Cell-Free DNA Genomic Profiling and Its Clinical Implementation in Advanced Prostate Cancer

前列腺癌 胎儿游离DNA 医学 肿瘤科 液体活检 内科学 DNA测序 循环肿瘤细胞 原发性肿瘤 个性化医疗 癌症 生物信息学 转移 生物 基因 遗传学 胎儿 产前诊断 怀孕
作者
Ivana Bratić Hench,Luca Roma,Floriana Conticelli,Lenard Bubendorf,Byron Calgua,Clémentine Le Magnen,Salvatore Piscuoglio,Mark A. Rubin,Alin Chirindel,Guillaume Nicolas,Tatjana Vlajnic,Tobias Zellweger,Arnoud J. Templeton,Frank Stenner,Christian Ruiz,Cyrill A. Rentsch,Lukas Bubendorf
出处
期刊:Cancers [MDPI AG]
卷期号:16 (1): 45-45 被引量:5
标识
DOI:10.3390/cancers16010045
摘要

Most men with prostate cancer (PCa), despite potentially curable localized disease at initial diagnosis, progress to metastatic disease. Despite numerous treatment options, choosing the optimal treatment for individual patients remains challenging. Biomarkers guiding treatment sequences in an advanced setting are lacking. To estimate the diagnostic potential of liquid biopsies in guiding personalized treatment of PCa, we evaluated the utility of a custom-targeted next-generation sequencing (NGS) panel based on the AmpliSeq HD Technology. Ultra-deep sequencing on plasma circulating free DNA (cfDNA) samples of 40 metastatic castration-resistant PCa (mCRPC) and 28 metastatic hormone-naive PCa (mCSPC) was performed. CfDNA somatic mutations were detected in 48/68 (71%) patients. Of those 68 patients, 42 had matched tumor and cfDNA samples. In 21/42 (50%) patients, mutations from the primary tumor tissue were detected in the plasma cfDNA. In 7/42 (17%) patients, mutations found in the primary tumor were not detected in the cfDNA. Mutations from primary tumors were detected in all tested mCRPC patients (17/17), but only in 4/11 with mCSPC. AR amplifications were detected in 12/39 (31%) mCRPC patients. These results indicate that our targeted NGS approach has high sensitivity and specificity for detecting clinically relevant mutations in PCa.
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