Koper Andre, Zeef Leo A H, Joseph Leena, Kerr Keith, Gosney John, Lindsay Mark A, Booton Richard
Qiagen GmbH, Hilden, 40724, Germany.
Faculty of Life Science, University of Manchester, Manchester, England, M13 9PT, UK.
Respir Res. 2017 Jan 10;18(1):12. doi: 10.1186/s12931-016-0496-3.
Preinvasive squamous cell cancer (PSCC) are local transformations of bronchial epithelia that are frequently observed in current or former smokers. Their different grades and sizes suggest a continuum of dysplastic change with increasing severity, which may culminate in invasive squamous cell carcinoma (ISCC). As a consequence of the difficulty in isolating cancerous cells from biopsies, the molecular pathology that underlies their histological variability remains largely unknown.
To address this issue, we have employed microdissection to isolate normal bronchial epithelia and cancerous cells from low- and high-grade PSCC and ISCC, from paraffin embedded (FFPE) biopsies and determined gene expression using Affymetric Human Exon 1.0 ST arrays. Tests for differential gene expression were performed using the Bioconductor package limma followed by functional analyses of differentially expressed genes in IPA.
Examination of differential gene expression showed small differences between low- and high-grade PSCC but substantial changes between PSCC and ISCC samples (184 vs 1200 p-value <0.05, fc ±1.75). However, the majority of the differentially expressed PSCC genes (142 genes: 77%) were shared with those in ISCC samples. Pathway analysis showed that these shared genes are associated with DNA damage response, DNA/RNA metabolism and inflammation as major biological themes. Cluster analysis identified 12 distinct patterns of gene expression including progressive up or down-regulation across PSCC and ISCC. Pathway analysis of incrementally up-regulated genes revealed again significant enrichment of terms related to DNA damage response, DNA/RNA metabolism, inflammation, survival and proliferation. Altered expression of selected genes was confirmed using RT-PCR, as well as immunohistochemistry in an independent set of 45 ISCCs.
Gene expression profiles in PSCC and ISCC differ greatly in terms of numbers of genes with altered transcriptional activity. However, altered gene expression in PSCC affects canonical pathways and cellular and biological processes, such as inflammation and DNA damage response, which are highly consistent with hallmarks of cancer.
侵袭前鳞状细胞癌(PSCC)是支气管上皮的局部转变,在当前或既往吸烟者中经常观察到。它们不同的分级和大小表明随着发育异常变化程度的增加存在一个连续过程,这可能最终发展为侵袭性鳞状细胞癌(ISCC)。由于从活检组织中分离癌细胞存在困难,其组织学变异性背后的分子病理学在很大程度上仍不为人知。
为解决这个问题,我们采用显微切割技术从石蜡包埋(FFPE)活检组织中的低级别和高级别PSCC以及ISCC中分离正常支气管上皮和癌细胞,并使用Affymetric Human Exon 1.0 ST芯片确定基因表达。使用Bioconductor软件包limma进行差异基因表达测试,随后在IPA中对差异表达基因进行功能分析。
差异基因表达检查显示低级别和高级别PSCC之间差异较小,但PSCC和ISCC样本之间有显著变化(184对1200,p值<0.05,fc±1.75)。然而,大多数差异表达的PSCC基因(142个基因:77%)与ISCC样本中的基因相同。通路分析表明,这些共享基因主要与DNA损伤反应、DNA/RNA代谢和炎症等生物学主题相关。聚类分析确定了12种不同的基因表达模式,包括PSCC和ISCC中逐渐上调或下调的模式。对逐渐上调基因的通路分析再次显示与DNA损伤反应、DNA/RNA代谢、炎症、存活和增殖相关的术语有显著富集。使用RT-PCR以及在45个独立的ISCC样本中进行免疫组织化学证实了所选基因的表达改变。
PSCC和ISCC中的基因表达谱在转录活性改变的基因数量方面有很大差异。然而,PSCC中基因表达的改变影响了典型通路以及细胞和生物学过程,如炎症和DNA损伤反应,这与癌症的特征高度一致。
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