Impact of timing of radium‑223 administration on the survival of patients with bone metastatic castration‑resistant prostate cancer.

Kenji Makita, Yasushi Hamamoto, Hiromitsu Kanzaki, Natsumi Yamashita, Kei Nagasaki, Teruhito Kido, Noriyoshi Miura, Takashi Saika, Katsuyoshi Hashine
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Abstract

The present study aimed to evaluate the optimal timing of radium-223 chloride (Ra-223) administration among patients with bone metastasis from castration-resistant prostate cancer (BmCRPC). Patients, who were diagnosed with BmCRPC and treated with Ra-223 therapy between October, 2016 and January, 2022, were reviewed. The survival time was calculated from the initiation of Ra-223 administration. The time from the diagnosis of BmCRPC to the initiation of Ra-223 administration was identified as a potential prognostic factor. A total of 51 patients were examined in the present study. Ra-223 was administered as the first- and second-line therapy (earlier Ra-223 administration) in 32 patients and as the third- to fifth-line therapy (later Ra-223 administration) in 19 patients. In the multivariate analysis, which considered the potential prognosis, the difference in survival times between patients who received early and late Ra-223 administration was not significant [hazard ratio (HR), 2.67; 95% confidence interval (CI), 0.79-9.07; P=0.11]. By contrast, an incomplete Ra-223 administration (HR, 128.03; 95% CI, 10.59-1548.42; P<0.01) and higher levels of prostate-specific antigen prior to Ra-223 administration (HR, 7.86; 95% CI, 2.7-27.24; P<0.01) were independent factors, significantly associated with a poorer prognosis. The timing of Ra-223 administration did not significantly affect the survival of patients from the initiation of treatment. Further studies are thus required to determine the optimal timing for Ra-223 administration.

Abstract Image

镭- 223给药时间对骨转移性去势抵抗性前列腺癌患者生存的影响
本研究旨在评价去势抵抗性前列腺癌(BmCRPC)骨转移患者给药镭-223氯(Ra-223)的最佳时机。本研究回顾了2016年10月至2022年1月期间诊断为BmCRPC并接受Ra-223治疗的患者。生存时间从Ra-223给药开始计算。从诊断为BmCRPC到开始给药Ra-223的时间被认为是一个潜在的预后因素。本研究共对51例患者进行了检查。在32例患者中,Ra-223作为一线和二线治疗(早期给药Ra-223),在19例患者中作为三线至五线治疗(后期给药Ra-223)。在考虑潜在预后的多因素分析中,早期和晚期给药Ra-223患者的生存时间差异不显著[危险比(HR), 2.67;95%置信区间(CI), 0.79-9.07;P = 0.11)。相反,Ra-223给药不完全(HR, 128.03;95% ci, 10.59-1548.42;P
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