T Cells Specific for a TAP-independent Self-peptide Remain Naïve in Tumor-bearing Mice and Are Fully Exploitable for Therapy

Overview

Journal Oncoimmunology

Specialty Allergy & Immunology

Date 2018 Feb 6

PMID 29399388

Citations 15

Authors

Elien M Doorduijn

Marjolein Sluijter

Koen A Marijt

Bianca J Querido

Sjoerd H van der Burg

Thorbald van Hall

Affiliations

Soon will be listed here.

Abstract

Cancers frequently evade immune-recognition by lowering peptide:MHC-I complexes on their cell surface. Limited peptide supply due to TAP-deficiency results in such MHC-I immune-escape variants. Previously, we reported on a category of TAP-independent self-peptides, called TEIPP, with selective presentation by these tumors. Here we demonstrate that in contrast to T cells specific for conventional tumor antigens, TEIPP-directed T cells remain naïve in mice bearing immune-escaped tumors. This unaffected state was caused by low levels of MHC-I on the tumors and the failure to cross-present low levels of antigenic protein by host APCs. Importantly, increased levels of MHC-I, antigen or co-stimulation resulted in potent activation of TEIPP-specific T cells via direct presentation. Genetic knockdown by CRISPR/Cas9 technology of the relevant MHC-I allele in tumor cells indeed abrogated T cell activation. Vaccine-mediated priming of TEIPP-specific T cells induced efficient homing to MHC-I tumors and subsequently protected mice against outgrowth of their MHC-I tumor. Thus, our data open up the search of TEIPP-specific T cells in cancer patients to explore their application against MHC-I tumor cells.

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