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首页> 外文期刊>Journal of oncology >Potential Functional Variants in DNA Repair Genes Are Associated with Efficacy and Toxicity of Radiotherapy in Patients with Non-Small-Cell Lung Cancer
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Potential Functional Variants in DNA Repair Genes Are Associated with Efficacy and Toxicity of Radiotherapy in Patients with Non-Small-Cell Lung Cancer

机译:DNA修复基因中的潜在功能变体与非小细胞肺癌患者放射疗法的疗效和毒性有关

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Background. Lung cancer is one of the leading causes of cancer-related deaths. Radiotherapy, either alone or with chemotherapy, is still the primary treatment for patients with non-small-cell lung cancer (NSCLC). There are variations in how patients with NSCLC respond to radiotherapy and how toxic the therapy is. DNA repair gene polymorphisms are related to cancer development; however, their association with radiotherapy outcomes remains unknown. We hypothesized that gDNA repair gene variation could affect the efficacy and toxicity of radiotherapy in patients with NSCLC. Methods. A total of 486 histologically confirmed patients with NSCLC were recruited from the Shengjing Hospital of China Medical University from July 2015 to September 2019. Eleven potentially functional single nucleotide polymorphisms (SNPs) in four DNA repair genes (XRCC1, XRCC2, XPD, and MSH2) were genotyped in these patients. A multiple factor logistic regression analysis was used to assess the association between these SNPs and the efficacy and toxicity of radiotherapy. Results. Three SNPs, rs25487 (XRCC1), rs3218556 (XRCC2), and rs13181 (XPD), were all significantly associated with the efficacy of radiotherapy. The allele frequencies of the rs25487 CC genotype (OR?=?0.457, 95% CI?=?0.259–0.804, p=0.006) and the rs3218556 AG or AA genotypes (AG genotype: OR?=?0.664, 95% CI?=?0.442–0.999, p=0.049; AA genotype: OR?=?0.380, 95% CI?=?0.181–0.795, p=0.008) were both significantly higher in the response group than in the nonresponse group. For rs13181, the radiotherapy efficacy was associated with the heterozygous genotype GT (OR?=?1.663, 95% CI?=?1.057–2.614,p=0.027). Statistically significant associations between radiation-induced toxic reactions and rs25487 (XRCC1), rs3218556 (XRCC2), and rs13181 (XPD) were also observed. The rs13181GT genotype was associated with lower toxic reactions than the TT genotype (OR?=?1.680, 95% CI?=?1.035–2.728,p=0.035). Conclusions. The variants rs25487 (XRCC1), rs3218556 (XRCC2), and rs13181 (XPD) all contribute to the efficacy and toxicity of radiotherapy in patients with NSCLC. Our findings may clarify the predictive value of DNA repair genes for prognosis in patients with NSCLC after radiotherapy. Further investigation of more genes and samples should be performed to confirm our findings.
机译:背景。肺癌是癌症相关死亡的主要原因之一。无论是单独的还是化疗的放射疗法仍然是非小细胞肺癌(NSCLC)患者的主要治疗方法。 NSCLC患者如何应对放射疗法以及治疗的毒性有多种变化。 DNA修复基因多态性与癌症发育有关;然而,它们与放射治疗结果的关联仍然未知。我们假设GDNA修复基因变异可能影响NSCLC患者放射治疗的疗效和毒性。方法。从2015年7月到2019年7月,从中国医科大学盛静医院招募了486名与NSCLC患者。四个DNA修复基因(XRCC1,XRCC2,XPD和MSH2)中,11个潜在的官能单核苷酸多态性(SNP)在这些患者中进行了基因分型。多因素逻辑回归分析用于评估这些SNP之间的关联和放射疗法的疗效和毒性。结果。三个SNP,RS25487(XRCC1),RS3218556(XRCC2)和RS13181(XPD)都与放射疗法的功效显着相关。 RS25487 CC基因型的等位基因频率(或?= 0.457,95%CI?= 0.259-0.804,P = 0.006)和RS3218556 AG或AA基因型(Ag基因型:或?= 0.664,95%CI? =?0.442-0.999,p = 0.049; AA基因型:或?= 0.380,95%ci?= 0.181-0.795,p = 0.008)在响应组中显着高于非响应组。对于RS13181,放射疗法疗效与杂合学基因型GT(或α=β1.663,95%CI =α1.1.057-2.614,P = 0.027)有关。还观察到辐射诱导的毒性反应和RS25487(XRCC1),RS3218556(XRCC2)和RS13181(XPD)之间的统计学上显着的关联。 RS13181GT基因型与TT基因型(或α=Δ1.680,95%CI =Δ1.035-2.728,P = 0.035)相关,RS13181GT基因型与较低的毒性反应相关。结论。 Variants RS25487(XRCC1),RS3218556(XRCC2)和RS13181(XPD)都有助于NSCLC患者放射治疗的疗效和毒性。我们的研究结果可以阐明DNA修复基因的预测值,以在放疗后NSCLC患者预后的预测值。应进行进一步调查更多基因和样品以确认我们的研究结果。

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