Group of Molecular Carcinogenesis, 150 Cours Albert Thomas, 69372 Lyon Cedex 08, France.
Carcinogenesis. 2011 Sep;32(9):1388-95. doi: 10.1093/carcin/bgr090. Epub 2011 May 17.
Genome-wide association studies have linked lung cancer risk with a region of chromosome 15q25.1 containing CHRNA3, CHRNA5 and CHRNB4 encoding α3, α5 and β4 subunits of nicotinic acetylcholine receptors (nAChR), respectively. One of the strongest associations was observed for a non-silent single-nucleotide polymorphism at codon 398 in CHRNA5. Here, we have used pharmacological (antagonists) or genetic (RNA interference) interventions to modulate the activity of CHRNA5 in non-transformed bronchial cells and in lung cancer cell lines. In both cell types, silencing CHRNA5 or inhibiting receptors containing nAChR α5 with α-conotoxin MII exerted a nicotine-like effect, with increased motility and invasiveness in vitro and increasing calcium influx. The effects on motility were enhanced by addition of nicotine but blocked by inhibiting CHRNA7, which encodes the homopentameric receptor α7 subunit. Silencing CHRNA5 also decreased the expression of cell adhesion molecules P120 and ZO-1 in lung cancer cells as well as the expression of DeltaNp63α in squamous cell carcinoma cell lines. These results demonstrate a role for CHRNA5 in modulating adhesion and motility in bronchial cells, as well as in regulating p63, a potential oncogene in squamous cell carcinoma.
全基因组关联研究将肺癌风险与包含 CHRNA3、CHRNA5 和 CHRNB4 的染色体 15q25.1 区域联系起来,分别编码烟碱型乙酰胆碱受体(nAChR)的α3、α5 和β4 亚单位。在 CHRNA5 的密码子 398 处观察到的非沉默单核苷酸多态性与最强的关联之一。在这里,我们使用药理学(拮抗剂)或遗传学(RNA 干扰)干预来调节非转化支气管细胞和肺癌细胞系中 CHRNA5 的活性。在这两种细胞类型中,沉默 CHRNA5 或用α-芋螺毒素 MII 抑制含有 nAChR α5 的受体,都会产生类似于尼古丁的作用,体外迁移性和侵袭性增加,钙内流增加。添加尼古丁可增强对迁移性的影响,但可被抑制 CHRNA7 的作用阻断,后者编码同源五聚体受体α7 亚单位。沉默 CHRNA5 还可降低肺癌细胞中细胞黏附分子 P120 和 ZO-1 的表达以及鳞状细胞癌细胞系中 DeltaNp63α 的表达。这些结果表明 CHRNA5 在调节支气管细胞的黏附和迁移以及调节 p63(鳞状细胞癌中的潜在癌基因)方面发挥作用。
