A Publication of the Center for Undergraduate Research and Scholarship at Barton College


Volume 1, No. 1
Online ISSN: 3071-0898

Copyright

© The authors. This article is published under the terms of the Creative Commons 4.0 License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.

Bayesian Integrative Approach Identifies Hidden Intermediates in DH270-Induced Structural Transitions of HIV-1 Envelope

CONFERENCE ABSTRACT

Alaina Vrable* and Ashley L. Bennett⁺

School of Health Sciences, Barton College, Wilson, NC, USA
*Student author, ⁺Faculty mentor


CITATION

Vrable, Alaina; & Bennett, Ashley L. (2026). Bayesian integrative approach identifies hidden intermediates in DH270-induced structural transitions of HIV-1 envelope [Conference abstract]. Barton Journal, 1(1), 156–157. https://bartonjournal.org/vol-1-no-1/2026-cat4-article-no-016


Abstract

HIV-1 Envelope glycoprotein (Env) undergoes a sequence of structural transitions, from a closed conformation to an open structure, initiates host-cell infection, and alters exposure of antibody epitopes. Closed-to-open transition proceeds through both short-lived disordered and more stable open-occluded intermediates, exposing distinct antibody binding surfaces. Designing effective HIV-1 vaccines requires a deeper understanding of how Env opening changes antibody engagement. DH270 is a broadly neutralizing antibody with neutralization capacity against a range of HIV-1 strains, and stabilizes closed Env structure. Env structural changes on microsecond timescales, induced by DH270 binding, were first captured at high temporal resolution using time-resolved, temperature-jump small-angle X-ray scattering (TR, T-Jump SAXS). Interpretation of these low-resolution data are challenging due to substantial conformational heterogeneity involved in binding processes. To enable high-confidence structural interpretation of TR, T-Jump SAXS signals, a novel integrative approach combining Markov state models, homology modeling, and a Bayesian inference framework to fit theoretical structures to experimental data was developed. Structural models for each known Env conformation, closed, disordered, open-occluded, and open, each in one of several possible DH270-bound states were generated. This yielded 9,600 unique DH270-bound Env models. Comparison of theoretical SAXS profiles from these models, along with experimental data indicates open-occluded intermediate and partially DH270-bound closed Env states contribute substantially to DH270-induced Env motions. Inclusion of these partially bound encounter complexes significantly improves model fits. Disordered intermediate and fully open Env conformations appear to play no role in DH270-induced structural response, consistent with prior evidence that DH270 stabilizes closed Env conformation. Improvements to the fit remain needed and suggests additional, as-yet-unidentified Env conformational states may be required to fully capture experimental TR, T-Jump SAXS signals. These results can be leveraged to engineer antibody affinity and neutralization potency in potential vaccine immunogen candidates. Newly characterized structural transitions provide a foundation for future structure-guided HIV-1 vaccine design.

Keywords: HIV-1, SAXS, time-resolved, structural biology, modeling, protein dynamics, immunogen design, vaccine, broadly neutralizing antibodies

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