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7 results on '"Vartuli, Rebecca L."'

1. Eya3 promotes breast tumor-associated immune suppression via threonine phosphatase-mediated PD-L1 upregulation

Author

Vartuli, Rebecca L., Zhou, Hengbo, Zhang, Lingdi, Powers, Rani K., Klarquist, Jared, Rudra, Pratyaydipta, Vincent, Melanie Y., Ghosh, Debashis, Costello, James C., Kedl, Ross M., Slansky, Jill E., Zhao, Rui, and Ford, Heide L.

Subjects
Immune response regulation -- Health aspects, Breast tumors -- Development and progression -- Genetic aspects, Membrane proteins -- Physiological aspects -- Health aspects, Transcriptional coactivators -- Physiological aspects -- Health aspects, Health care industry
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.sup.+] 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.sup.+] 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., Introduction The eyes absent family of proteins (Eyas 1-4) are crucial regulators of embryogenesis, contributing to the development of diverse tissues such as the ear (1, 2), eye (3), craniofacial [...]

Published
2018
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6. Eya3 partners with PP2A to induce c-Myc stabilization and tumor progression.

Author

Lingdi Zhang, Hengbo Zhou, Xueni Li, Vartuli, Rebecca L., Rowse, Michael, Yongna Xing, Rudra, Pratyaydipta, Ghosh, Debashis, Rui Zhao, and Ford, Heide L.

Subjects
CANCER invasiveness, PHOSPHOPROTEIN phosphatases, PHOSPHATASES, PROTEIN-protein interactions, BREAST cancer
Abstract

Eya genes encode a unique family of multifunctional proteins that serve as transcriptional coactivators and as haloacid dehalogenase-family Tyr phosphatases. Intriguingly, the Nterminal domain of Eyas, which does not share sequence similarity to any known phosphatases, contains a separable Ser/Thr phosphatase activity. Here, we demonstrate that the Ser/ Thr phosphatase activity of Eya is not intrinsic, but arises from its direct interaction with the protein phosphatase 2A (PP2A)-B55α holoenzyme. Importantly, Eya3 alters the regulation of c-Myc by PP2A, increasing c-Myc stability by enabling PP2A-B55α to dephosphorylate pT58, in direct contrast to the previously described PP2A-B56α-mediated dephosphorylation of pS62 and c-Myc destabilization. Furthermore, Eya3 and PP2A-B55α promote metastasis in a xenograft model of breast cancer, opposing the canonical tumor suppressive function of PP2A-B56α. Our study identifies Eya3 as a regulator of PP2A, a major cellular Ser/Thr phosphatase, and uncovers a mechanism of controlling the stability of a critical oncogene, c-Myc. [ABSTRACT FROM AUTHOR]

Published
2018
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