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Defining a mutational signature for endometrial cancer screening and early detection

机译:定义子宫内膜癌筛选和早期检测的突变签名

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Introduction The current availability of genomic information represents an opportunity to develop new strategies for early detection of cancer. New molecular tests for endometrial cancer may improve performance and failure rates of histological aspirate-based diagnosis, and provide promising perspectives for a potential screening scenario. However, the selection of relevant biomarkers to develop efficient strategies can be a challenge. Materials and methods: We developed an algorithm to identify the largest number of patients with endometrial cancer using the minimum number of somatic mutations based on The Cancer Genome Atlas (TCGA) dataset. Results: The algorithm provided the number of subjects with mutations (sensitivity) for a given number of biomarkers included in the signature. For instance, by evaluating the 50 most representative point mutations, up to 81.9% of endometrial cancers can be identified in the TCGA dataset. At gene level, a 92.9% sensitivity can be obtained by interrogating five genes. Discussion: We developed a computational method to aid in the selection of relevant genomic biomarkers in endometrial cancer that can be adapted to other cancer types or diseases.
机译:简介目前基因组信息的可用性代表了开发新癌症的新策略的机会。子宫内膜癌的新分子试验可以改善组织学吸引的诊断的性能和失效率,并为潜在的筛查情景提供有希望的观点。然而,选择相关的生物标志物,以发展有效的策略可能是一个挑战。材料和方法:我们开发了一种使用基于癌症基因组地图集(​​TCGA)数据集的体细胞突变数量的最小数量的子宫内膜癌鉴定最大数量的算法。结果:该算法为特定数量的生物标志物提供了具有突变(灵敏度)的受试者的数量。例如,通过评估50个最代表性的点突变,可以在TCGA数据集中鉴定高达81.9%的子宫内膜癌。在基因水平下,通过询问五个基因可以获得92.9%的灵敏度。讨论:我们开发了一种计算方法,以帮助选择子宫内膜癌中的相关基因组生物标志物,其可以适应其他癌症类型或疾病。

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