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Citations to this article

FGFR2 signaling underlies p63 oncogenic function in squamous cell carcinoma
Matthew R. Ramsey, … , Alea A. Mills, Leif W. Ellisen
Matthew R. Ramsey, … , Alea A. Mills, Leif W. Ellisen
Published July 8, 2013
Citation Information: J Clin Invest. 2013;123(8):3525-3538. https://doi.org/10.1172/JCI68899.
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FGFR2 signaling underlies p63 oncogenic function in squamous cell carcinoma

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Abstract

Oncogenic transcription factors drive many human cancers, yet identifying and therapeutically targeting the resulting deregulated pathways has proven difficult. Squamous cell carcinoma (SCC) is a common and lethal human cancer, and relatively little progress has been made in improving outcomes for SCC due to a poor understanding of its underlying molecular pathogenesis. While SCCs typically lack somatic oncogene-activating mutations, they exhibit frequent overexpression of the p53-related transcription factor p63. We developed an in vivo murine tumor model to investigate the function and key transcriptional programs of p63 in SCC. Here, we show that established SCCs are exquisitely dependent on p63, as acute genetic ablation of p63 in advanced, invasive SCC induced rapid and dramatic apoptosis and tumor regression. In vivo genome-wide gene expression analysis identified a tumor-survival program involving p63-regulated FGFR2 signaling that was activated by ligand emanating from abundant tumor-associated stroma. Correspondingly, we demonstrate the therapeutic efficacy of extinguishing this signaling axis in endogenous SCCs using the clinical FGFR2 inhibitor AZD4547. Collectively, these results reveal an unanticipated role for p63-driven paracrine FGFR2 signaling as an addicting pathway in human cancer and suggest a new approach for the treatment of SCC.

Authors

Matthew R. Ramsey, Catherine Wilson, Benjamin Ory, S. Michael Rothenberg, William Faquin, Alea A. Mills, Leif W. Ellisen

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Year: 2025 2024 2023 2022 2021 2020 2019 2018 2017 2016 2015 2014 Total
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Citations to this article (69)

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2024
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Context dependent activity of p63-bound gene regulatory elements.
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Distinct interactors define the p63 transcriptional signature in epithelial development or cancer.
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Biochemical Journal 2022
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eLife 2020
Maintaining protein stability of ∆Np63 via USP 28 is required by squamous cancer cells
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EMBO Molecular Medicine 2020
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M Yi, Y Tan, L Wang, J Cai, X Li, Z Zeng, W Xiong, G Li, X Li, P Tan, B Xiang
Cellular and Molecular Life Sciences 2020
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International journal of molecular sciences 2019
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