[Therapy sequences and duration in mCRPC: a retrospective review of the Lübeck mCRPC cohort].

IF 0.3 4区 医学 Q4 UROLOGY & NEPHROLOGY Aktuelle Urologie Pub Date : 2025-02-01 Epub Date: 2024-06-25 DOI:10.1055/a-2295-8720
Marten Müller, Semih Sarcan, Anne Offermann, Duan Kang, Judith Riccarda Wießmeyer, Mario Kramer, Axel S Merseburger, Marie Christine Roesch
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引用次数: 0

Abstract

Background: Prostate cancer is one of the most common cancers in men in Europe. Several classes of agents can be considered for the treatment of metastatic prostate carcinoma, and their use is supported by extensive guidelines. In the treatment of metastatic castration-resistant prostate cancer (mCRPC), it is currently unclear which sequence of systemic therapies is most effective. Currently approved system therapies in the castration-resistant setting generally include hormone-manipulating agents, taxane-based chemotherapies, radioactive agents, or inhibitiors of DNA repair mechanisms. This study aims to summarize real world data of mCRPC therapy.

Methods: Retrospectively, 90 mCRPC patients undergoing treatment at the University Hospital Schleswig-Holstein, Lübeck Campus between February 2006 and March 2020 were identified. The patient data were analyzed for their treatment sequence and disease progression. Due to the inclusion period, the mCRPC therapy sequences studied were limited to: Abiraterone, Cabazitaxel, Docetaxel, Enzalutamide, Lutetium-177-PSMA and Radium-223. The analysis includes the therapy sequences and their duration, clinical information of the respective cohort, overall and cancer-specific survival (OS/CSS) as well as time to second-line therapy in relation to the respective first-line therapy.

Results: Approximately two-thirds of patients underwent a true therapy sequence (at least two of the drugs listed above), with this proportion halving by the third line.The majority of patients received the sequence (first/second line) abiraterone/docetaxel (n=13), followed by docetaxel/abiraterone (n=12) and abiraterone/enzalutamid (n=10) and docetaxel/docetaxel (n=8).Within the different docetaxel sequences, first-line (mean 4.7 months ± SD 3.1; median 4.0) and rechallenge (mean 5.3 months ± SD 5.9; median 3.0) therapy durations were the longest. The subjective side effect rate of docetaxel was lower in the second line, so that a better tolerability can be assumed here.The abiraterone/docetaxel sequence was used mainly in patients with metachronous metastases. Among the different sequences of abiraterone, first-line (mean 10.8 months ± SD 10.2; median 9.0) and second-line (mean 10.6 months ± SD 9.0; median 7.0) therapy durations were the longest.The sequence abiraterone/enzalutamide was prescribed mainly to older patients with synchronous metastases. Among the different enzalutamide sequences first-line (mean 9.6 months ± SD 7.1; median 7.0) and rechallenge (mean 11.0 ± SD 0.0; median 11.0) therapy durations were the longest.In contrast, the sequence docetaxel/docetaxel was used mainly in younger patients with a high initial PSA.The evaluation shows a trend that both abiraterone and enzalutamide can account for a survival advantage in the first line.

Conclusion: Ultimately, an optimal treatment sequence cannot be confidently derived from these data.However, it was found that only a small proportion of patients underwent fourth- or even fifth-line treatment at all. Thus, the focus on first- and second-line in this study seems reasonable. It could be shown in a trend that docetaxel as first-line therapy seems to be disadvantegous regarding OS as well as CSS when compared to abiraterone or enzalutamide. However, due to the small number of patients in this study, a clear significance cannot be derived. Moreover, the subjectively better tolerability of docetaxel in the second-line setting could provide an impetus for treatment planning in multimorbid elderly patients in the future. The sequence abiraterone/docetaxel may offer a beneficial option for initial mCRPC therapy.

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[mCRPC的治疗顺序和持续时间:吕贝克mCRPC队列回顾]。
背景:前列腺癌是欧洲最常见的男性癌症之一:前列腺癌是欧洲男性最常见的癌症之一。在治疗转移性前列腺癌时可考虑使用几类药物,这些药物的使用得到了广泛指南的支持。在治疗转移性去势抵抗性前列腺癌(mCRPC)时,目前还不清楚哪种系统疗法最有效。目前获准用于耐受性前列腺癌的系统疗法一般包括激素调节剂、以类固醇为基础的化疗、放射性药物或 DNA 修复机制抑制剂。本研究旨在总结 mCRPC 治疗的实际数据:方法:回顾性分析 2006 年 2 月至 2020 年 3 月期间在石勒苏益格-荷尔斯泰因大学医院吕贝克院区接受治疗的 90 名 mCRPC 患者。对患者的治疗顺序和疾病进展情况进行了分析。由于纳入时间有限,所研究的 mCRPC 治疗顺序仅限于以下几种:阿比特龙、卡巴齐他赛、多西他赛、恩扎鲁胺、Lutetium-177-PSMA 和镭-223。分析内容包括治疗序列及其持续时间、各组群的临床信息、总生存率和癌症特异性生存率(OS/CSS)以及与各一线治疗相关的二线治疗时间:大多数患者接受了阿比特龙/多西他赛(13人)、多西他赛/阿比特龙(12人)、阿比特龙/苯扎鲁胺(10人)和多西他赛/多西他赛(8人)的治疗顺序(一线/二线)。在不同的多西他赛序列中,一线(平均4.7个月±标准差3.1;中位数4.0)和再挑战(平均5.3个月±标准差5.9;中位数3.0)治疗持续时间最长。多西他赛的主观副作用发生率在二线治疗中较低,因此可以认为其耐受性较好。阿比特龙/多西他赛序列主要用于有远处转移的患者。在阿比特龙的不同序列中,一线(平均10.8个月±标准差10.2;中位数9.0)和二线(平均10.6个月±标准差9.0;中位数7.0)治疗持续时间最长。在不同的恩杂鲁胺序列中,一线(平均9.6个月±标准差7.1;中位数7.0)和再次复查(平均11.0个月±标准差0.0;中位数11.0)治疗持续时间最长:但研究发现,只有一小部分患者接受了四线甚至五线治疗。因此,本研究将重点放在一线和二线治疗上似乎是合理的。有趋势表明,与阿比特龙或恩杂鲁胺相比,多西他赛作为一线疗法似乎在OS和CSS方面处于劣势。不过,由于这项研究的患者人数较少,因此无法得出明确的意义。此外,多西他赛在二线治疗中的主观耐受性更好,这可能会为今后多病老年患者的治疗计划提供动力。阿比特龙/多西他赛序列可能会为mCRPC的初始治疗提供一个有益的选择。
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来源期刊
Aktuelle Urologie
Aktuelle Urologie 医学-泌尿学与肾脏学
CiteScore
0.60
自引率
33.30%
发文量
104
审稿时长
>12 weeks
期刊介绍: Die entscheidenden Ergebnisse der internationalen Forschung – für Sie auf den Punkt zusammengefasst und kritisch kommentiert Übersichtsarbeiten zu den maßgeblichen Themen der täglichen Praxis Auf dem Laufenden über die klinische Forschung durch interessante Originalien CME-Punkte sammeln mit der Rubrik "Operative Techniken" In jeder Ausgabe: Techniken wichtiger Standard-OPs – Schritt für Schritt Erstklassige OP-Skizzen mit verständlichen Erläuterungen
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