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Palliative effects and adverse events of strontium-89 for prostate cancer patients with bone metastasis

机译:锶89对前列腺癌骨转移患者的姑息作用和不良事件

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摘要

The aim of the present study was to evaluate the palliative effects and adverse events of strontium-89 (Sr-89) in patients with bone metastasis from prostate cancer. A total of 18 patients with prostate cancer and painful bone metastases, as diagnosed on bone scintigraphy, who were treated with Sr-89 at the National Kyushu Cancer Center between February, 2008 and April, 2014 were reviewed. Of the 18 subjects, 13 (72.2%) achieved a pain response, whereas 5 were classified as pain non-responders (27.8%). According to a logistic regression analysis, the pre-administration characteristics, including age, prostate-specific antigen (PSA), alkaline phosphatase (ALP), history of bone-modifying agent administration, opioid use or palliative radiation therapy, time after the combined androgen blockade nadir and time since the pain onset, were not found to be significant predictors of the pain response. Similarly, the post-administration characteristics, including pain flares and the PSA and ALP response, were not found to be significant predictors of the pain response. Although no patients exhibited leukocyte toxicities, 2 patients experienced myelosuppression, involving anemia and thrombocytopenia, requiring transfusion of red cell or platelet concentrate following Sr-89 treatment. Of the 18 patients, 5 (27.8%) reported pain flares, all of whom were successfully treated with rescue drugs alone. According to the logistic regression analysis, of the pre-administration characteristics, only ALP was identified as a significant predictor of bone marrow suppression in the univariate and multivariate analyses (P=0.006). Therefore, Sr-89 treatment was found to be effective in ameliorating bone pain associated with metastasis from prostate cancer. Although it is difficult to identify the patients who will receive pain relief prior to Sr-89 administration, this drug should be administered during the early stages due to the potential for bone marrow suppression in patients with high ALP levels.
机译:本研究的目的是评估锶89(Sr-89)在前列腺癌骨转移患者中的姑息作用和不良事件。回顾了2008年2月至2014年4月间在国家九州癌症中心接受Sr-89治疗的18例经骨闪烁显像诊断为前列腺癌并疼痛的骨转移患者。在18位受试者中,有13位(72.2%)达到了疼痛反应,而5位被归类为疼痛无反应者(27.8%)。根据逻辑回归分析,给药前的特征包括年龄,前列腺特异性抗原(PSA),碱性磷酸酶(ALP),骨修饰剂的给药史,使用阿片类药物或姑息性放射疗法,合并雄激素后的时间自疼痛发作以来的最低点和时间的封锁,未发现是疼痛反应的重要预测因子。同样,给药后的特征(包括疼痛发作,PSA和ALP应答)也未发现是疼痛应答的重要预测指标。尽管没有患者表现出白细胞毒性,但2名患者经历了骨髓抑制,涉及贫血和血小板减少症,需要在Sr-89治疗后输注红细胞或血小板浓缩液。在18例患者中,有5例(27.8%)报告有疼痛发作,所有患者均仅接受了抢救药物即可成功治愈。根据逻辑回归分析,在单变量和多变量分析中,仅在给药前的特征中,只有ALP被确定为骨髓抑制的重要预测因子(P = 0.006)。因此,发现Sr-89治疗在减轻与前列腺癌转移相关的骨痛方面是有效的。尽管很难确定在Sr-89给药之前会缓解疼痛的患者,但由于ALP水平高的患者可能会抑制骨髓,因此应在早期阶段给药。

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