IL-1-conferred gene expression pattern in ERα+ BCa and AR+ PCa cells is intrinsic to ERα− BCa and AR− PCa cells and promotes cell survival

Afshan F. Nawas; Mohammed Kanchwala; Shayna Thomas-Jardin; Haley Dahl; Kelly Daescu; Monica Bautista; Vanessa Anunobi; Ally Wong; Rachel K. Meade; Ragini M. Mistry; Nisha Ghatwai; Felix Bayerl; Chao Xing; Nikkí A. Delk

doi:10.1186/s12885-020-6529-9

IL-1-conferred gene expression pattern in ERα+ BCa and AR+ PCa cells is intrinsic to ERα− BCa and AR− PCa cells and promotes cell survival

Afshan F. Nawas(The University of Texas at Dallas), Mohammed Kanchwala(The University of Texas Southwestern Medical Center), Shayna Thomas-Jardin(The University of Texas at Dallas), Haley Dahl(The University of Texas at Dallas), Kelly Daescu(The University of Texas at Dallas), Monica Bautista(The University of Texas at Dallas), Vanessa Anunobi(The University of Texas at Dallas), Ally Wong(The University of Texas at Dallas), Rachel K. Meade(The University of Texas at Dallas), Ragini M. Mistry(The University of Texas at Dallas), Nisha Ghatwai(The University of Texas at Dallas), Felix Bayerl(The University of Texas at Dallas), Chao Xing(The University of Texas Southwestern Medical Center), Nikkí A. Delk(The University of Texas at Dallas)

BMC Cancer

January 20, 2020

10.1186/s12885-020-6529-9

Cited by 17Open Access

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Abstract

Abstract Background Breast (BCa) and prostate (PCa) cancers are hormone receptor (HR)-driven cancers. Thus, BCa and PCa patients are given therapies that reduce hormone levels or directly block HR activity; but most patients eventually develop treatment resistance. We have previously reported that interleukin-1 (IL-1) inflammatory cytokine downregulates ERα and AR mRNA in HR-positive (HR + ) BCa and PCa cell lines, yet the cells can remain viable. Additionally, we identified pro-survival proteins and processes upregulated by IL-1 in HR + BCa and PCa cells, that are basally high in HR − BCa and PCa cells. Therefore, we hypothesize that IL-1 confers a conserved gene expression pattern in HR + BCa and PCa cells that mimics conserved basal gene expression patterns in HR − BCa and PCa cells to promote HR-independent survival and tumorigenicity. Methods We performed RNA sequencing (RNA-seq) for HR + BCa and PCa cell lines exposed to IL-1 and for untreated HR − BCa and PCa cell lines. We confirmed expression patterns of select genes by RT-qPCR and used siRNA and/or drug inhibition to silence select genes in the BCa and PCa cell lines. Finally, we performed Ingenuity Pathway Analysis (IPA) and used the gene ontology web-based tool, GOrilla, to identify signaling pathways encoded by our RNA-seq data set. Results We identified 350 genes in common between BCa and PCa cells that are induced or repressed by IL-1 in HR + cells that are, respectively, basally high or low in HR − cells. Among these genes, we identified Sequestome-1 ( SQSTM1/p62 ) and SRY ( Sex-Determining Region Y ) -Box 9 ( SOX9 ) to be essential for survival of HR − BCa and PCa cell lines. Analysis of publicly available data indicates that p62 and SOX9 expression are elevated in HR-independent BCa and PCa sublines generated in vitro, suggesting that p62 and SOX9 have a role in acquired hormone receptor independence and treatment resistance. We also assessed HR − cell line viability in response to the p62-targeting drug, verteporfin, and found that verteporfin is cytotoxic for HR − cell lines. Conclusions Our 350 gene set can be used to identify novel therapeutic targets and/or biomarkers conserved among acquired (e.g. due to inflammation) or intrinsic HR-independent BCa and PCa.

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