首页> 外文期刊>Lung cancer: Journal of the International Association for the Study of Lung Cancer >Association of L-myc polymorphism with lung cancer susceptibility and prognosis in relation to age-selected controls and stratified cases.
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Association of L-myc polymorphism with lung cancer susceptibility and prognosis in relation to age-selected controls and stratified cases.

机译:L-myc基因多态性与肺癌易感性和预后的关系,与年龄选择的对照组和分层病例有关。

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The association of L-myc polymorphism with cancer susceptibility and prognosis has produced conflicting results. This may have been due to racial/ethnic differences and methodological variations in the studies, such as, control selection and case stratification. Therefore, we investigated the genotype distribution of the L-myc polymorphism in 169 lung cancer patients and 169 non-cancer controls, and analyzed the association of this polymorphism with cancer susceptibility and prognosis in relation to age-specific controls as well as stratified cases. The genotype frequencies in the Taiwanese non-cancer controls were 0.56 (L) and 0.44 (S). Chi-square (chi(2)) analysis indicated a significant difference in the Taiwanese genotype distribution of L-myc compared with that of African-Americans (P=0.001). Logistic regression analysis of cases/controls, adjusted for both age and sex, indicated that an increased frequency of the LL genotype was observed in early-staged patients compared with the non-cancer controls (OR=0.43, 95% CI, 0.20-0.94, P=0.03). In addition, the frequency of the LL genotype was significantly higher in stages I+II patients (47.4%) than in stages III+IV patients (28.4%) (P=0.05). Furthermore, the S allele frequency was significantly increased in stages III+IV patients (P=0.005). As both L-myc and p53 polymorphisms were analyzed for their prognostic value, the patients with an S allele of the L-myc gene and a Pro/Pro variant genotype of the p53 gene had significantly poorer prognoses compared with other patients (P=0.004, by the log rank test). These data suggest that the S allele of the L-myc polymorphism may be associated with lung cancer progression.
机译:L-myc基因多态性与癌症易感性和预后的关系产生了矛盾的结果。这可能是由于种族/种族差异和研究方法的差异,例如对照选择和病例分层。因此,我们调查了169例肺癌患者和169例非癌对照中L-myc基因多态性的基因型分布,并分析了该多态性与特定年龄对照和分层病例的癌症易感性和预后的关系。台湾非癌症对照的基因型频率为0.56(L)和0.44(S)。卡方(chi(2))分析表明,与非裔美国人相比,台湾地区L-myc基因型分布存在显着差异(P = 0.001)。对年龄/性别进行调整的病例/对照的逻辑回归分析表明,与非癌症对照相比,早期患者观察到LL基因型的频率增加(OR = 0.43、95%CI,0.20-0.94 ,P = 0.03)。此外,I + II期患者的LL基因型频率(47.4%)明显高于III + IV期患者的(28.4%)(P = 0.05)。此外,III + IV期患者的S等位基因频率显着增加(P = 0.005)。由于分析了L-myc和p53多态性的预后价值,与其他患者相比,具有L-myc基因的S等位基因和p53基因的Pro / Pro变异基因型的患者的预后明显较差(P = 0.004 ,通过日志等级测试)。这些数据表明,L-myc多态性的S等位基因可能与肺癌的进展有关。

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