This dissertation included 3 studies to investigate the associations between EGFR mutation status and the genetic background and environmental carcinogens in never-smoking lung adenocarcinoma. Therefore, there will be several analyses and assays to be carried out: (1) Using the questionnaires, the relationships between exposures to the cigarette smoke, environmental tobacco smoke (ETS) and EGFR hotspot mutations will be delineated. (2) The genetic polymorphisms of the biosynthesis and catabolism of estrogen and DNA repair pathways will be studied in terms of the mechanisms of EGFR hotspot mutations. Study1: The Associations between Sex and Smoking Status on EGFR Mutations in Adenocarcinoma Background and Aims: To assess the impact of cigarette smoke and environmental tobacco smoke (ETS) are associated with the EGFR mutations status in adenocarcinoma patients. Methods: We enrolled 617 patients with lung adenocarcinoma. The history of cigarette smoking-related characteristics was obtained from a questionnaire; Among 132 patients who were also participated in the Genetic Epidemiological Study of Lung Adenocarcinoma (GELAC) study, the history of ETS exposure were obtained. Results: Patients with more than 21 pack-years of smoking histories or smokers with the fist use cigarette before the age of 29, or those who quit smoking less than 21 years had a significant lower frequency of EGFR mutations than never-smokers. Furthermore, there was a significantly inverse trend between smoking dose and EGFR mutation (p<0.0001). With regard to ETS, there was not a significant dose-response relationship of patients exposed to ETS with EGFR mutations. But a significant association was found for patients exposed to ETS for ≦ 16 years compared to patients not exposed to ETS (p=0.05). Additionally, Sex was significantly associated with EGFR mutation status in never-smokers (p=0.03). The percentage of in-frame deletion was higher in males than females (36.1% vs. 23.5%), and the percentage of L858R mutation was higher in females than males (28.8% vs. 20.4%). Conclusion: The amount and duration of cigarette smoking history were inversely associated with the EGFR mutations status. However, the impact of ETS remains inconclusive. In never-smokers, a significant difference was found between EGFR mutation subtypes and sex, this sex difference implies different mechanisms for the EGFR mutagenesis in EGFR mutation subtypes. Study2: EGFR L858R Mutation and Polymorphisms of Genes related to Estrogen Biosynthesis and Metabolism in Never-smoking Female Lung Adenocarcinoma Patients Background and Aims: To assess whether polymorphisms of genes related to estrogen biosynthesis and metabolism are associated with EGFR mutations. Methods: We studied 617 patients with lung adenocarcinoma, including 410 never-smoking patients. On the basis of multiple candidate genes approach, the effects of polymorphisms of CYP17, CYP19A1, ERα and COMT in association with the EGFR mutations status were evaluated using logistic regression analysis. Results: In female never-smokers, significant associations with EGFR L858R mutation were found for the (TTTA)n repeats in CYP19A1 (odds ratio [OR], 2.6; 95% confidence interval [CI], 1.2-5.7 for one or two alleles with (TTTA)n repeats >7 compared to both alleles with (TTTA)n repeats ≦7), and the rs2234693 in ERα (OR,2.1; 95% CI, 1.1-4.0 for C/T and C/C genotypes compared to T/T genotype). The C/C genotype (vs. T/T genotype) of ERα was significantly associated with EGFR L858R mutation (OR, 3.0; 95% CI, 1.1-8.1), in-frame deletion (OR, 2.9; 95% CI, 1.1-7.6) and other mutations (OR, 4.3; 95% CI, 1.3-14.0). The genotype of COMT rs4680 was significantly associated with EGFR L858R mutation in female and male never-smokers showing OR’s (95% CI) of 1.8 (1.0-3.2) and 3.6 (1.1-11.3), respectively, for genotypes G/A and G/G compared to genotype A/A. The number of risk alleles of CYP17, CYP19A1, ERα and COMT was associated with an increasing OR of EGFR L858R mutation in female never-smokers (P=.0002 for trend). Conclusions: The L858R mutation of EGFR is associated with polymorphisms of genes related to estrogen biosynthesis and metabolism in never-smoking female lung adenocarcinoma patients. The findings provide a clue for the genesis of EGFR mutations. Study3: EGFR Exon 19 In-frame Deletion and Polymorphisms of EGFR and DNA Repair Genes in Never-smoking Female Lung Adenocarcinoma Patients Background and Aims: To explore whether the genetic polymorphisms in genes related to DNA repair and detoxification metabolism and in epidermal growth factor receptor (EGFR) are associated with EGFR mutations. Methods: We studied 410 never-smoking patients with lung adenocarcinoma. Multivariate-adjusted OR [aOR] with the corresponding 95% confidence intervals [CI] of EGFR mutation status in association with genotypes were evaluated using logistic regression analysis. Results: The rs744154C/G in ERCC4 was significantly associated with EGFR exon19 in-frame deletion both in never-smokers (aOR, 1.7 with 95% CI, 1.0-3.0) and female never-smokers (aOR, 1.9 with 95% CI, 1.0-3.6), respectively. A significant association with EGFR exon19 in-frame deletion was found for the rs1800566C/T in NQO1 (aOR, 2.2 with 95% CI, 1.0-4.8) in female never-smokers. The rs1047840A/A genotype in EXO1 showed a 7.6-fold increase in the exon19 in-frame deletion in female never-smokers, but the association was marginally significant. Furthermore, the number of risk alleles in NQO1, ERCC4 and EXO1 was associated with an increasing aOR of EGFR exon19 in-frame deletion both in never-smokers and female never-smokers (P= 0.007 and 0.002 for trend, respectively). Additionally, the CA-repeat polymorphism in EGFR was significantly associated with exon19 in-frame deletion both in never-smokers (aOR, 1.7 with 95% CI, 1.0-2.9) and female never-smokers (aOR, 1.9 with 95% CI, 1.0-3.5), respectively, for both alleles with (CA)n repeats > 18 vs. one or two alleles ≦18). Conclusions: The exon19 in-frame deletion of EGFR is associated with polymorphisms in EGFR and DNA repair and detoxification metabolism genes in never-smoking lung adenocarcinoma patients, especially in females. The findings provide a clue about the genesis of EGFR mutations. In summary, EGFR hotspot mutations were more frequently found in never-smoking lung adenocarcinoma. Moreover, the sex difference in EGFR mutation subtypes was found in never-smoking lung adenocarcinoma, the exon 19 in-frame deletion was more frequently associated with male gender, while exon 21 mutations were more frequent in females. Additionally, from the viewpoints of molecular mechanisms of mutagenesis, the exon19 in-frame deletion of EGFR is associated with polymorphisms in EGFR and DNA repair and detoxification metabolism genes, while the L858R mutation of EGFR is associated with polymorphisms of genes related to estrogen biosynthesis and metabolism in never-smoking lung adenocarcinoma patients.