使用 PARP 抑制剂治疗转移性乳腺癌患者的处方模式和临床结果的真实世界证据:梅奥诊所的经验。

IF 2.9 3区 医学 Q2 ONCOLOGY Clinical breast cancer Pub Date : 2024-10-17 DOI:10.1016/j.clbc.2024.10.006
Nusrat Jahan, Jodi Taraba, Nicholas J Boddicker, Karthik V Giridhar, Roberto A Leon-Ferre, Amye J Tevaarwerk, Elizabeth Cathcart-Rake, Ciara C O'Sullivan, Prema P Peethambaram, Timothy J Hobday, Lida A Mina, Felipe Batalini, Pooja Advani, Kostandinos Sideras, Tufia C Haddad, Kathryn J Ruddy, Matthew P Goetz, Fergus J Couch, Siddhartha Yadav
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引用次数: 0

摘要

目的:本研究评估了PARP抑制剂(PARPis)治疗转移性乳腺癌(MBC)的真实世界结果、毒性和处方模式:分析了梅奥诊所系统在2017年至2022年期间接受奥拉帕利(n = 48)或他拉唑帕利(talazoparib)治疗的62名MBC患者的电子健康记录。采用卡普兰-梅耶法评估了治疗失败时间(TTF)。在调整相关肿瘤和人口统计学特征的多变量考克斯比例危险回归模型中确定了TTF的预测因素:结果:在62例接受PARPis治疗的MBC患者中,55例患者存在种系(g)致病变异(PVs)(gBRCA1 = 24、gBRCA2 = 26和gPALB2 = 4),8例患者存在体细胞(s)致病变异(sBRCA1 = 4、sBRCA2 = 2、sATM = 1和sCDKN2A = 1)。gBRCA1、gBRCA2和gPALB2 PV携带者的中位TTF分别为7、8和9个月(P = .37)。在 51.8% 的 gBRCA 或 gPALB2 PV 患者中观察到了完全或部分反应。在多变量分析中,HER2 阳性(危险比,HR:4.9,P = .007)和除 BRCA(sATM 或 sCDKN2A)以外的同源重组修复 (HRR) 基因中的体细胞 PV(HR:11.7,P = .01)与较短的 TTF 相关。根据 PARPi 的类型、雌激素和孕激素受体状态、年龄或既往治疗次数,TTF 没有明显差异。8名(16.7%)接受奥拉帕利治疗的患者和7名(50%)接受塔拉唑帕利治疗的患者因毒性反应而需要减少剂量:在实际应用中,PARPis在gBRCA1/2和gPALB2携带者中耐受性良好,TTF前景看好。进一步的研究将明确 PARPis 在其他 MBC 亚群中的临床疗效,如 sBRCA 突变、HER2 阳性疾病和中枢神经系统转移。
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Real-World Evidence on Prescribing Patterns and Clinical Outcomes of Metastatic Breast Cancer Patients Treated with PARP Inhibitors: The Mayo Clinic Experience.

Purpose: This study evaluates real-world outcomes, toxicities, and prescribing patterns of PARP inhibitors (PARPis) for the treatment of metastatic breast cancer (MBC).

Patients and methods: Electronic health records of 62 MBC patients treated with olaparib (n = 48) or talazoparib (n = 14) at Mayo Clinic System between 2017 and 2022 were analyzed. Time-to-treatment-failure (TTF) was assessed utilizing the Kaplan-Meier method. Predictors of TTF were identified in a multivariate Cox-proportional hazard regression model adjusting for relevant tumor and demographic characteristics.

Results: Among 62 patients who received PARPis for MBC, 55 had germline (g) pathogenic variants (PVs) (gBRCA1 = 24, gBRCA2 = 26, and gPALB2 = 4) and 8 patients had somatic (s) PVs (sBRCA1 = 4, sBRCA2 = 2, sATM = 1, sCDKN2A = 1). Median TTF in the gBRCA1, gBRCA2, and gPALB2 PV carriers were 7, 8, and 9 months, respectively (P = .37). Complete or partial responses were observed among 51.8% of patients with gBRCA or gPALB2 PVs. In multivariate analysis, HER2 positivity (hazard ratio, HR: 4.9, P = .007) and somatic PVs in homologous recombination repair (HRR) genes other than BRCA (sATM or sCDKN2A) (HR: 11.7, P = .01) were associated with a shorter TTF. No significant difference in TTF was observed by the type of PARPi, estrogen and progesterone receptor status, age, or number of prior therapies. Eight (16.7%) patients receiving olaparib and seven (50%) receiving talazoparib required dose reductions due to toxicities.

Conclusions: In real-world practice, PARPis are well-tolerated with promising TTF in gBRCA1/2 and gPALB2 carriers. Further studies will delineate the clinical efficacy of PARPis in other MBC subsets, such as sBRCA mutations, HER2-positive disease, and CNS metastasis.

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来源期刊
Clinical breast cancer
Clinical breast cancer 医学-肿瘤学
CiteScore
5.40
自引率
3.20%
发文量
174
审稿时长
48 days
期刊介绍: Clinical Breast Cancer is a peer-reviewed bimonthly journal that publishes original articles describing various aspects of clinical and translational research of breast cancer. Clinical Breast Cancer is devoted to articles on detection, diagnosis, prevention, and treatment of breast cancer. The main emphasis is on recent scientific developments in all areas related to breast cancer. Specific areas of interest include clinical research reports from various therapeutic modalities, cancer genetics, drug sensitivity and resistance, novel imaging, tumor genomics, biomarkers, and chemoprevention strategies.
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