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Robust Iterative Stimulation with Self-Antigens Overcomes CD8+ T Cell Tolerance to Self- and Tumor Antigens.


ABSTRACT: The immune system adapts to constitutive antigens to preserve self-tolerance, which is a major barrier for anti-tumor immunity. Antigen-specific reversal of tolerance constitutes a major goal to spur therapeutic applications. Here, we show that robust, iterative, systemic stimulation targeting tissue-specific antigens in the context of acute infections reverses established CD8+ T cell tolerance to self, including in T cells that survive negative selection. This strategy results in large numbers of circulating and resident memory self-specific CD8+ T cells that are widely distributed and can be co-opted to control established malignancies bearing self-antigen without concomitant autoimmunity. Targeted expansion of both self- and tumor neoantigen-specific T cells acts synergistically to boost anti-tumor immunity and elicits protection against aggressive melanoma. Our findings demonstrate that T cell tolerance can be re-adapted to responsiveness through robust antigenic exposure, generating self-specific CD8+ T cells that can be used for cancer treatment.

SUBMITTER: Nelson CE 

PROVIDER: S-EPMC6874401 | biostudies-literature | 2019 Sep

REPOSITORIES: biostudies-literature

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Robust Iterative Stimulation with Self-Antigens Overcomes CD8<sup>+</sup> T Cell Tolerance to Self- and Tumor Antigens.

Nelson Christine E CE   Thompson Emily A EA   Quarnstrom Clare F CF   Fraser Kathryn A KA   Seelig Davis M DM   Bhela Siddheshvar S   Burbach Brandon J BJ   Masopust David D   Vezys Vaiva V  

Cell reports 20190901 12


The immune system adapts to constitutive antigens to preserve self-tolerance, which is a major barrier for anti-tumor immunity. Antigen-specific reversal of tolerance constitutes a major goal to spur therapeutic applications. Here, we show that robust, iterative, systemic stimulation targeting tissue-specific antigens in the context of acute infections reverses established CD8<sup>+</sup> T cell tolerance to self, including in T cells that survive negative selection. This strategy results in lar  ...[more]

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