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The association of host and genetic melanoma risk factors with Breslow thickness in the Western Australian Melanoma Health Study

机译:在澳大利亚西部黑色素瘤健康研究中,宿主和遗传性黑素瘤危险因素与Breslow厚度的关联

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摘要

BACKGROUND: Breslow thickness is the most important predictor of survival in localized malignant melanoma. A number of melanoma risk factors have been shown to be associated with Breslow thickness; however, the role of genetic loci has been little investigated to date. OBJECTIVES: To investigate the association of known melanoma susceptibility genetic loci with Breslow thickness. METHODS: Participants were 800 individuals from the Western Australian Melanoma Health Study who completed a questionnaire and provided a DNA sample. Genetic association analyses between single-nucleotide polymorphisms (SNPs) from 15 candidate melanoma susceptibility genes and Breslow thickness were performed, controlling for relevant covariates. RESULTS: Older age at diagnosis and absence of naevi were associated with increased Breslow thickness. Following adjustment for multiple testing, no SNPs were significantly associated with Breslow thickness. CONCLUSIONS: Associations observed between Breslow thickness and age and naevi reinforce current knowledge. Some evidence of shared genetic determinants between melanoma risk and Breslow thickness was found. Further studies are required to confirm this finding.
机译:背景:Breslow厚度是局部恶性黑色素瘤生存的最重要预测指标。许多黑色素瘤危险因素已被证明与Breslow厚度有关。然而,迄今为止,基因座的作用尚未得到研究。目的:探讨已知的黑色素瘤易感性基因位点与Breslow厚度的关系。方法:参与者来自西澳大利亚黑素瘤健康研究的800个人,他们完成了问卷并提供了DNA样本。进行了来自15个候选黑色素瘤易感基因的单核苷酸多态性(SNP)与Breslow厚度之间的遗传关联分析,以控制相关的协变量。结果:诊断时年龄较大和没有naevi与Breslow厚度增加有关。经过多次测试调整后,没有任何SNP与Breslow厚度显着相关。结论:Breslow厚度与年龄和naevi之间的关联增强了当前的知识。发现了黑色素瘤风险和Breslow厚度之间共有遗传决定因素的一些证据。需要进一步的研究以证实这一发现。

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