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Molecular epidemiologic studies within the Selenium and Vitamin E Cancer Prevention Trial (SELECT).

机译:硒和维生素E癌症预防试验(SELECT)中的分子流行病学研究。

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OBJECTIVE: To conduct timely epidemiologic investigations of molecular/genetic markers that may contribute to the development of prostate, lung, colorectal, or other cancers within the Selenium and Vitamin E Cancer Prevention Trial (SELECT), and to evaluate interactions between these markers and the study interventions. METHODS: The epidemiologic studies within SELECT will be based on 32,400 men aged 55 years or older (age 50 or older for the African-American men) enrolled into an intergroup, randomized, placebo-controlled, double-blind, phase III prevention trial of supplemental selenium and vitamin E developed and funded by the National Cancer Institute, and coordinated by the Southwest Oncology Group. During the 12-year study period approximately 1500-2000 cases of prostate cancer, 800 lung cancers, and 500 colon cancers are estimated to be diagnosed, based on data from the ongoing Prostate Cancer Prevention Trial of finasteride. A modified fasting blood sample will be processed to collect plasma for analysis of micronutrients, hormones, cytokines, and other proteins. Buffy-coat derived white blood cells collected at baseline will be used for isolation of DNA and establishment of immortalized cell lines. Red blood cells will be stored for analysis of hemoglobin adducts and other components. RESULTS: Specific results anticipated from these molecular studies will provide information on factors hypothesized to contribute to prostate cancer risk and that may modify the efficacy of either trial supplement, including: steroid sex hormones and several polymorphic genes that encode proteins affecting androgenic stimulation of the prostate, including the androgen receptor, steroid 5alpha-reductase type II, CYP17, and beta-hydroxysteroid dehydrogenase; polymorphisms of DNA repair genes and carcinogen metabolism genes, including those involved in the activation of chemical carcinogens to reactive intermediates (e.g., CYP1A1) or the detoxification of reactive intermediates (e.g., glutathione S-transferase M1); DNA and protein adducts; and insulin-like growth factors and leptin. CONCLUSION: SELECT offers an excellent opportunity to conduct molecular epidemiologic investigations to assess gene-environment interactions and their role in prostate, lung, and colon carcinogenesis.
机译:目的:对硒和维生素E癌症预防试验(SELECT)中可能有助于前列腺癌,肺癌,结肠直肠癌或其他癌症发展的分子/遗传标记物进行及时的流行病学调查,并评估这些标记物与肝癌之间的相互作用。研究干预措施。方法:SELECT研究中的流行病学研究将基于32400名55岁或以上男性(非裔美国人年龄在50岁或以上)的研究,该研究纳入了一项小组间,安慰剂对照,双盲,III期预防试验。由国家癌症研究所开发和资助,并由西南肿瘤学小组协调的补充硒和维生素E。在12年的研究期内,根据正在进行的非那雄胺前列腺癌预防试验的数据,估计可诊断出约1500-2000例前列腺癌,800例肺癌和500例结肠癌。修改后的空腹血样将被处理以收集血浆,以分析微量营养素,激素,细胞因子和其他蛋白质。在基线收集的血沉棕黄层来源的白细胞将用于分离DNA和建立永生化细胞系。红细胞将被存储用于血红蛋白加合物和其他成分的分析。结果:从这些分子研究中预期得到的特定结果将提供有关可能导致前列腺癌风险的因素的信息,这些因素可能会改变任一试验补充剂的功效,包括:类固醇性激素和几种多态性基因,这些基因编码影响前列腺素的蛋白质。 ,包括雄激素受体,II型甾体5α-还原酶,CYP17和β-羟基甾体脱氢酶; DNA修复基因和致癌物代谢基因的多态性,包括与化学致癌物活化为反应性中间体(例如CYP1A1)或反应性中间体的解毒(例如谷胱甘肽S-转移酶M1)有关的基因; DNA和蛋白质加合物;以及胰岛素样生长因子和瘦素。结论:SELECT提供了进行分子流行病学研究以评估基因与环境相互作用及其在前列腺,肺和结肠癌发生中的作用的绝好机会。

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