Contemporary HIV-1 consensus Env with AI-assisted redesigned hypervariable loops promote antibody binding
Nature Communications, ISSN: 2041-1723, Vol: 15, Issue: 1, Page: 3924
2024
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- 13Captures
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Study Findings on HIV/AIDS Are Outlined in Reports from U.S. Military HIV Research Program (Contemporary HIV-1 consensus Env with AI-assisted redesigned hypervariable loops promote antibody binding)
2024 MAY 29 (NewsRx) -- By a News Reporter-Staff News Editor at Vaccine Daily -- Research findings on HIV/AIDS are discussed in a new report.
Article Description
An effective HIV-1 vaccine must elicit broadly neutralizing antibodies (bnAbs) against highly diverse Envelope glycoproteins (Env). Since Env with the longest hypervariable (HV) loops is more resistant to the cognate bnAbs than Env with shorter HV loops, we redesigned hypervariable loops for updated Env consensus sequences of subtypes B and C and CRF01_AE. Using modeling with AlphaFold2, we reduced the length of V1, V2, and V5 HV loops while maintaining the integrity of the Env structure and glycan shield, and modified the V4 HV loop. Spacers are designed to limit strain-specific targeting. All updated Env are infectious as pseudoviruses. Preliminary structural characterization suggests that the modified HV loops have a limited impact on Env’s conformation. Binding assays show improved binding to modified subtype B and CRF01_AE Env but not to subtype C Env. Neutralization assays show increases in sensitivity to bnAbs, although not always consistently across clades. Strikingly, the HV loop modification renders the resistant CRF01_AE Env sensitive to 10-1074 despite the absence of a glycan at N332.
Bibliographic Details
Springer Science and Business Media LLC
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