Epigenomic study identifies a novel mesenchyme homeobox2-GLI1 transcription axis involved in cancer drug resistance, overall survival and therapy prognosis in lung cancer patients

Leonel Armas-López; Patricia Piña-Sánchez; Oscar Arrieta; Enrique Guzman de Alba; Blanca Ortiz-Quintero; Patricio Santillán-Doherty; David C Christiani; Joaquín Zúñiga; Federico Ávila-Moreno

doi:10.18632/oncotarget.17715

Epigenomic study identifies a novel mesenchyme homeobox2-GLI1 transcription axis involved in cancer drug resistance, overall survival and therapy prognosis in lung cancer patients

Oncotarget. 2017 May 9;8(40):67056-67081. doi: 10.18632/oncotarget.17715. eCollection 2017 Sep 15.

Authors

Leonel Armas-López¹, Patricia Piña-Sánchez², Oscar Arrieta³, Enrique Guzman de Alba⁴, Blanca Ortiz-Quintero⁴, Patricio Santillán-Doherty⁴, David C Christiani⁵, Joaquín Zúñiga⁴, Federico Ávila-Moreno^{1

4}

Affiliations

¹ National University Autonomous of México (UNAM), Facultad de Estudios Superiores (FES) Iztacala, Biomedicine Research Unit (UBIMED), Lung Diseases And Cancer Epigenomics Laboratory, Mexico State, Mexico.
² Instituto Mexicano del Seguro Social (IMSS), Centro Medico Nacional (CMN) Siglo XXI, Unidad de Investigación Médica en Enfermedades Oncológicas (UIMEO), Molecular Oncology Laboratory, Mexico City, Mexico.
³ National Cancer Institute (INCAN), Thoracic Oncology Clinic, Mexico City, Mexico.
⁴ National Institute of Respiratory Diseases (INER) "Ismael Cosío Villegas", Mexico City, Mexico.
⁵ Harvard Medical School, Harvard School of Public Health, Department of Environmental Health, Boston, Massachusetts, USA.

Abstract

Several homeobox-related gene (HOX) transcription factors such as mesenchyme HOX-2 (MEOX2) have previously been associated with cancer drug resistance, malignant progression and/or clinical prognostic responses in lung cancer patients; however, the mechanisms involved in these responses have yet to be elucidated. Here, an epigenomic strategy was implemented to identify novel MEOX2 gene promoter transcription targets and propose a new molecular mechanism underlying lung cancer drug resistance and poor clinical prognosis. Chromatin immunoprecipitation (ChIP) assays derived from non-small cell lung carcinomas (NSCLC) hybridized on gene promoter tiling arrays and bioinformatics analyses were performed, and quantitative, functional and clinical validation were also carried out. We statistically identified a common profile consisting of 78 gene promoter targets, including Hedgehog-GLI1 gene promoter sequences (FDR≤0.1 and FDR≤0.2). The GLI-1 gene promoter region from -2,192 to -109 was occupied by MEOX2, accompanied by transcriptionally active RNA Pol II and was epigenetically linked to the active histones H3K27Ac and H3K4me3; these associations were quantitatively validated. Moreover, siRNA genetic silencing assays identified a MEOX2-GLI1 axis involved in cellular cytotoxic resistance to cisplatinum in a dose-dependent manner, as well as cellular migration and proliferation. Finally, Kaplan-Maier survival analyses identified significant MEOX2-dependent GLI-1 protein expression associated with clinical progression and poorer overall survival using an independent cohort of NSCLC patients undergoing platinum-based oncological therapy with both epidermal growth factor receptor (EGFR)-non-mutated and EGFR-mutated status. In conclusion, this is the first study to investigate epigenome-wide MEOX2-transcription factor occupation identifying a novel overexpressed MEOX2-GLI1 axis and its clinical association with platinum-based cancer drug resistance and EGFR-tyrosine kinase inhibitor (TKI)-based therapy responses in NSCLC patients.

Keywords: epigenetics cancer drug resistance; homeobox transcription factors; lung cancer; overall survival; treatment prognosis.

Grants and funding

R35 CA197449/CA/NCI NIH HHS/United States