Department of Health Sciences, University of Genoa, Italy.
Cancer Prev Res (Phila). 2010 Jan;3(1):62-72. doi: 10.1158/1940-6207.CAPR-09-0202.
We previously showed that exposure to environmental cigarette smoke (ECS) for 28 days causes extensive downregulation of microRNA expression in the lungs of rats, resulting in the overexpression of multiple genes and proteins. In the present study, we evaluated by microarray the expression of 484 microRNAs in the lungs of either ECS-free or ECS-exposed rats treated with the orally administered chemopreventive agents N-acetylcysteine, oltipraz, indole-3-carbinol, 5,6-benzoflavone, and phenethyl isothiocyanate (as single agents or in combinations). This is the first study of microRNA modulation by chemopreventive agents in nonmalignant tissues. Scatterplot, hierarchical cluster, and principal component analyses of microarray and quantitative PCR data showed that none of the above chemopreventive regimens appreciably affected the baseline microRNA expression, indicating potential safety. On the other hand, all of them attenuated ECS-induced alterations but to a variable extent and with different patterns, indicating potential preventive efficacy. The main ECS-altered functions that were modulated by chemopreventive agents included cell proliferation, apoptosis, differentiation, Ras activation, P53 functions, NF-kappaB pathway, transforming growth factor-related stress response, and angiogenesis. Some microRNAs known to be polymorphic in humans were downregulated by ECS and were protected by chemopreventive agents. This study provides proof-of-concept and validation of technology that we are further refining to screen and prioritize potential agents for continued development and to help elucidate their biological effects and mechanisms. Therefore, microRNA analysis may provide a new tool for predicting at early carcinogenesis stages both the potential safety and efficacy of cancer chemopreventive agents.
我们之前的研究表明,暴露于环境香烟烟雾(ECS)中 28 天会导致大鼠肺部的 microRNA 表达广泛下调,导致多个基因和蛋白质的过表达。在本研究中,我们通过微阵列评估了暴露于 ECS 或未暴露于 ECS 的大鼠肺部中 484 种 microRNA 的表达,这些大鼠接受了口服化学预防剂 N-乙酰半胱氨酸、奥替普拉、吲哚-3-甲醇、5,6-苯并黄酮和苯乙基异硫氰酸酯(单独或联合使用)的治疗。这是首次研究化学预防剂对非恶性组织中 microRNA 调节的研究。微阵列和定量 PCR 数据的散点图、层次聚类和主成分分析表明,上述化学预防方案均未明显影响 microRNA 的基线表达,表明潜在的安全性。另一方面,它们都减弱了 ECS 诱导的改变,但程度和模式不同,表明潜在的预防效果。化学预防剂调节的主要 ECS 改变功能包括细胞增殖、凋亡、分化、Ras 激活、P53 功能、NF-κB 途径、转化生长因子相关应激反应和血管生成。一些在人类中已知具有多态性的 microRNAs 被 ECS 下调,并被化学预防剂保护。这项研究提供了概念验证和技术验证,我们正在进一步完善这项技术,以筛选和优先考虑潜在的候选药物进行进一步开发,并帮助阐明它们的生物学效应和机制。因此,microRNA 分析可能为预测癌症化学预防剂的潜在安全性和疗效提供一种新的工具,特别是在早期癌发生阶段。