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Integrative genetic analysis suggests that skin color modifies the genetic architecture of melanoma

机译:综合遗传分析表明肤色可改变黑色素瘤的遗传结构

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摘要

Melanoma is the deadliest form of skin cancer and presents a significant health care burden in many countries. In addition to ultraviolet radiation in sunlight, the main causal factor for melanoma, genetic factors also play an important role in melanoma susceptibility. Although genome-wide association studies have identified many single nucleotide polymorphisms associated with melanoma, little is known about the proportion of disease risk attributable to these loci and their distribution throughout the genome. Here, we investigated the genetic architecture of melanoma in 1,888 cases and 990 controls of European non-Hispanic ancestry. We estimated the overall narrow-sense heritability of melanoma to be 0.18 (P < 0.03), indicating that genetics contributes significantly to the risk of sporadically-occurring melanoma. We then demonstrated that only a small proportion of this risk is attributable to known risk variants, suggesting that much remains unknown of the role of genetics in melanoma. To investigate further the genetic architecture of melanoma, we partitioned the heritability by chromosome, minor allele frequency, and functional annotations. We showed that common genetic variation contributes significantly to melanoma risk, with a risk model defined by a handful of genomic regions rather than many risk loci distributed throughout the genome. We also demonstrated that variants affecting gene expression in skin account for a significant proportion of the heritability, and are enriched among melanoma risk loci. Finally, by incorporating skin color into our analyses, we observed both a shift in significance for melanoma-associated loci and an enrichment of expression quantitative trait loci among melanoma susceptibility variants. These findings suggest that skin color may be an important modifier of melanoma risk. We speculate that incorporating skin color and other non-genetic factors into genetic studies may allow for an improved understanding of melanoma susceptibility and guide future investigations to identify melanoma risk genes.
机译:黑色素瘤是最致命的皮肤癌形式,在许多国家/地区构成了巨大的医疗保健负担。除了阳光中的紫外线外,黑素瘤的主要致病因素,遗传因素在黑素瘤易感性中也起重要作用。尽管全基因组关联研究已经确定了许多与黑色素瘤相关的单核苷酸多态性,但对于这些基因座引起的疾病风险比例及其在整个基因组中的分布知之甚少。在这里,我们调查了1888例黑色素瘤的遗传结构和990例欧洲非西班牙裔血统的对照。我们估计黑色素瘤的总体狭义遗传力为0.18(P <0.03),这表明遗传因素对偶发性黑色素瘤的风险有重大贡献。然后,我们证明了这种风险的一小部分可归因于已知的风险变异,这表明遗传因素在黑素瘤中的作用仍然未知。为了进一步研究黑色素瘤的遗传结构,我们按染色体,次要等位基因频率和功能注释对遗传力进行了划分。我们发现,常见的遗传变异对黑色素瘤风险有显着贡献,其风险模型由少数基因组区域而不是整个基因组分布的许多风险基因座定义。我们还证明,影响皮肤中基因表达的变异体占遗传力的很大比例,并且在黑色素瘤风险基因座中富集。最后,通过将肤色纳入我们的分析,我们观察到黑素瘤相关基因座的重要性发生了变化,并且黑素瘤易感性变体之间的表达数量性状基因座也有所增加。这些发现表明肤色可能是黑色素瘤风险的重要调节剂。我们推测,将肤色和其他非遗传因素纳入遗传研究可能有助于更好地了解黑色素瘤易感性,并指导今后的研究以鉴定黑色素瘤的风险基因。

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