Role of O6-alkylguanine in nitrosamine-induced cancers

O6-烷基鸟嘌呤在亚硝胺诱发的癌症中的作用

• 批准号: 7060517
• 负责人: Lisa A Peterson
• 金额: $ 25.39万
• 依托单位: UNIVERSITY OF MINNESOTA
• 依托单位国家: 美国
• 财政年份: 2005
• 资助国家: 美国
• 起止时间: 2005-05-01 至 2010-04-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/7060517
• 关键词: DNA repair; adduct; cancer risk; chemical carcinogen; chemical carcinogenesis; clinical research; genetic susceptibility; human tissue; laboratory mouse; lung neoplasms; methylguanine DNA methyltransferase; mutagens; nitrosamines; pyridine; tobacco

DESCRIPTION (provided by applicant): Tobacco-specific nitrosamines, NNK and NNN, are carcinogenic in laboratory and are potential human carcinogens. NNN is metabolized to a DNA pyridyloxobutylating agent whereas NNK is metabolized to both DNA pyridyloxobutylating and methylating intermediates. Pyridyloxobutylation of DNA results in the formation of a variety of DNA adducts, one of which is O6-[4-oxo-4-(3-pyridyl)butyl]guanine (O6-pobG). Our previous studies indicate that this mutagenic adduct is repaired by O6-alkylguanine-DNA alkyltransferase (AGT). Human AGT variants differ substantially in their ability to repair O6-pobG, suggesting that individuals with reduced repair capacity may be at increased risk of tobacco-related cancers. However, it is unclear what the overall role O6-pobG makes in the mutagenic and carcinogenic properties of pyridyloxobutylating nitrosamines. The central hypothesis under investigation in this grant is that O6-pobG contributes significantly to the mutagenic and carcinogenic activity of the tobacco-specific nitrosamines, NNK and NNN, when not repaired. We plan to test our central hypothesis by pursuing the following specific aims: 1) Determine if O6-pobG formation and persistence are linked to the pulmonary carcinogenic properties of NNN and NNKOAc in A/J mice. 2) Phenotype human livers for their ability to repair bulky O6-alkylguanine adducts relative to O6-mG adducts by AGT. 3) Determine the involvement of other repair pathways in the overall repair of the mutagenic O6-pobG and determine whether these pathways affect the mutagenic properties of pyridyloxobutylating agents. Collectively, these aims will establish the importance of formation and repair of O6-pobG in the mutagenic and carcinogenic properties of pyridyloxobutylating nitrosamines. These studies will set the stage for a molecular epidemiological study to determine whether individuals who are unable to repair this mutagenic adduct are at increased risk of tobacco-related cancers.

描述（由申请人提供）：烟草特有的亚硝胺，NNK和NNN，在实验室中具有致癌性，是潜在的人类致癌物。NNN代谢为DNA吡啶氧丁基化试剂，而NNK代谢为DNA吡啶氧丁基化和甲基化中间体。DNA的吡啶基氧代丁基化导致形成多种DNA加合物，其中之一是O 6-[4-氧代-4-（3-吡啶基）丁基]鸟嘌呤（O 6-pobG）。我们以前的研究表明，这种致突变加合物是修复的O 6-烷基鸟嘌呤-DNA烷基转移酶（AGT）。人类AGT变异体在修复O 6-pobG的能力上有很大的不同，这表明修复能力降低的个体患烟草相关癌症的风险可能会增加。然而，目前还不清楚O 6-pobG在吡啶氧丁基化亚硝胺的致突变性和致癌性中的总体作用。在这项研究中，研究的中心假设是，O 6-pobG在未修复时对烟草特有的亚硝胺NNK和NNN的致突变和致癌活性有显著影响。我们计划通过追求以下具体目标来测试我们的中心假设：1）确定O 6-pobG形成和持久性是否与A/J小鼠中NNN和NNKOAc的肺致癌特性相关。2)表型人类肝脏的能力，修复庞大的O 6-烷基鸟嘌呤加合物相对于O 6-mG加合物AGT。3)确定其他修复途径参与致突变O 6-pobG的整体修复，并确定这些途径是否影响吡啶氧代丁基化试剂的致突变性。总的来说，这些目标将建立的重要性，形成和修复的O 6-pobG的致突变性和致癌性的吡啶氧丁基亚硝胺。这些研究将为分子流行病学研究奠定基础，以确定无法修复这种诱变加合物的个体是否会增加患烟草相关癌症的风险。