4.6 Article

Identification of HLA-E Binding Mycobacterium tuberculosis-Derived Epitopes through Improved Prediction Models

Journal

JOURNAL OF IMMUNOLOGY
Volume 209, Issue 8, Pages 1555-1565

Publisher

AMER ASSOC IMMUNOLOGISTS
DOI: 10.4049/jimmunol.2200122

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Funding

  1. European Union [707404, 793027]
  2. National Instituteof Allergy and Infectious Diseases of the National Institutes of Health [R21AI127133, R01AI141315]
  3. Nederlandse Organisatie voor Wetenschappelijk Onderzoek Medium Investment (ZonMw) [91116004]
  4. Marie Curie Actions (MSCA) [793027] Funding Source: Marie Curie Actions (MSCA)

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Tuberculosis remains a deadly infectious disease worldwide, causing significant social and economic burden. This study developed an improved algorithm to identify Mycobacterium tuberculosis-derived peptides that can activate specific HLA-E-restricted T cells.
Tuberculosis (TB) remains one of the deadliest infectious diseases worldwide, posing great social and economic burden to affected countries. Novel vaccine approaches are needed to increase protective immunity against the causative agent Mycobacterium tuberculosis (Mtb) and to reduce the development of active TB disease in latently infected individuals. Donor-unrestricted T cell responses represent such novel potential vaccine targets. HLA-E-restricted T cell responses have been shown to play an important role in protection against TB and other infections, and recent studies have demonstrated that these cells can be primed in vitro. However, the identification of novel pathogen-derived HLA-E binding peptides presented by infected target cells has been limited by the lack of accurate prediction algorithms for HLA-E binding. In this study, we developed an improved HLA-E binding peptide prediction algorithm and implemented it to identify (to our knowledge) novel Mtb-derived peptides with capacity to induce CD8+ T cell activation and that were recognized by specific HLA-E-restricted T cells in Mycobacterium-exposed humans. Altogether, we present a novel algorithm for the identification of pathogen-or self-derived HLA-E-presented peptides. The Journal of Immunology, 2022, 209: 1555-1565.

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