Protective HLA Alleles Recruit Biased and Largely Similar Antigen-Specific T Cell Repertoires across Different Outcomes in HIV Infection

Publication date

2022-01-01

Authors

Koning, Dan
Quakkelaar, Esther D
Schellens, Ingrid M M
Spierings, EricORCID 0000-0001-9441-1019ISNI 0000000391074963
van Baarle, D.ISNI 000000038873051X

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Document Type

Article

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taverne

Abstract

CD8+ T cells play an important role in the control of untreated HIV infection. Several studies have suggested a decisive role of TCRs involved in anti-HIV immunity. HLA-B*27 and B*57 are often associated with a delayed HIV disease progression, but the exact correlates that provide superior immunity against HIV are not known. To investigate if the T cell repertoire underlies the protective effect in disease outcome in HLA-B*27 and B*57+ individuals, we analyzed Ag-specific TCR profiles from progressors (n = 13) and slow progressors (n = 11) expressing either B*27 or B*57. Our data showed no differences in TCR diversity between progressors and slow progressors. Both alleles recruit biased T cell repertoires (i.e., TCR populations skewed toward specific TRBV families or CDR3 regions). This bias was unrelated to disease progression and was remarkably profound for HLA-B*57, in which TRBV family usage and CDR3 sequences were shared to some extent even between epitopes. Conclusively, these data suggest that the T cell repertoires recruited by protective HLA alleles are highly similar between progressors and slow progressors in terms of TCR diversity, TCR usage, and cross-reactivity.

Keywords

Taverne, Immunology and Allergy, Immunology, Journal Article

Citation

Koning, D, Quakkelaar, E D, Schellens, I M M, Spierings, E & van Baarle, D 2022, 'Protective HLA Alleles Recruit Biased and Largely Similar Antigen-Specific T Cell Repertoires across Different Outcomes in HIV Infection', Journal of Immunology, vol. 208, no. 1, pp. 3-15. https://doi.org/10.4049/jimmunol.2001145