使用不含阿糖胞苷的伊达比星、依托泊苷和卡铂方案对初治急性髓系白血病进行缓解诱导治疗。
Remission induction therapy of untreated acute myeloid leukemia using a non-cytarabine-containing regimen of idarubicin, etoposide, and carboplatin.
作者信息
Bow E J, Gallant G, Williams G J, Woloschuk D, Shore T B, Rubinger M, Schacter B A
机构信息
Department of Medicine, University of Manitoba, the Health Sciences Centre, Winnipeg, Canada.
出版信息
Cancer. 1998 Oct 1;83(7):1344-54.
BACKGROUND
The safety and efficacy of idarubicin, etoposide, and carboplatin as remission induction therapy for patients younger than 60 years with untreated acute myeloid leukemia was studied as an alternative to standard regimens based on cytarabine plus anthracycline.
METHODS
Eligible patients received idarubicin (36-40 mg/m2), etoposide (500 mg/m2), and carboplatin (1000-1500 mg/m2) over 5 days. Those who achieved complete remission received a single course of cytarabine 1.5 gm/m2 every 12 hours for a total of 12 doses. D-xylose absorption was studied as a marker for cytotoxic therapy-induced gut mucosal damage. Cytogenetic and immunophenotyping studies were performed at the time of diagnosis and examined for prognostic importance.
RESULTS
Remission was achieved in 29 (67%) of 43 patients with a single induction course. The median leukemia free and overall survival times were 15.4 months (95% CI 6.5-24.2) and 12.5 months (95% CI 5.9-19.1), respectively. Induction mortality was 14%. Karyotype (normal, simple, or complex vs. very complex) was the strongest predictor of remission (79% vs. 25%, P=0.01), leukemia free survival (odds ratio [OR] 19.3, 95% CI 2.7-138.9), and overall survival (OR 5.4, 95% CI 2.1-13.9). Dose-limiting gut mucosal toxicity was greatest during Weeks 2 and 3. Bloodstream infections occurred in 49% of patients at a median of 12 days. Grade 3-4 diarrhea, nausea, stomatitis, esophagitis/dysphagia, and vomiting developed in 33%, 26%, 23%, 9%, and 2% of cases, respectively, at a median of 17, 16, 11, 15.5, and 21 days, respectively.
CONCLUSIONS
This regimen was active in adults younger than 60 years with untreated acute myeloid leukemia and normal, simple, or complex karyotypes. Remission duration was confounded by karyotype. Mucosal toxicity limited the tolerability of this regimen. These adverse effects might be overcome by increasing the intensity of postremission therapy and modifying the dosing schedule.
背景
研究了伊达比星、依托泊苷和卡铂作为60岁以下初治急性髓系白血病患者缓解诱导治疗方案的安全性和有效性,以替代基于阿糖胞苷加蒽环类药物的标准方案。
方法
符合条件的患者在5天内接受伊达比星(36 - 40mg/m²)、依托泊苷(500mg/m²)和卡铂(1000 - 1500mg/m²)治疗。达到完全缓解的患者接受单疗程阿糖胞苷1.5g/m²,每12小时一次,共12剂。研究D - 木糖吸收作为细胞毒性治疗引起的肠道黏膜损伤的标志物。在诊断时进行细胞遗传学和免疫表型研究,并检查其预后重要性。
结果
43例患者中29例(67%)通过单次诱导疗程达到缓解。无白血病生存期和总生存期的中位数分别为15.4个月(95%CI 6.5 - 24.2)和12.5个月(95%CI 5.9 - 19.1)。诱导死亡率为14%。核型(正常、简单或复杂与非常复杂)是缓解(79%对
25%,P = 0.01)、无白血病生存期(比值比[OR] 19.3,95%CI 2.7 - 138.9)和总生存期(OR 5.4,95%CI 2.1 - 13.9)的最强预测因素。剂量限制性肠道黏膜毒性在第2周和第3周最大。49%的患者发生血流感染,中位时间为12天。3 - 4级腹泻、恶心、口腔炎、食管炎/吞咽困难和呕吐分别在33%、26%、23%、9%和2%的病例中出现,中位时间分别为17天、16天、11天、15.5天和21天。
结论
该方案对60岁以下初治急性髓系白血病且核型正常、简单或复杂的成人患者有效。缓解持续时间受核型影响。黏膜毒性限制了该方案的耐受性。这些不良反应可能通过增加缓解后治疗强度和调整给药方案来克服。
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