NBS1基因的替换与年轻乳腺癌患者的临床病理特征

Roberta Vadeikienė, A. Savukaitytė, R. Ugenskienė, Jurgita Gudaitienė, E. Juozaitytė
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摘要

*通讯作者。电子邮件:roberta.vadeikiene@lsmuni.lt;r.jankauskaite@gmail.com本研究的目的是确定年轻(≤50岁)乳腺癌患者中可能与NBS1突变和多态性相关的特征。收集了80名乳腺癌患者的血液。采用PCR-RFLP方法对NBS1基因突变C .657_661del、p.R215W、p.I171V和多态性C . 8360g >C、C . 30537g >C进行基因分型。单因素分析采用双侧卡方检验,优势比评价采用logistic回归分析。未发现c.657_661del、p.R215W和p.I171V突变携带者。logistic回归分析显示,GC和CC基因型与GG基因型相比,低级别肿瘤的风险分别降低了2.885倍(OR = 2.885, 95% CI 0.173 ~ 0.735, P = 0.005)和2.186倍(OR = 2.186, 95% CI 0.188 ~ 0.888, P = 0.024)。与GG基因型相比,8360 CC基因型(OR = 3.034, 95% CI 0.156 ~ 0.778, P = 0.010)显著增加了HER2扩增的机会。NBS1 8360 GC基因型乳腺癌进展风险较高(OR = 1.673, 95% CI 0.233 ~ 0.915, P = 0.027)。纯合子8360 CC携带者的疾病进展风险约为6倍(OR = 5.946, 95% CI 0.098-0.585, P = 0.002)。NBS1 8360 CC基因型的三阴性乳腺癌患病率显著高于NBS1 8360 CC基因型(OR = 2.186, 95% CI 0.188 ~ 0.888, P = 0.024)。关于C . 30537g >C多态性,各基因型对病理特征均无显著影响。NBS1基因C . 8360g >C多态性可能与年轻乳腺癌患者的乳腺癌侵袭性有关。
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Substitutions of the NBS1 gene and clinicopathological characteristics of young breast cancer patients
* Corresponding author. Email: roberta.vadeikiene@lsmuni.lt; r.jankauskaite@gmail.com The purpose of this study was to determine characteristics potentially related to NBS1 mutations and polymorphisms in young (≤50 years of age) breast cancer patients. Blood from 80 breast cancer patients was collected. NBS1 mutations c.657_661del, p.R215W, p.I171V, and polymorphisms c.8360G>C, c.30537G>C were genotyped by the PCR-RFLP method. Two-sided Chi-square test was used for univariate analysis and logistic regression analysis was used to evaluate the odds ratio. No carriers of the c.657_661del, p.R215W and p.I171V mutations were found. NBS1 c.8360G>C logistic regression analysis showed that GC and CC genotypes compared with GG genotype had decreased risk of low grade tumour, 2.885-fold (OR = 2.885, 95% CI 0.173–0.735, P = 0.005) and 2.186-fold (OR = 2.186, 95% CI 0.188–0.888, P = 0.024), respectively. 8360 CC genotype (OR = 3.034, 95% CI 0.156–0.778, P = 0.010) significantly increased the chances of HER2 amplification compared to GG genotype. NBS1 8360 GC genotype had a higher risk for breast cancer progression (OR = 1.673, 95% CI 0.233–0.915, P = 0.027). The homozygote 8360 CC carriers had approximately a six times higher risk for the disease progress (OR = 5.946, 95% CI 0.098–0.585, P = 0.002). The prevalence of triple negative breast cancer type was significantly higher in individuals with NBS1 8360 CC genotype (OR = 2.186, 95% CI 0.188–0.888, P = 0.024). Regarding c.30537G>C polymorphism, none of the genotypes had a significant influence on pathological characteristics. NBS1 gene c.8360G>C polymorphism might be associated with breast cancer aggressiveness in young breast cancer patients.
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