台湾国民健康保险报销后,镭-223 治疗转移性耐阉割前列腺癌的生存结果。

Shan-Fan Yao, William J Huang, Tzu-Chun Wei, Yuh-Feng Wang, Ko-Han Lin, Lien-Hsin Hu, Chien-Hsin Ting, Tse-Hao Lee, Skye Hsin-Hsien Yeh, Nan-Jing Peng
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引用次数: 0

摘要

背景:二氯化镭-223(Ra-223)可延长有症状骨转移的转移性抗性前列腺癌(mCRPC)的总生存期(OS)。然而,个体之间的结果差异很大。我们的目的是评估台湾地区国民健康保险(NHI)报销Ra-223疗法后与患者生存相关的预后决定因素:方法:我们对在台北荣民总医院接受Ra-223治疗的mCRPC患者进行了回顾性登记。每次静脉注射 Ra-223 的剂量为 55 kBq/kg,间隔四周。临床结果来自医疗记录;评估了潜在的生存预后因素。采用 Kaplan-Meier 分析法生成累积生存曲线;采用卡方检验法评估组间差异。统计显著性以 p < 0.05 为标准:76名患者接受了Ra-223治疗;62名患者获得了国家医疗保险报销,其余患者自费。50名患者(65.8%)完成了6个周期的治疗;26名患者(34.2%)接受了1-5个周期的治疗。47 名患者死亡。与存活率明显相关的因素包括:≦五个骨转移灶(p = 0.0018)、基线前列腺特异性抗原(PSA)≦ 36 ng/mL(p = 0.0004)、基线碱性磷酸酶(ALP)< 115 U/L(p = 0.0007)和基线血红蛋白(Hb)> 12 g/dL(p = 0.0029)。与未完成治疗的患者相比,完成六个周期治疗的患者的OS明显更高(p < 0.0001)。自报销开始以来,患者人数增加了4.4倍;获得国家健康保险报销的患者与自费患者的OS无明显差异:结论:Ra-223的施用在延长mCRPC患者的生存期方面具有相当大的潜力。结论:Ra-223的应用显示出延长mCRPC患者生存期的巨大潜力。生存期结果可能会受到各种预后因素的影响。然而,在台湾,通过国民健康保险制度报销Ra-223治疗mCRPC的费用后,观察到OS没有明显差异。
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Survival outcomes of radium-223 therapy for metastatic castration-resistant prostate cancer following national health insurance reimbursement in Taiwan.

Background: Radium-223 dichloride (Ra-223) prolongs overall survival (OS) in metastatic castration-resistant prostate cancer (mCRPC) with symptomatic bone metastases. However, there is considerable variation in outcomes among individuals. We aimed to evaluate the prognostic determinants associated with patient survival following National Health Insurance (NHI) reimbursement for Ra-223 therapy in Taiwan.

Methods: Patients with mCRPC who underwent Ra-223 treatment at Taipei Veterans General Hospital were retrospectively enrolled. Each intravenous Ra-223 dose was administered at 55 kBq/kg at 4-week intervals. Clinical outcomes were obtained from medical records; potential prognostic factors for survival were assessed. Kaplan-Meier analysis was used to generate cumulative survival curves; between-group differences were evaluated using the Chi-squared test. Statistical significance was set at p < 0.05.

Results: Seventy-six patients underwent Ra-223 therapy; 62 patients received NHI reimbursement and the remainder self-paid. Fifty patients (65.8%) completed six cycles of treatment; 26 (34.2%) received 1 to 5 cycles. Mortality occurred in 47 patients. Factors significantly associated with survival included ≤five bone metastases ( p = 0.0018), baseline prostate-specific antigen (PSA) ≤36 ng/mL ( p = 0.0004), baseline alkaline phosphate (ALP) <115 U/L ( p = 0.0007), and baseline hemoglobin (Hb) >12 g/dL ( p = 0.0029). Patients who completed six cycles of treatment achieved significantly higher OS compared to those who did not ( p < 0.0001). There has been a 4.4-fold increase in the number of patients since reimbursement began; there was no significant difference in OS between patients who received NHI reimbursement and those who self-paid.

Conclusion: Administration of Ra-223 demonstrates considerable potential to extend the survival of patients with mCRPC. Survival outcomes may be influenced by various prognostic factors. However, no significant difference in OS was observed subsequent to reimbursement of Ra-223 therapy for mCRPC through the NHI system in Taiwan.

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