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No patient left behind: The promise of immune priming with epigenetic agents.


ABSTRACT: Checkpoint inhibitors, monoclonal antibodies that inhibit PD-1 or CTLA-4, have revolutionized the treatment of multiple cancers. Despite the enthusiasm for the clinical successes of checkpoint inhibitors, and immunotherapy, in general, only a minority of patients with specific tumor types actually benefit from treatment. Emerging evidence implicates epigenetic alterations as a mechanism of clinical resistance to immunotherapy. This review presents evidence for that association, summarizes the epi-based mechanisms by which tumors evade immunogenic cell death, discusses epigenetic modulation as a component of an integrated strategy to boost anticancer T cell effector function in relation to a tumor immunosuppression cycle and, finally, makes the case that the success of this no-patient-left-behind strategy critically depends on the toxicity profile of the epigenetic agent(s).

SUBMITTER: Carter CA 

PROVIDER: S-EPMC5665084 | biostudies-literature | 2017

REPOSITORIES: biostudies-literature

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No patient left behind: The promise of immune priming with epigenetic agents.

Carter Corey A CA   Oronsky Bryan T BT   Roswarski Joseph J   Oronsky Arnold L AL   Oronsky Neil N   Scicinski Jan J   Lybeck Harry H   Kim Michelle M MM   Lybeck Michelle M   Reid Tony R TR  

Oncoimmunology 20170830 10


Checkpoint inhibitors, monoclonal antibodies that inhibit PD-1 or CTLA-4, have revolutionized the treatment of multiple cancers. Despite the enthusiasm for the clinical successes of checkpoint inhibitors, and immunotherapy, in general, only a minority of patients with specific tumor types actually benefit from treatment. Emerging evidence implicates epigenetic alterations as a mechanism of clinical resistance to immunotherapy. This review presents evidence for that association, summarizes the ep  ...[more]

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