Homologous Recombination Repair Testing Patterns and Outcomes in mCRPC by Alteration Status and Race.

IF 2.1 Q3 HEALTH CARE SCIENCES & SERVICES

ClinicoEconomics and Outcomes Research Pub Date : 2024-09-06 eCollection Date: 2024-01-01 DOI:10.2147/CEOR.S468680

Mehmet Asim Bilen, Ibrahim Khilfeh, Carmine Rossi, Erik Muser, Laura Morrison, Annalise Hilts, Lilian Diaz, Patrick Lefebvre, Dominic Pilon, Daniel J George

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Abstract

Background: Alterations in DNA damage repair genes in advanced prostate cancer (PC) may impact responses to therapy and clinical outcomes. This study described homologous recombination repair (HRR) testing patterns and clinical outcomes among patients with metastatic castration-resistant prostate cancer (mCRPC) by HRR alteration status and race in the United States (US).

Methods: Clinical data in the nationwide (US-based) Flatiron Health-Foundation Medicine, Inc. (FMI) Metastatic PC Clinico-Genomic Database were evaluated (01/01/2011-12/31/2022). Patients initiating first-line (1L) mCRPC therapy on or after mCRPC diagnosis were included. Testing patterns, time-to-next treatment, overall survival (OS), and time-to-prostate specific antigen response were described.

Results: Of the 1367 patients with mCRPC and at least one HRR panel test prior to or on the date of 1L mCRPC therapy initiation, 332 (24.3%) were HRR positive (White patients: n = 219 [66.0%]; Black patients: n = 37 [11.1%]) and 1035 (75.7%) were HRR negative (White patients: n = 702 [67.8%]; Black patients: n = 84 [8.1%]). The mean time between first positive test and 1L mCRPC therapy initiation date was 588 days (White patients: 589 days; Black patients: 639 days). Among HRR positive relative to negative patients, trends for faster progression (respective 12-month rate overall: 71.1% and 63.7%; White patients: 72.5% and 64.0%; Black patients: 65.4% and 56.4%), shorter OS (respective 24-month rate overall: 46.8% and 51.9%; White patients: 48.6% and 46.2%; Black patients: 52.8% and 54.1%), and decreased treatment response (respective 12-month rate overall: 24.3% and 37.9%; White patients: 24.5% and 35.2%; Black patients: 17.0% and 43.9%) were observed.

Conclusion: Patients with mCRPC positive for HRR alterations tended to exhibit poorer treatment responses and clinical outcomes than those with a negative status. These findings highlight the importance of timely genetic testing in mCRPC, particularly among Black patients, and the need for improved 1L targeted therapies to address the unmet need in HRR positive mCRPC.

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按基因变异状态和种族划分的同源重组修复测试模式和 mCRPC 的治疗结果。

背景：晚期前列腺癌（PC）DNA损伤修复基因的改变可能会影响治疗反应和临床预后。本研究描述了美国（US）转移性去势抵抗性前列腺癌（mCRPC）患者的同源重组修复（HRR）检测模式和临床结果，并按HRR改变状态和种族进行了分类：评估了全国（美国）Flatiron Health-Foundation Medicine, Inc.（FMI）转移性前列腺癌临床基因组数据库中的临床数据（01/01/2011-12/31/2022）。纳入了在确诊 mCRPC 时或确诊后开始接受一线 (1L) mCRPC 治疗的患者。对检测模式、下次治疗时间、总生存期（OS）和前列腺特异性抗原反应时间进行了描述：在1367名mCRPC患者中，有332人（24.3%）在开始1L mCRPC治疗前或开始1L mCRPC治疗当日进行了至少一次HRR面板检测，其中332人（24.3%）为HRR阳性（白人患者：n = 219 [66.0%]；黑人患者：n = 37 [11.1%]），1035人（75.7%）为HRR阴性（白人患者：n = 702 [67.8%]；黑人患者：n = 84 [8.1%]）。从首次检测呈阳性到开始 1L mCRPC 治疗的平均时间为 588 天（白人患者：589 天；黑人患者：639 天）。相对于阴性患者，HRR阳性患者的病情发展速度有加快的趋势（12个月的总比率分别为71.1%和63.7%；白人患者分别为72.5%和64.0%）：白人患者：72.5% 和 64.0%；黑人患者：65.4% 和 56.4%：65.4% 和 56.4%）、较短的 OS（24 个月的总体比率分别为：46.8% 和 51.9%；白人患者：48.6% 和 46.2%；黑人患者：48.6% 和 46.2%）：白人患者：48.6% 和 46.2%；黑人患者：52.8% 和 54.1%）：52.8%和54.1%），治疗反应降低（12个月总反应率分别为：24.3%和37.9%；白人患者：24.5%和35.2%；黑人患者：24.5%和35.2%）：白人患者：24.5%和 35.2%；黑人患者：17.0%和 43.9%：结论结论：与阴性患者相比，HRR改变阳性的mCRPC患者的治疗反应和临床预后往往较差。这些发现强调了及时进行mCRPC基因检测的重要性，尤其是在黑人患者中，同时也强调了改进1L靶向疗法的必要性，以满足HRR阳性mCRPC患者尚未得到满足的需求。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

ClinicoEconomics and Outcomes Research HEALTH CARE SCIENCES & SERVICES-

CiteScore

3.70

自引率

0.00%

发文量

审稿时长

16 weeks