| Literature DB >> 29757193 |
Rebecca L Vartuli1,2, Hengbo Zhou1,3, Lingdi Zhang4, Rani K Powers1,5, Jared Klarquist6, Pratyaydipta Rudra7, Melanie Y Vincent1, Debashis Ghosh7, James C Costello1,3,5, Ross M Kedl6, Jill E Slansky3,6, Rui Zhao2,4, Heide L Ford1,2,3,4.
Abstract
Eya proteins are critical developmental regulators that are highly expressed in embryogenesis but downregulated after development. Amplification and/or re-expression of Eyas occurs in many tumor types. In breast cancer, Eyas regulate tumor progression by acting as transcriptional cofactors and tyrosine phosphatases. Intriguingly, Eyas harbor a separate threonine (Thr) phosphatase activity, which was previously implicated in innate immunity. Here we describe what we believe to be a novel role for Eya3 in mediating triple-negative breast cancer-associated immune suppression. Eya3 loss decreases tumor growth in immune-competent mice and is associated with increased numbers of infiltrated CD8+ T cells, which, when depleted, reverse the effects of Eya3 knockdown. Mechanistically, Eya3 utilizes its Thr phosphatase activity to dephosphorylate Myc at pT58, resulting in a stabilized form. We show that Myc is required for Eya3-mediated increases in PD-L1, and that rescue of PD-L1 in Eya3-knockdown cells restores tumor progression. Finally, we demonstrate that Eya3 significantly correlates with PD-L1 in human breast tumors, and that tumors expressing high levels of Eya3 have a decreased CD8+ T cell signature. Our data uncover a role for Eya3 in mediating tumor-associated immune suppression, and suggest that its inhibition may enhance checkpoint therapies.Entities:
Keywords: Breast cancer; Immunology; Oncology; T cells
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Year: 2018 PMID: 29757193 PMCID: PMC5983346 DOI: 10.1172/JCI96784
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808