| Literature DB >> 28931755 |
Pearl Bakhru1, Meng-Lei Zhu1, Hsing-Hui Wang1, Lee K Hong1, Imran Khan2, Maria Mouchess2, Ajay S Gulati1,3,4, Joshua Starmer5, Yafei Hou6, David Sailer1, Sandra Lee7,8, Fengmin Zhao1, John M Kirkwood8,9, Stergios Moschos8,10,11, Lawrence Fong6, Mark S Anderson2, Maureen A Su1,11.
Abstract
Blockade of immune checkpoint proteins (e.g., CTLA-4, PD-1) improves overall survival in advanced melanoma; however, therapeutic benefit is limited to only a subset of patients. Because checkpoint blockade acts by "removing the brakes" on effector T cells, the efficacy of checkpoint blockade may be constrained by the limited pool of melanoma-reactive T cells in the periphery. In the thymus, autoimmune regulator (Aire) promotes deletion of T cells reactive against self-antigens that are also expressed by tumors. Thus, while protecting against autoimmunity, Aire also limits the generation of melanoma-reactive T cells. Here, we show that Aire deficiency in mice expands the pool of CD4+ T cells capable of melanoma cell eradication and has additive effects with anti-CTLA-4 antibody in slowing melanoma tumor growth and increasing survival. Moreover, pharmacologic blockade of central T cell tolerance and peripheral checkpoint blockade in combination enhanced antimelanoma immunity in a synergistic manner. In melanoma patients treated with anti-CTLA-4 antibody, clinical response to therapy was associated with a human Aire polymorphism. Together, these findings suggest that Aire-mediated central tolerance constrains the efficacy of peripheral checkpoint inhibition and point to simultaneous blockade of Aire and checkpoint inhibitors as a novel strategy to enhance antimelanoma immunity.Entities:
Keywords: Cancer immunotherapy; Cellular immune response; Immunology; Melanoma
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Year: 2017 PMID: 28931755 PMCID: PMC5621898 DOI: 10.1172/jci.insight.93265
Source DB: PubMed Journal: JCI Insight ISSN: 2379-3708