曾接受多西他赛强化治疗的转移性钙化敏感性前列腺癌患者首次接受后续紫杉类药物治疗的结果

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS
Gabrielle Robin, Naveen S. Basappa, Scott North, Sunita Ghosh, Michael Kolinsky
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引用次数: 0

摘要

背景:晚期前列腺癌的治疗方法仍在迅速发展,尤其是在转移性阉割敏感性前列腺癌(mCSPC)中较早使用了延长生存期的疗法。尽管在mCSPC使用强化疗法之前就已获批,但基于类固醇的化疗仍是转移性耐受性前列腺癌(mCRPC)患者的相关选择。然而,对于在mCSPC中接受过多西他赛强化治疗(DI)的mCRPC患者来说,几乎没有证据可以确定以类固醇化疗作为首次后续类固醇治疗(FST)的疗效。本研究旨在比较多西他赛和卡巴他赛这两种延长生存期的类固醇化疗药作为多西他赛强化治疗后的首个后续类固醇化疗的疗效。研究方法回顾性审查2014年7月1日至2020年12月31日在克罗斯癌症研究所就诊的新患者。如果患者接受了mCSPC的DI治疗,然后又接受了多西他赛或卡巴齐他赛治疗mCRPC,则被认为符合条件。相关变量均来自电子病历。主要终点是12周时FST相对于基线的PSA反应≥50%。次要终点包括自确诊 mCSPC 起的 OS,以及自 FST 开始之日起的 PFS 和 OS。PSA 反应采用卡方检验进行比较,基于时间的终点采用卡普兰-梅耶法进行比较。结果共有 34 名患者被确定为 FST 患者:多西他赛 = 22 名,卡巴齐他赛 = 12 名。91.2%的患者(多西他赛95.5%,卡巴齐他赛83.3%)在二线mCRPC中接受了FST治疗。多西他赛和卡巴他赛的中位诊断年龄(63.1岁 vs. 67.1岁,p = 0.236)和中位CRPC时间(18.6个月 vs. 14.2个月,p = 0.079)分别相似。与多西他赛相比,接受卡巴他赛治疗的患者的FST中位时间(24.1天 vs. 34.6天,p = 0.036)和mCSPC诊断后的OS(30.9天 vs. 52.7天,p = 0.002)明显更短。接受多西他赛治疗的患者中40.9%出现PSA反应,而接受卡巴他赛治疗的患者中25.0%出现PSA反应(p = 0.645)。接受多西他赛治疗的患者与接受卡巴齐他赛治疗的患者从FST开始的中位PFS(2.7个月 vs. 3.5个月,p = 0.727)或中位OS(11.4个月 vs. 8.1个月,p = 0.132)没有明显差异。结论多西他赛和卡巴齐他赛在mCSPC DI后的FST中均显示出活性。接受卡巴齐他赛治疗的患者从mCSPC到FST和OS的时间更短。其原因可能是临床医生倾向于在病情恶化或进展迅速的患者中使用卡巴他赛。与卡巴齐他赛相比,多西他赛的PSA反应、PFS或FST后的OS均无差异。虽然这项研究具有回顾性和样本量小的局限性,但它表明,在mCSPC中,多西他赛作为FST具有活性,尽管使用DI治疗。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Outcomes of First Subsequent Taxane Therapy in Patients with Metastatic Castration-Resistant Prostate Cancer Who Previously Received Docetaxel Intensification for Metastatic Castration-Sensitive Prostate Cancer
Background: The management of advanced prostate cancer continues to evolve rapidly, particularly with the earlier use of survival-prolonging therapies in metastatic castration-sensitive prostate cancer (mCSPC). Though approved prior to the use of intensification therapy in mCSPC, taxane-based chemotherapies remain a relevant option for patients with metastatic castration-resistant prostate cancer (mCRPC). However, there is little evidence determining the outcomes of taxane chemotherapies as the first subsequent taxane (FST) in mCRPC pts who received docetaxel intensification (DI) in mCSPC. The purpose of this study is to compare outcomes between the survival-prolonging taxanes, docetaxel and cabazitaxel as FST after DI. Methods: New patient consults seen at the Cross Cancer Institute from 1 July 2014 to 31 December 2020 were retrospectively reviewed. Pts were considered eligible if they received DI for mCSPC and then received either docetaxel or cabazitaxel in mCRPC. Variables of interest were collected from electronic medical records. The primary endpoint was ≥50% PSA response at 12 weeks relative to baseline for FST. Secondary endpoints included OS from mCSPC diagnosis, as well as PFS and OS from the FST start date. PSA responses were compared using the chi-squared test, and time-based endpoints were compared using the Kaplan–Meier method. Results: In total, 34 pts were identified: docetaxel = 22 and cabazitaxel = 12 as FST. 91.2% of pts (docetaxel 95.5% vs. cabazitaxel 83.3%) received FST in 2nd line mCRPC. The median age at diagnosis (63.1 vs. 67.1 yrs, p = 0.236) and the median time to CRPC (18.6 vs. 14.2 mos, p = 0.079) were similar for docetaxel and cabazitaxel, respectively. The median time to FST (24.1 vs. 34.6 mos, p = 0.036) and OS from mCSPC diagnosis (30.9 vs. 52.7 mos, p = 0.002) were significantly shorter for pts receiving cabazitaxel vs. docetaxel. PSA responses occurred in 40.9% of pts treated with docetaxel compared to 25.0% treated with cabazitaxel (p = 0.645). There was no significant difference in median PFS (2.7 vs. 3.5 mos, p = 0.727) or median OS (11.4 vs. 8.1 mos, p = 0.132) from the time of FST for pts treated with docetaxel vs. cabazitaxel, respectively. Conclusions: Both docetaxel and cabazitaxel demonstrated activity as FST after DI in mCSPC. Pts who received cabazitaxel had a shorter time to FST and OS from mCSPC. The reasons for this may reflect clinician preference for cabazitaxel in pts with aggressive or rapidly progressing disease. No difference was found in PSA response, PFS, or OS from FST with docetaxel compared to cabazitaxel. While limited by its retrospective nature and small sample size, this study suggests that docetaxel is active as FST despite treatment with DI in mCSPC.
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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