9 (doubly) and PG16 (singly) by mass spectral analysis. We further showed that tyrosine sulfation plays a role in binding and neutralization. An N-linked glycan modification is observed in the variable light chain, but not required for antigen recognition. Further, the crystal structure of the PG9 light chain at 3.0 {angstrom} facilitated homology modeling to support the presence of these unusual features in PG9. Thus, PG9 and PG16 use unique structural features to mediate potent neutralization of HIV-1 that may be of utility in antibody engineering and for high-affinity recognition of a variety of therapeutic targets.

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Research Organization:: Argonne National Lab. (ANL), Argonne, IL (United States). Advanced Photon Source (APS)

Sponsoring Organization:: USDOE

OSTI ID:: 1002842

Journal Information:: Proc. Natl. Acad. Sci. USA, Vol. 107, Issue (25) ; 06, 2010; ISSN 0027-8424

Country of Publication:: United States

Language:: ENGLISH

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36 MATERIALS SCIENCE
ANTIBODIES
ANTIGENS
CHAINS
CRYSTAL STRUCTURE
ELECTRON DENSITY
GLYCOPROTEINS
MODIFICATIONS
MONOCLONAL ANTIBODIES
RESOLUTION
SIMULATION
SPECIFICITY
SULFATION
TARGETS
TYROSINE
VACCINES

Title: Structure and function of broadly reactive antibody PG16 reveal an H3 subdomain that mediates potent neutralization of HIV-1

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