在接受雄激素受体靶向药物治疗的晚期前列腺癌男性中,Sipuleucel-T 对总生存的真实世界疗效。
Real-World Effectiveness of Sipuleucel-T on Overall Survival in Men with Advanced Prostate Cancer Treated with Androgen Receptor-Targeting Agents.
机构信息
William Beaumont School of Medicine, Oakland University, Auburn Hills, MI, USA.
, 130 Town Center Drive, Troy, MI, 48084, USA.
出版信息
Adv Ther. 2022 Jun;39(6):2515-2532. doi: 10.1007/s12325-022-02085-6. Epub 2022 Mar 30.
INTRODUCTION
The treatment landscape for metastatic castration-resistant prostate cancer (mCRPC) continues to evolve. Sipuleucel-T was the first immunotherapy approved by the US Food and Drug Administration (FDA) to treat asymptomatic or minimally symptomatic mCRPC. The androgen receptor-targeting agents (ARTAs) abiraterone acetate and enzalutamide were initially approved to treat mCRPC. Looking at chemotherapy-naïve men with mCRPC, we compared survival outcomes between the sipuleucel-T + ARTA cohort (men who received either sipuleucel-T or an ARTA in the first line, and then the other in the second line within 6 months) and the ARTA monotherapy cohort (men who only received ARTA monotherapy).
METHODS
This retrospective cohort analysis used longitudinal, adjudicated claims data from the US Medicare Fee-for-Service 100% research identifiable dataset that includes both urologic and oncologic practice settings. Eligible men started their first mCRPC treatment with either sipuleucel-T or ARTA in either 2014 or 2015 and had continuous Medicare Parts A, B, and D eligibility for the subsequent 3 years. A multivariable Cox proportional hazards regression model was used to analyze overall survival (OS), both overall and by index year, and to control for differences.
RESULTS
The sipuleucel-T + ARTA and ARTA monotherapy cohorts comprised 773 and 4642 men, respectively, with different characteristics at treatment start. The most commonly used ARTAs were enzalutamide in the former and abiraterone in the latter cohort. Median OS was 30.4 and 14.3 months in the sipuleucel-T + ARTA and ARTA monotherapy cohorts, respectively, with the sipuleucel-T + ARTA cohort having a 28.3% lower risk of death than the ARTA monotherapy cohort (hazard ratio 0.717; 95% CI 0.648, 0.793; p < 0.01).
CONCLUSIONS
This real-world study of mCRPC treatment indicates that men receiving sipuleucel-T and ARTAs had a longer median OS than patients receiving treatment with an ARTA alone, suggesting that leveraging mechanisms of action can be beneficial in treating patients with mCRPC.
简介
转移性去势抵抗性前列腺癌(mCRPC)的治疗领域仍在不断发展。Sipuleucel-T 是首个获得美国食品和药物管理局(FDA)批准用于治疗无症状或轻度症状 mCRPC 的免疫疗法。雄激素受体靶向药物(ARTAs)醋酸阿比特龙和恩扎鲁胺最初被批准用于治疗 mCRPC。在化疗初治的 mCRPC 男性中,我们比较了 sipuleucel-T+ARTA 队列(接受 sipuleucel-T 或 ARTA 一线治疗,然后在 6 个月内二线使用另一种药物的男性)和 ARTA 单药治疗队列(仅接受 ARTA 单药治疗的男性)的生存结局。
方法
这项回顾性队列分析使用了来自美国医疗保险全服务 100%可识别数据集的纵向、裁定索赔数据,该数据集包括泌尿科和肿瘤科的实践环境。符合条件的男性在 2014 年或 2015 年开始接受 sipuleucel-T 或 ARTA 的首次 mCRPC 治疗,并且在随后的 3 年内连续有医疗保险 A、B 和 D 部分的资格。多变量 Cox 比例风险回归模型用于分析总生存期(OS),包括总体和按索引年度,并进行差异控制。
结果
sipuleucel-T+ARTA 和 ARTA 单药治疗队列分别包含 773 名和 4642 名男性,他们在治疗开始时具有不同的特征。最常用的 ARTA 在前一队列中是恩扎鲁胺,在后一队列中是阿比特龙。sipuleucel-T+ARTA 和 ARTA 单药治疗队列的中位 OS 分别为 30.4 个月和 14.3 个月,sipuleucel-T+ARTA 队列的死亡风险比 ARTA 单药治疗队列低 28.3%(风险比 0.717;95%CI 0.648,0.793;p<0.01)。
结论
这项 mCRPC 治疗的真实世界研究表明,接受 sipuleucel-T 和 ARTA 治疗的男性的中位 OS 长于接受单独 ARTA 治疗的患者,这表明利用作用机制可能有益于治疗 mCRPC 患者。
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