Lam David Chi-Leung, Girard Luc, Ramirez Ruben, Chau Wing-Shun, Suen Wai-sing, Sheridan Shelley, Tin Vicky P C, Chung Lap-ping, Wong Maria P, Shay Jerry W, Gazdar Adi F, Lam Wah-kit, Minna John D
Department of Medicine, University of Hong Kong, HKSAR, China.
Cancer Res. 2007 May 15;67(10):4638-47. doi: 10.1158/0008-5472.CAN-06-4628.
Nicotine and its derivatives, by binding to nicotinic acetylcholine receptors (nAChR) on bronchial epithelial cells, can regulate cellular proliferation and apoptosis via activating the Akt pathway. Delineation of nAChR subtypes in non-small-cell lung cancers (NSCLC) may provide information for prevention or therapeutic targeting. Expression of nAChR subunit genes in 66 resected primary NSCLCs, 7 histologically non-involved lung tissues, 13 NSCLC cell lines, and 6 human bronchial epithelial cell lines (HBEC) was analyzed with quantitative PCR and microarray analysis. Five nonmalignant HBECs were exposed to nicotine in vitro to study the variation of nAChR subunit gene expression with nicotine exposure and removal. NSCLCs from nonsmokers showed higher expression of nAChR alpha6 (P < 0.001) and beta3 (P = 0.007) subunit genes than those from smokers, adjusted for gender. In addition, nAChR alpha4 (P < 0.001) and beta4 (P = 0.029) subunit gene expression showed significant difference between NSCLCs and normal lung. Using Affymetrix GeneChip U133 Sets, 65 differentially expressed genes associated with NSCLC nonsmoking nAChR alpha6beta3 phenotype were identified, which gave high sensitivity and specificity of prediction. nAChR alpha1, alpha5, and alpha7 showed significant reversible changes in expression levels in HBECs upon nicotine exposure. We conclude that between NSCLCs from smokers and nonsmokers, different nAChR subunit gene expression patterns were found, and a 65-gene expression signature was associated with nonsmoking nAChR alpha6beta3 expression. Finally, nicotine exposure in HBECs resulted in reversible differences in nAChR subunit gene expression. These results further implicate nicotine in bronchial carcinogenesis and suggest targeting nAChRs for prevention and therapy in lung cancer.
尼古丁及其衍生物通过与支气管上皮细胞上的烟碱型乙酰胆碱受体(nAChR)结合,可通过激活Akt途径调节细胞增殖和凋亡。明确非小细胞肺癌(NSCLC)中nAChR亚型可能为预防或治疗靶点提供信息。采用定量PCR和微阵列分析技术,分析了66例手术切除的原发性NSCLC、7例组织学上未受累的肺组织、13株NSCLC细胞系和6株人支气管上皮细胞系(HBEC)中nAChR亚基基因的表达情况。将5例非恶性HBECs体外暴露于尼古丁,研究尼古丁暴露和去除后nAChR亚基基因表达的变化。校正性别后,非吸烟者的NSCLC中nAChRα6(P<0.001)和β3(P = 0.007)亚基基因表达高于吸烟者。此外,NSCLC与正常肺组织之间nAChRα4(P<0.001)和β4(P = 0.029)亚基基因表达存在显著差异。使用Affymetrix GeneChip U133芯片组,鉴定出65个与NSCLC非吸烟nAChRα6β3表型相关的差异表达基因,其预测具有高敏感性和特异性。尼古丁暴露后,HBECs中nAChRα1、α5和α7的表达水平呈现显著的可逆变化。我们得出结论,吸烟者和非吸烟者的NSCLC之间存在不同的nAChR亚基基因表达模式,65个基因的表达特征与非吸烟nAChRα6β3表达相关。最后,HBECs中的尼古丁暴露导致nAChR亚基基因表达出现可逆差异。这些结果进一步表明尼古丁与支气管癌发生有关,并提示将nAChRs作为肺癌预防和治疗的靶点。
