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吸烟相关的 O4-乙基胸腺嘧啶在人肺组织中的形成及其与大体积 DNA 加合物的比较。

Smoking-related O4-ethylthymidine formation in human lung tissue and comparisons with bulky DNA adducts.

机构信息

Department of Molecular Environmental Epidemiology, National Institute of Environmental Health, Gyáli út 2-6, H-1097 Budapest, Hungary.

出版信息

Mutagenesis. 2011 Jul;26(4):523-7. doi: 10.1093/mutage/ger011. Epub 2011 Mar 30.

Abstract

Tobacco smoke contains many alkylating agents that can react with DNA to produce O(4)-ethylthymidine (O(4)-etT) and several other types of promutagenic base modifications. Our aims were (i) to confirm results of a pilot study (Godschalk, R., Nair, J., Schooten, F. J., Risch, A., Drings, P., Kayser, K., Dienemann, H. and Bartsch, H. (2002) Comparison of multiple DNA adduct types in tumor adjacent human lung tissue: effect of cigarette smoking. Carcinogenesis, 23, 2081-2086) on the formation of O(4)-etT in smokers' lung; (ii) to explore associations between levels of O(4)-etT and smoking status and (iii) to investigate whether a correlation exists between levels of O(4)-etT and bulky (polycyclic aromatic hydrocarbons-derived) DNA adducts. Archived DNA samples originated from histologically normal peripheral lung tissues of 64 Hungarian lung cancer patients, who underwent lung resection. O(4)-etT was determined by an immunoenriched (32)P-postlabelling-high-performance liquid chromatography method. Levels of bulky DNA adducts were determined by the nuclease P1 adduct-enriched (32)P-postlabelling. O(4)-etT levels ranged from 0.01 to 3.91 adducts/10(8) thymidines. In the combined group of subjects who smoked until surgery or gave up smoking at most 1 year before it, the mean level of O(4)-etT was 1.7-fold (P = 0.015) and of bulky DNA adducts 2.2-fold (P < 0.0001) higher than in long-term ex-smokers (LES) and never-smokers (NS) combined. We found no significant correlation between the individual levels of the two DNA adduct types. No dose-response was detected between O(4)-etT formation and smoking dose. In one-third of LES, O(4)-etT levels were above the 2.0-fold mean level of adducts found in NS, indicating its high persistence. Our results confirm the smoking-related formation of O(4)-etT in human lung DNA that should be explored as biomarker. Its long persistence in target tissue implicates a role of this potentially miscoding lesion in tobacco smoking-associated cancers.

摘要

烟草烟雾中含有许多烷化剂,可与 DNA 发生反应生成 O(4)-乙基胸腺嘧啶 (O(4)-etT) 和其他几种促突变碱基修饰物。我们的目的是:(i) 证实一项初步研究(Godschalk, R., Nair, J., Schooten, F. J., Risch, A., Drings, P., Kayser, K., Dienemann, H. 和 Bartsch, H. (2002) 比较肿瘤旁人肺组织中多种 DNA 加合物类型:吸烟的影响。致癌作用,23, 2081-2086)中关于吸烟者肺中 O(4)-etT 形成的结果;(ii) 探讨 O(4)-etT 水平与吸烟状况之间的关系;(iii) 研究 O(4)-etT 水平与大体积(多环芳烃衍生)DNA 加合物之间是否存在相关性。从 64 名匈牙利肺癌患者的组织学正常外周肺组织中提取存档 DNA 样本,这些患者接受了肺切除术。通过免疫富集(32)P-后标记-高效液相色谱法测定 O(4)-etT 的水平。通过核酸酶 P1 加合物富集(32)P-后标记测定大体积 DNA 加合物的水平。O(4)-etT 水平范围为 0.01 至 3.91 个加合物/10(8)胸腺嘧啶。在联合组中,直到手术前仍在吸烟或在手术前最多 1 年内戒烟的受试者,O(4)-etT 的平均水平是长期戒烟者(LES)和从不吸烟者(NS)组合的 1.7 倍(P=0.015),大体积 DNA 加合物的水平是 2.2 倍(P<0.0001)。我们没有发现两种 DNA 加合物类型的个体水平之间存在显著相关性。O(4)-etT 形成与吸烟剂量之间没有剂量反应关系。在三分之一的 LES 中,O(4)-etT 水平高于 NS 中发现的加合物平均水平的 2.0 倍,表明其高持久性。我们的结果证实了 O(4)-etT 在人类肺 DNA 中的吸烟相关形成,这应该作为生物标志物进行探索。其在靶组织中的长期持久性表明,这种潜在的错配损伤在与吸烟相关的癌症中发挥作用。

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