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.

译文

背景:乳腺癌(BCa)和前列腺癌(PCa)是激素受体(HR)驱动的癌症。因此,为BCa和PCa患者提供降低激素水平或直接阻断HR活动的疗法;但是大多数患者最终都会产生治疗抵抗力。我们以前曾报道过白介素1(IL-1)炎性细胞因子下调HR阳性(HR)BCa和PCa细胞系中的ERα和AR mRNA,但这些细胞仍可以保持活力。另外,我们在HR Bca和PCa细胞中基本较高的HR BCa和PCa细胞中鉴定了促存活蛋白和IL-1上调的过程。因此,我们假设IL-1赋予HR BCa和PCa细胞保守的基因表达模式,该模式模仿HR-BCa和PCa细胞中保守的基础基因表达模式,从而促进HR非依赖性生存和致瘤性。
方法:我们对暴露于IL-1的HR BCa和PCa细胞系以及未经处理的HR- BCa和PCa细胞系进行了RNA测序(RNA-seq)。我们通过RT-qPCR证实了选择基因的表达模式,并使用siRNA和/或药物抑制使BCa和PCa细胞系中的选择基因沉默。最后,我们进行了创新途径分析(IPA),并使用了基于基因本体网络的工具GOrilla来识别由RNA-seq数据集编码的信号传导途径。
结果:我们确定了BCa和PCa细胞之间共有350个基因,这些基因分别由HR细胞中基本高或低的HR细胞中的IL-1诱导或抑制。在这些基因中,我们确定了Sequestome-1(SQSTM1 / p62)和SRY(性决定区Y)-Box 9(SOX9)对HR-BCa和PCa细胞系的存活至关重要。公开数据的分析表明,在体外产生的HR非依赖性BCa和PCa亚系中p62和SOX9表达升高,表明p62和SOX9在获得性激素受体独立性和治疗耐药性中起作用。我们还评估了针对p62靶向药物verteporfin的HR细胞系活力,并发现verteporfin对HR细胞系具有细胞毒性。
结论:我们的350个基因集可用于鉴定在获得性(例如由于炎症)或内源性HR无关的BCa和PCa中保守的新治疗靶标和/或生物标志物。

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