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肺癌患者的遗传变异与患者报告的生活质量。

Genetic variations and patient-reported quality of life among patients with lung cancer.

机构信息

Mayo Clinic, Rochester, MN 55905, USA.

出版信息

J Clin Oncol. 2012 May 10;30(14):1699-704. doi: 10.1200/JCO.2010.34.5629. Epub 2012 Mar 26.

DOI:10.1200/JCO.2010.34.5629
PMID:22454423
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3383115/
Abstract

PURPOSE

Recent evidence has suggested a relationship between the baseline quality of life (QOL) self-reported by patients with cancer and genetic disposition. We report an analysis exploring relationships among baseline QOL assessments and candidate genetic variations in a large cohort of patients with lung cancer.

PATIENTS AND METHODS

QOL data were provided by 1,299 patients with non-small-cell lung cancer observed at the Mayo Clinic between 1997 and 2007. Overall QOL and subdomains were assessed by either Lung Cancer Symptom Scale or Linear Analog Self Assessment measures; scores were transformed to a scale of 0 to 10, with higher scores representing better status. Baseline QOL scores assessed within 1 year of diagnosis were dichotomized as clinically deficient (CD) or not. A total of 470 single nucleotide polymorphisms (SNPs) in 56 genes of three biologic pathways were assessed for association with QOL measures. Logistic regression with training/validation samples was used to test the association of SNPs with CD QOL.

RESULTS

Six SNPs on four genes were replicated using our split schemes. Three SNPs in the MGMT gene (adjusted analysis, rs3858300; unadjusted analysis, rs10741191 and rs3852507) from DNA repair pathway were associated with overall QOL. Two SNPs (rs2287396 [GSTZ1] and rs9524885 [ABCC4]) from glutathione metabolic pathway were associated with fatigue in unadjusted analysis. In adjusted analysis, two SNPs (rs2756109 [ABCC2] and rs9524885 [ABCC4]) from glutathione metabolic pathway were associated with pain.

CONCLUSION

We identified three SNPs in three glutathione metabolic pathway genes and three SNPs in two DNA repair pathway genes associated with QOL measures in patients with non-small-cell lung cancer.

摘要

目的

最近的证据表明,癌症患者基线生活质量(QOL)自评与遗传倾向之间存在关系。我们报告了一项分析,该分析探讨了在大型肺癌患者队列中基线 QOL 评估与候选遗传变异之间的关系。

患者和方法

1997 年至 2007 年间,在梅奥诊所观察到的 1299 名非小细胞肺癌患者提供了 QOL 数据。通过肺癌症状量表或线性模拟自我评估量表评估总体 QOL 和子领域;评分转换为 0 到 10 的量表,得分越高表示状态越好。诊断后 1 年内评估的基线 QOL 评分分为临床不足(CD)或不。评估了三个生物学途径中 56 个基因的 470 个单核苷酸多态性(SNP)与 QOL 测量值的关联。使用训练/验证样本的逻辑回归测试 SNP 与 CD QOL 的关联。

结果

使用我们的拆分方案复制了四个基因中的六个 SNP。DNA 修复途径中 MGMT 基因的三个 SNP(调整分析,rs3858300;未调整分析,rs10741191 和 rs3852507)与总体 QOL 相关。谷胱甘肽代谢途径中的两个 SNP(rs2287396 [GSTZ1]和 rs9524885 [ABCC4])与疲劳在未调整分析中相关。在调整分析中,谷胱甘肽代谢途径中的两个 SNP(rs2756109 [ABCC2]和 rs9524885 [ABCC4])与疼痛相关。

结论

我们鉴定了三个来自三个谷胱甘肽代谢途径基因的 SNP 和两个来自两个 DNA 修复途径基因的 SNP,这些 SNP 与非小细胞肺癌患者的 QOL 测量值相关。

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Systematic evaluation of genetic variants in three biological pathways on patient survival in low-stage non-small cell lung cancer.三种生物途径中遗传变异对低分期非小细胞肺癌患者生存的系统评价。
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Genetic variation in glutathione metabolism and DNA repair genes predicts survival of small-cell lung cancer patients.谷胱甘肽代谢和 DNA 修复基因的遗传变异可预测小细胞肺癌患者的生存。
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