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Genetic Variation and Antioxidant Response Gene Expression in the Bronchial Airway Epithelium of Smokers at Risk for Lung Cancer

机译：肺癌风险吸烟者支气管上皮的遗传变异和抗氧化反应基因表达

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Prior microarray studies of smokers at high risk for lung cancer have demonstrated that heterogeneity in bronchial airway epithelial cell gene expression response to smoking can serve as an early diagnostic biomarker for lung cancer. As a first step in applying functional genomic analysis to population studies, we have examined the relationship between gene expression variation and genetic variation in a central molecular pathway (NRF2-mediated antioxidant response) associated with smoking exposure and lung cancer. We assessed global gene expression in histologically normal airway epithelial cells obtained at bronchoscopy from smokers who developed lung cancer (SC, n = 20), smokers without lung cancer (SNC, n = 24), and never smokers (NS, n = 8). Functional enrichment analysis showed that the NRF2-mediated, antioxidant response element (ARE)-regulated genes, were significantly lower in SC, when compared with expression levels in SNC. Importantly, we found that the expression of MAFG (a binding partner of NRF2) was correlated with the expression of ARE genes, suggesting MAFG levels may limit target gene induction. Bioinformatically we identified single nucleotide polymorphisms (SNPs) in putative ARE genes and to test the impact of genetic variation, we genotyped these putative regulatory SNPs and other tag SNPs in selected NRF2 pathway genes. Sequencing MAFG locus, we identified 30 novel SNPs and two were associated with either gene expression or lung cancer status among smokers. This work demonstrates an analysis approach that integrates bioinformatics pathway and transcription factor binding site analysis with genotype, gene expression and disease status to identify SNPs that may be associated with individual differences in gene expression and/or cancer status in smokers. These polymorphisms might ultimately contribute to lung cancer risk via their effect on the airway gene expression response to tobacco-smoke exposure.

机译：先前对高风险肺癌吸烟者进行的微阵列研究表明，吸烟对支气管气道上皮细胞基因表达的异质性可作为肺癌的早期诊断生物标记。作为将功能基因组分析应用于人群研究的第一步，我们研究了与吸烟和肺癌相关的中央分子途径（NRF2介导的抗氧化反应）中基因表达变异与遗传变异之间的关系。我们评估了通过支气管镜检查从患有肺癌（SC，n = 20），无肺癌的吸烟者（SNC，n = 24）和从未吸烟者（NS，n = 8）的支气管镜检查获得的组织学正常的气道上皮细胞中的整体基因表达。功能富集分析表明，与SNC中的表达水平相比，NRF2介导的抗氧化反应元件（ARE）调控的基因在SC中明显较低。重要的是，我们发现MAFG（NRF2的结合伴侣）的表达与ARE基因的表达相关，这表明MAFG的水平可能会限制靶基因的诱导。通过生物信息学，我们在推定的ARE基因中鉴定了单核苷酸多态性（SNP），并测试遗传变异的影响，我们在选定的NRF2途径基因中对这些推定的SNP和其他标签SNP进行了基因分型。对MAFG基因座进行测序，我们确定了30个新的SNP，其中两个与吸烟者的基因表达或肺癌状态有关。这项工作证明了一种分析方法，该方法将生物信息学途径和转录因子结合位点分析与基因型，基因表达和疾病状态相结合，以鉴定可能与吸烟者基因表达和/或癌症状态的个体差异有关的SNP。这些多态性可能通过影响烟气暴露引起的气道基因表达反应而最终导致肺癌风险。

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Wang, Xuting; Chorley, Brian N.; Pittman, Gary S.; Kleeberger, Steven R.; Brothers, John; Liu, Gang; Spira, Avrum; Bell, Douglas A.;
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年度 2010
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正文语种 {"code":"en","name":"English","id":9}
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专利

1. Bronchial airway gene expression in smokers with lung or head and neck cancer [J] . Arnaud Muller, Ceacute, line Mascaux, Cancer Medicine . 2014,第2期

机译：吸烟者患有肺癌或头颈癌的支气管气道基因表达
2. Cis-acting genetic variation at an E2F1/YY1 response site and putative p53 site is associated with altered allele-specific expression of ERCC5 (XPG) transcript in normal human bronchial epithelium. [J] . Blomquist TM, Crawford EL, Willey JC Carcinogenesis . 2010,第7期

机译：E2F1 / YY1反应位点和推定的p53位点的顺式遗传变异与正常人支气管上皮中ERCC5（XPG）转录本的等位基因特异性表达改变有关。
3. Cis-acting genetic variation at an E2F1/YY1 response site and putative p53 site is associated with altered allele-specificn expression of ERCC5 (XPG) transcript in normal human bronchial epithelium [J] . James C. Willey Carcinogenesis . 2010,第7期

机译：E2F1 / YY1反应位点和推定的p53位点的顺式遗传变异与正常人支气管上皮中ERCC5（XPG）转录本的等位基因特异性表达改变有关
4. TRUE-SCALE BIOMIMETIC MULTI-GENERATION AIRWAY PLATFORMS OF THE HUMAN BRONCHIAL EPITHELIUM FOR IN VITRO CYTOTOXICITY SCREENING [C] . Shani Elias-Kirma, Arbel Artzy-Schnirman, Rami Fishier, Nanotechnology in medicine II: briding translational in vitro and in vivo interfaces . 2018

机译：真人生物支气管上皮多代气道平台用于体外细胞毒性检查
5. MicroRNAs as modulators of the airway gene expression response to smoking and lung cancer [D] . Perdomo, Maria Catalina 2012

机译：MicroRNA作为调节剂对吸烟和肺癌的气道基因表达反应
6. Genetic Variation and Antioxidant Response Gene Expression in the Bronchial Airway Epithelium of Smokers at Risk for Lung Cancer [O] . Xuting Wang, Brian N. Chorley, Gary S. Pittman, 2010

机译：肺癌风险吸烟者支气管上皮的遗传变异和抗氧化反应基因表达
7. Genetic variation and antioxidant response gene expression in the bronchial airway epithelium of smokers at risk for lung cancer. [O] . Xuting Wang, Brian N Chorley, Gary S Pittman, 2010

机译：肺癌患者支气管气道上皮细胞遗传变异及抗氧化应答基因表达。
8. Acute Airway Injury and Response: Combined Effect of Smoke and CombustionProducts on Mucin Gene Expression and Regulated Mucin Production in the Tracheal-Bronchial Epithelium (CIC3) [R] . Bhattacharyya, S. 1997

机译：急性气道损伤和反应：烟雾和燃烧产物对气管 - 支气管上皮细胞（CIC3）中粘蛋白基因表达和调节粘蛋白产生的联合作用

Genetic Variation and Antioxidant Response Gene Expression in the Bronchial Airway Epithelium of Smokers at Risk for Lung Cancer

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