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Analysis of cell-free circulating tumor DNA in 419 patients with glioblastoma and other primary brain tumors

机译:419例胶质母细胞瘤和其他原发性脑肿瘤患者无细胞循环肿瘤DNA的分析

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Aim: Genomically matched trials in primary brain tumors (PBTs) require recent tumor sequencing. We evaluated whether circulating tumor DNA (ctDNA) could facilitate genomic interrogation in these patients. Methods: Data from 419 PBT patients tested clinically with a ctDNA NGS panel at a CLIA-certified laboratory were analyzed. Results:?A total of?211 patients (50%) had ≥1 somatic alteration detected. Detection was highest in meningioma (59%) and gliobastoma (55%). Single nucleotide variants were detected in 61 genes, with amplifications detected in ERBB2, MET, EGFR?and others. Conclusion: Contrary to previous studies with very low yields, we found half of PBT patients had detectable ctDNA with genomically targetable off-label or clinical trial options for almost 50%. For those PBT patients with detectable ctDNA, plasma cfDNA genomic analysis is a clinically viable option for identifying genomically driven therapy options.
机译:目的:在原发性脑肿瘤(PBT)中进行基因组匹配的试验需要最近的肿瘤测序。我们评估了循环肿瘤DNA(ctDNA)是否可以促进这些患者的基因组研究。方法:分析了在CLIA认证的实验室中用ctDNA NGS小组临床测试的419名PBT患者的数据。结果:总共211例患者(50%)的体细胞变化≥1。在脑膜瘤(59%)和胶质母细胞瘤(55%)中检出率最高。在61个基因中检测到单核苷酸变异,并在ERBB2,MET,EGFR?等中检测到扩增。结论:与先前的低产率研究相反,我们发现一半的PBT患者具有可检测的ctDNA,且具有基因组靶向的脱标签或临床试验选择,几乎占50%。对于那些可检测到ctDNA的PBT患者,血浆cfDNA基因组分析是确定基因组驱动疗法的临床可行选择。

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