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A cell-free antigen processing system informs HIV-1 epitope selection and vaccine design
- Sengupta, Srona;
- Zhang, Josephine;
- Reed, Madison C;
- Yu, Jeanna;
- Kim, Aeryon;
- Boronina, Tatiana N;
- Board, Nathan L;
- Wrabl, James O;
- Shenderov, Kevin;
- Welsh, Robin A;
- Yang, Weiming;
- Timmons, Andrew E;
- Hoh, Rebecca;
- Cole, Robert N;
- Deeks, Steven G;
- Siliciano, Janet D;
- Siliciano, Robert F;
- Sadegh-Nasseri, Scheherazade
- et al.
Published Web Location
https://doi.org/10.1084/jem.20221654Abstract
Distinct CD4+ T cell epitopes have been associated with spontaneous control of HIV-1 replication, but analysis of antigen-dependent factors that influence epitope selection is lacking. To examine these factors, we used a cell-free antigen processing system that incorporates soluble HLA-DR (DR1), HLA-DM (DM), cathepsins, and full-length protein antigens for epitope identification by LC-MS/MS. HIV-1 Gag, Pol, Env, Vif, Tat, Rev, and Nef were examined using this system. We identified 35 novel epitopes, including glycopeptides. Epitopes from smaller HIV-1 proteins mapped to regions of low protein stability and higher solvent accessibility. HIV-1 antigens associated with limited CD4+ T cell responses were processed efficiently, while some protective epitopes were inefficiently processed. 55% of epitopes obtained from cell-free processing induced memory CD4+ T cell responses in HIV-1+ donors, including eight of 19 novel epitopes tested. Thus, an in vitro processing system utilizing the components of Class II processing reveals factors influencing epitope selection of HIV-1 and represents an approach to understanding epitope selection from non-HIV-1 antigens.
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