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Immunopeptidomics reveals determinants of Mycobacterium tuberculosis antigen presentation on MHC class I

Owen Leddy, Forest M. White, Bryan D. Bryson

2023eLife54 citationsDOIOpen Access PDF

Abstract

CD8+ T cell recognition of Mycobacterium tuberculosis ( Mtb )-specific peptides presented on major histocompatibility complex class I (MHC-I) contributes to immunity to tuberculosis (TB), but the principles that govern presentation of Mtb antigens on MHC-I are incompletely understood. In this study, mass spectrometry (MS) analysis of the MHC-I repertoire of Mtb -infected primary human macrophages reveals that substrates of Mtb ’s type VII secretion systems (T7SS) are overrepresented among Mtb -derived peptides presented on MHC-I. Quantitative, targeted MS shows that ESX-1 activity is required for presentation of Mtb peptides derived from both ESX-1 substrates and ESX-5 substrates on MHC-I, consistent with a model in which proteins secreted by multiple T7SSs access a cytosolic antigen processing pathway via ESX-1-mediated phagosome permeabilization. Chemical inhibition of proteasome activity, lysosomal acidification, or cysteine cathepsin activity did not block presentation of Mtb antigens on MHC-I, suggesting involvement of other proteolytic pathways or redundancy among multiple pathways. Our study identifies Mtb antigens presented on MHC-I that could serve as targets for TB vaccines, and reveals how the activity of multiple T7SSs interacts to contribute to presentation of Mtb antigens on MHC-I.

Topics & Concepts

Mycobacterium tuberculosisMHC class IIImmunologyTuberculosisMHC class IAntigen presentationAntigenMajor histocompatibility complexAntigen processingPresentation (obstetrics)CD74BiologyVirologyMedicineImmune systemT cellPathologyRadiologyTuberculosis Research and Epidemiologyvaccines and immunoinformatics approachesMycobacterium research and diagnosis
Immunopeptidomics reveals determinants of Mycobacterium tuberculosis antigen presentation on MHC class I | Litcius