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Deciphering intratumor heterogeneity using cancer genome analysis

机译:使用癌症基因组分析破译肿瘤内异质性

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摘要

Intratumor heterogeneity within individual cancer tissues underlies the numerous phenotypes of cancer. Tumor subclones ultimately affect therapeutic outcomes due to their distinct molecular features. Drug-resistant subclones are present at a low frequency in tissues at the time of biopsy, but can also arise as a result of acquired somatic mutations. A number of different approaches have been utilized to understand the nature of intratumor heterogeneity. Clonal analysis using whole exome or genome sequencing data can help monitor subclones in the context of tumor progression. Multiregional biopsies permit the molecular characterization of subclones within tumors. Deep sequencing has also provided researchers with the ability to measure the low allele fraction variant within a small number of cells. Ultimately, single-cell sequencing will enable the identification of every minor population within a tumor microenvironment. In the clinical context, the ability to identify and monitor the subclonal architecture of a tumor is valuable for the development of precise cancer therapeutic methods.
机译:单个癌症组织内的肿瘤内异质性是癌症众多表型的基础。肿瘤亚克隆由于其独特的分子特征而最终影响治疗效果。在活检时,耐药性亚克隆在组织中的存在频率较低,但也可能由于获得性体细胞突变而产生。已经利用许多不同的方法来了解肿瘤内异质性的性质。使用整个外显子组或基因组测序数据进行的克隆分析可帮助监测肿瘤进展过程中的亚克隆。多区域活检可以对肿瘤内的亚克隆进行分子鉴定。深度测序还为研究人员提供了测量少量细胞中低等位基因片段变异的能力。最终,单细胞测序将能够鉴定肿瘤微环境中的每个未成年人。在临床背景下,鉴定和监测肿瘤亚克隆结构的能力对于开发精确的癌症治疗方法非常有价值。

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