促红细胞生成素治疗顺铂相关性贫血的Ⅰ-Ⅱ期试验

Phase I-II trial of erythropoietin in the treatment of cisplatin-associated anemia.

作者信息

Miller C B, Platanias L C, Mills S R, Zahurak M L, Ratain M J, Ettinger D S, Jones R J

机构信息

Johns Hopkins Oncology Center, Baltimore, Md 21205.

出版信息

J Natl Cancer Inst. 1992 Jan 15;84(2):98-103. doi: 10.1093/jnci/84.2.98.

DOI:10.1093/jnci/84.2.98

PMID:1735886

Abstract

BACKGROUND

Cancer patients undergoing chemotherapy with cisplatin-containing regimens often develop anemia. Although the cause is multifactorial, erythropoietin deficiency appears to play an important role. Recombinant human erythropoietin (epoetin) has been reported to be effective in reversing cisplatin-associated anemia in animal studies but not in clinical trials.

PURPOSE

This pahse I-II clinical trial was designed to assess the safety and efficacy of treatment with epoetin for anemia associated with cisplatin chemotherapy.

METHODS

Twenty-one cancer patients treated with cisplatin and manifesting anemia (hemoglobin level less than 110 g/L) received epoetin at escalating doses (25, 50, 100, or 200 U/kg body weight) intravenously five times a week for 4 weeks.

RESULTS

Epoetin was well tolerated, and a maximal tolerated dose was not reached. Two patients experienced hypertension, which responded to standard antihypertensive therapy. No dose-dependent severe toxic effects were seen. The increase in hemoglobin levels from baseline on day 1 of the study was statistically significant after 4 weeks of epoetin therapy in the groups receiving 100 U/kg (mean change +/- SD = 19 +/- 13 g/L; P = .03) or 200 U/kg (mean change = 24 +/- 17 g/L; P = .007). A clinical response--an increase in hemoglobin level greater than 10 g/L--was achieved in 12 patients after 4 weeks of treatment. For these responders, the mean increase in hemoglobin level was 25 +/- 3.3 g/L over the level observed at the same time in the chemotherapy cycle preceding epoetin treatment, and this increase was statistically significant (P = .0001). Neither serum erythropoietin level nor hemoglobin level predicted a patient's response to epoetin.

CONCLUSIONS

These preliminary findings suggest that epoetin is effective and well tolerated for the reversal of cisplatin-associated anemia, with the 100-U/kg and 200-U/kg dose levels offering optimal clinical response.

IMPLICATIONS

We are conducting a phase III trial to determine the effect of epoetin on transfusion requirements in patients undergoing chemotherapy.

摘要

背景

接受含顺铂化疗方案的癌症患者常出现贫血。尽管病因是多方面的，但促红细胞生成素缺乏似乎起重要作用。在动物研究中，重组人促红细胞生成素（依泊汀）已被报道可有效逆转顺铂相关性贫血，但在临床试验中却并非如此。

目的

本I-II期临床试验旨在评估依泊汀治疗顺铂化疗相关性贫血的安全性和有效性。

方法

21例接受顺铂治疗且出现贫血（血红蛋白水平低于110 g/L）的癌症患者，每周静脉注射递增剂量（25、50、100或200 U/kg体重）的依泊汀5次，共4周。

结果

依泊汀耐受性良好，未达到最大耐受剂量。2例患者出现高血压，对标准抗高血压治疗有反应。未见剂量依赖性严重毒性作用。在接受100 U/kg（平均变化±标准差=19±13 g/L；P = 0.03）或200 U/kg（平均变化=24±17 g/L；P = 0.007）的组中，依泊汀治疗4周后，血红蛋白水平较研究第1天的基线水平升高具有统计学意义。治疗4周后，12例患者实现了临床反应——血红蛋白水平升高大于10 g/L。对于这些有反应者，血红蛋白水平较依泊汀治疗前化疗周期同期观察到的水平平均升高25±3.3 g/L，且这种升高具有统计学意义（P = 0.0001）。血清促红细胞生成素水平和血红蛋白水平均不能预测患者对依泊汀的反应。