循环肿瘤DNA在转移性去势抵抗性前列腺癌临床管理中的应用:一项多中心真实世界研究
Use of Circulating Tumor DNA for the Clinical Management of Metastatic Castration-Resistant Prostate Cancer: A Multicenter, Real-World Study.
作者信息
Dong Baijun, Fan Liancheng, Yang Bin, Chen Wei, Li Yonghong, Wu Kaijie, Zhang Fengbo, Dong Haiying, Cheng Huihua, Pan Jiahua, Zhu Yinjie, Chi Chenfei, Dong Liang, Sha Jianjun, Li Lei, Yao Xudong, Xue Wei
机构信息
1Department of Urology, Renji Hospital, School of Medicine, Shanghai Jiao Tong University, Shanghai.
2Department of Urology, Shanghai Tenth People's Hospital, Tongji University School of Medicine, Shanghai.
出版信息
J Natl Compr Canc Netw. 2021 May 14;19(8):905-914. doi: 10.6004/jnccn.2020.7663.
BACKGROUND
This study aimed to describe the aberrations of DNA damage repair genes and other important driving genes in Chinese patients with metastatic castration-resistant prostate cancer (mCRPC) using circulating tumor (ctDNA) sequencing and to evaluate the associations between the clinical outcomes of multiple therapies and key genomic alterations in mCRPC, especially DNA damage repair genes.
PATIENTS AND METHODS
A total of 292 Chinese patients with mCRPC enrolled from 8 centers. Multigene targeted sequencing was performed on 306 ctDNA samples and 23 matched tumor biopsies. The frequency of genomic alterations were compared with the Stand Up to Cancer-Prostate Cancer Foundation (SU2C-PCF) cohort. The Kaplan-Meier method was used to evaluate progression-free survival (PFS) following standard systemic treatments for mCRPC. Cox regression analyses were performed to determine prognostic factors associated with PFS resulting from treatments for mCRPC.
RESULTS
In total, 33 of 36 (91.7%) mutations were found consistently between ctDNA and paired biopsy samples. The most common recurrent genomic alterations were found in AR (34.6%), TP53 (19.5%), CDK12 (15.4%), BRCA2 (13%), and RB1 (5.8%). The frequency of CDK12 alterations (15.4%) in our cohort was significantly higher than that in Western populations (5%-7%). AR amplification and TP53 and/or RB1 alterations were associated with resistance to abiraterone or docetaxel. Patients with a CDK12 defect showed rapid disease progression after abiraterone treatment. However, the clinical outcome after docetaxel treatment was similar between patients with and without CDK12 defects. In multivariate Cox regression analysis, a CDK12 defect was significantly associated with inferior PFS after abiraterone treatment. Patients with a BRCA2 defect showed marked response to both PARP inhibitors and platinum-based chemotherapy.
CONCLUSIONS
Our study explored the genomic landscape of Chinese patients with mCRPC at different treatment stages using minimally invasive methods and evaluated the clinical implications of the driver genomic alterations on patients' response to the most widely used therapies for mCRPC. We observed a significantly higher alteration frequency of CDK12 in our cohort compared with the SU2C-PCF cohort.
背景
本研究旨在利用循环肿瘤(ctDNA)测序描述中国转移性去势抵抗性前列腺癌(mCRPC)患者DNA损伤修复基因及其他重要驱动基因的畸变情况,并评估多种治疗的临床结局与mCRPC关键基因组改变之间的关联,尤其是DNA损伤修复基因。
患者与方法
共纳入来自8个中心的292例中国mCRPC患者。对30⑥份ctDNA样本和23份匹配的肿瘤活检组织进行多基因靶向测序。将基因组改变的频率与“勇敢对抗癌症 - 前列腺癌基金会”(SU2C - PCF)队列进行比较。采用Kaplan - Meier法评估mCRPC标准全身治疗后的无进展生存期(PFS)。进行Cox回归分析以确定与mCRPC治疗所致PFS相关的预后因素。
结果
总体而言,36个突变中有33个(91.7%)在ctDNA和配对活检样本中一致被发现。最常见的复发性基因组改变见于AR(34.6%)、TP53(19.5%)、CDK12(15.4%)、BRCA2(13%)和RB1(5.8%)。我们队列中CDK12改变的频率(15.4%)显著高于西方人群(5% - 7%)。AR扩增以及TP53和/或RB1改变与阿比特龙或多西他赛耐药相关。CDK12缺陷的患者在阿比特龙治疗后疾病进展迅速。然而,多西他赛治疗后,有无CDK12缺陷的患者临床结局相似。在多变量Cox回归分析中,CDK12缺陷与阿比特龙治疗后较差的PFS显著相关。BRCA2缺陷的患者对PARP抑制剂和铂类化疗均有显著反应。
结论
我们的研究采用微创方法探索了不同治疗阶段中国mCRPC患者的基因组格局,并评估了驱动基因组改变对患者对mCRPC最广泛使用治疗反应的临床意义。与SU2C - PCF队列相比,我们队列中CDK12的改变频率显著更高。
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