Pavanello Sofia, Pulliero Alessandra, Lupi Silvia, Gregorio Pasquale, Clonfero Erminio
Occupational Health Section, Department of Environmental Medicine and Public Health, University of Padova, Via Giustiniani 2, Padova 35128, Italy.
Mutat Res. 2005 Nov 10;587(1-2):59-66. doi: 10.1016/j.mrgentox.2005.08.008. Epub 2005 Sep 26.
The functional significance of genetic polymorphisms on tobacco smoke-induced CYP1A2 activity was examined. The influence of three polymorphisms of the cytochrome P450 1A2 gene (CYP1A2) (-3860 G-->A (allele *1C), -2467 T-->delT (allele *1D), -163C-->A (allele *1F)), located in the 5'-noncoding promoter region of the gene, on CYP1A2 activity (measured as caffeine metabolic ratio, CMR), was studied in Caucasian current smokers (n=95). Tobacco smoke intake was calculated from the number of cigarettes/day. Also, studied was the influence of these CYP1A2 genotypes on smoking-associated urinary mutagenicity, detected in Salmonella typhimurium strain YG1024 with S9 mix, considering the urinary excretion of nicotine plus its metabolites as an internal indicator of tobacco smoke exposure. Smokers with at least one of the variant alleles CYP1A2 -3860A and -2467 delT showed a significantly increased CYP1A2 CMR (-3860 G/A versus G/G, p<0.05; -2467 delT/delT versus T/delT and T/T, p<0.01). Multiple regression analysis showed that the increase in CYP1A2 CMR (ln values) was again significantly related to the presence of CYP1A2 variants -2467delT and also to variant -163A (p<0.05), but moderately to -3860A (p=0.084). No influence of the number of cigarettes smoked per day by each subject was found. Heavy smokers (n=48, with urinary nicotine plus its metabolites>or=0.69 mg/mmol creatinine) with variant allele -2467delT or -163A had significantly increased urinary mutagenicity (p<0.01 and <0.05). CYP1A2 genetic polymorphisms are shown to influence the CYP1A2 phenotype in smokers, -2467 T-->delT having the main effect. This information is of interest for future studies assessing the possible role of tobacco smoke-inducible CYP1A2 genotypes as individual susceptibility factors in exposure to carcinogens.
研究了基因多态性对烟草烟雾诱导的CYP1A2活性的功能意义。细胞色素P450 1A2基因(CYP1A2)位于基因5'-非编码启动子区域的三种多态性(-3860 G→A(等位基因1C)、-2467 T→delT(等位基因1D)、-163C→A(等位基因*1F))对CYP1A2活性(以咖啡因代谢率,CMR衡量)的影响,在白种人现吸烟者(n = 95)中进行了研究。根据每天吸烟支数计算烟草烟雾摄入量。此外,考虑到尿中尼古丁及其代谢产物的排泄作为烟草烟雾暴露的内部指标,研究了这些CYP1A2基因型对吸烟相关尿致突变性的影响,该致突变性在鼠伤寒沙门氏菌菌株YG1024与S9混合液中检测。携带至少一个CYP1A2 -3860A和-2467 delT变异等位基因的吸烟者显示CYP1A2 CMR显著增加(-3860 G/A与G/G相比,p<0.05;-2467 delT/delT与T/delT和T/T相比,p<0.01)。多元回归分析表明,CYP1A2 CMR(ln值)的增加再次与CYP1A2变异体-2467delT以及变异体-163A的存在显著相关(p<0.05),但与-3860A呈中度相关(p = 0.084)。未发现每位受试者每天吸烟支数的影响。携带变异等位基因-2467delT或-163A的重度吸烟者(n = 48,尿中尼古丁及其代谢产物≥0.69 mg/mmol肌酐)尿致突变性显著增加(p<0.01和<0.05)。结果表明,CYP1A2基因多态性影响吸烟者的CYP1A2表型,其中-2467 T→delT起主要作用。该信息对于未来评估烟草烟雾诱导的CYP1A2基因型作为个体对致癌物暴露易感性因素的可能作用的研究具有重要意义。
