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Diagnostic value of next-generation sequencing in an unusual sphenoid tumor

机译:下一代测序对罕见蝶骨肿瘤的诊断价值

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Extraordinary advancements in sequencing technology have made what was once a decade-long multi-institutional endeavor into a methodology with the potential for practical use in a clinical setting. We therefore set out to examine the clinical value of next-generation sequencing by enrolling patients with incurable or ambiguous tumors into the Personalized OncoGenomics initiative at the British Columbia Cancer Agency whereby whole genome and transcriptome analyses of tumor/ normal tissue pairs are completed with the ultimate goal of directing therapeutics. First, we established that the sequencing, analysis, and communication with oncologists could be completed in less than 5 weeks Second, we found that cancer diagnostics is an area that can greatly benefit from the comprehensiveness of a whole genome analysis. Here, we present a scenario in which a metastasized sphenoid mass, which was initially thought of as an undifferentiated squamous cell carcinoma, was rediagnosed as an SMARCB1-negative rhabdoid tumor based on the newly acquired finding of homozygous SMARCB1 deletion. The new diagnosis led to a change in chemotherapy and a complete nodal response in the patient. This study also provides additional insight into the mutational landscape of an adult SMARCB1-negative tumor that has not been explored at a whole genome and transcriptome level.
机译:测序技术的非凡进步,使曾经是长达十年之久的多机构研究成果成为一种具有实际临床应用潜力的方法。因此,我们着手通过将不治之症或模棱两可的肿瘤患者纳入不列颠哥伦比亚癌症局的“个性化肿瘤基因组学”计划,以检验肿瘤/正常组织对的全基因组和转录组分析,从而完成下一代测序的临床价值指导治疗的目标。首先,我们确定测序,分析和与肿瘤科医生的交流可以在不到5周的时间内完成。其次,我们发现癌症诊断是一个可以从全基因组分析的全面性中受益的领域。在这里,我们提出了一种场景,其中基于最初获得的纯合子SMARCB1缺失发现,最初被认为是未分化的鳞状细胞癌的蝶骨转移瘤被重新诊断为SMARCB1阴性横纹肌瘤。新的诊断导致化学疗法的改变和患者的完全淋巴结反应。这项研究还提供了对成人SMARCB1阴性肿瘤的突变态势的进一步了解,该突变态尚未在整个基因组和转录组水平上进行研究。

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