Oncotarget

Research Papers:

Addiction of lung cancer cells to GOF p53 is promoted by up-regulation of epidermal growth factor receptor through multiple contacts with p53 transactivation domain and promoter

Catherine A. Vaughan, Isabella Pearsall, Shilpa Singh, Brad Windle, Swati P. Deb, Steven R. Grossman, W. Andrew Yeudall and Sumitra Deb _

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Oncotarget. 2016; 7:12426-12446. https://doi.org/10.18632/oncotarget.6998

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Abstract

Catherine A. Vaughan1, Isabella Pearsall2, Shilpa Singh3, Brad Windle1,2,4, Swati P. Deb1,2,3, Steven R. Grossman2,5, W. Andrew Yeudall1,2,4,6 and Sumitra Deb1,2,3

1 Department of Biochemistry and Molecular Biology, Virginia Commonwealth University, Richmond, VA, USA

2 Massey Cancer Center, Virginia Commonwealth University, Richmond, VA, USA

3 Integrated Life Sciences Program, Virginia Commonwealth University, Richmond, VA, USA

4 Philips Institute, Virginia Commonwealth University, Richmond, VA, USA

5 Division of Hematology, Oncology and Palliative Care, Virginia Commonwealth University, Richmond, VA, USA

6 Department of Oral Biology, Augusta University, Augusta, GA, USA

Correspondence to:

Sumitra Deb, email:

Keywords: addiction, mutant, p53, transcription, EGFR

Received: January 05, 2016 Accepted: January 16, 2016 Published: January 25, 2016

Abstract

Human lung cancers harboring gain-of-function (GOF) p53 alleles express higher levels of the epidermal growth factor receptor (EGFR). We demonstrate that a number of GOF p53 alleles directly upregulate EGFR. Knock-down of p53 in lung cancer cells lowers EGFR expression and reduces tumorigenicity and other GOF p53 properties. However, addiction of lung cancer cells to GOF p53 can be compensated by overexpressing EGFR, suggesting that EGFR plays a critical role in addiction. Chromatin immunoprecipitation (ChIP) using lung cancer cells expressing GOF p53 alleles showed that GOF p53 localized to the EGFR promoter. The sequence where GOF p53 is found to interact by ChIP seq can act as a GOF p53 response element. The presence of GOF p53 on the EGFR promoter increased histone H3 acetylation, indicating a mechanism whereby GOF p53 enhances chromatin opening for improved access to transcription factors (TFs). ChIP and ChIP-re-ChIP with p53, Sp1 and CBP histone acetylase (HAT) antibodies revealed docking of GOF p53 on Sp1, leading to increased binding of Sp1 and CBP to the EGFR promoter. Up-regulation of EGFR can occur via GOF p53 contact at other novel sites in the EGFR promoter even when TAD-I is inactivated; these sites are used by both intact and TAD-I mutated GOF p53 and might reflect redundancy in GOF p53 mechanisms for EGFR transactivation. Thus, the oncogenic action of GOF p53 in lung cancer is highly dependent on transactivation of the EGFR promoter via a novel transcriptional mechanism involving coordinated interactions of TFs, HATs and GOF p53.


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