University of Washington, Seattle, 98108, USA.
Br J Haematol. 2010 Jan;148(1):48-58. doi: 10.1111/j.1365-2141.2009.07919.x. Epub 2009 Oct 11.
Attempts to overcome multi-drug resistance in acute myeloid leukaemia (AML) have been limited by toxicities. To investigate the effect of reducing peak drug levels, we performed sequential phase II studies using continuous infusion daunorubicin and cytarabine without (AD) and then with ciclosporin (ADC) in older patients with AML. Untreated patients (age 56+ years) received daunorubicin (45 mg/m2 per day for 3 d) and cytarabine (200 mg/m2 per day for 7 d), both by continuous infusion, without (S0112, 60 patients) and then with (S0301, 50 patients) the addition of ciclosporin. Complete response (CR) rates were 38% on S0112 and 44% on S0301. Fatal induction toxicities occurred in 17% and 12% respectively, arising primarily from infection and haemorrhage. Median overall and relapse-free survival was 7 and 8 months for AD respectively, and 6 and 14 months for ADC. Patients with phenotypic or functional P-glycoprotein had somewhat higher CR rates with ADC than AD, although confidence intervals overlapped. In these sequential trials, continuous infusion AD produced CR rates comparable to those with bolus daunorubicin. The addition of ciclosporin did not cause undue toxicities, produced a similar CR rate, and possibly improved relapse-free survival. Further correlate analyses did not identify a subpopulation specifically benefitting from the addition of ciclosporin.
为了研究降低峰浓度药物毒性的效果,我们在老年 AML 患者中进行了连续输注柔红霉素和阿糖胞苷(AD)和随后加用环孢素(ADC)的序贯 2 期研究。未经治疗的患者(年龄≥56 岁)接受柔红霉素(45 mg/m2/天,连续输注 3 天)和阿糖胞苷(200 mg/m2/天,连续输注 7 天),不加(S0112,60 例)和加用(S0301,50 例)环孢素。S0112 组和 S0301 组的完全缓解(CR)率分别为 38%和 44%。分别有 17%和 12%的患者因感染和出血发生致命性诱导毒性。AD 的中位总生存和无复发生存分别为 7 个月和 8 个月,ADC 分别为 6 个月和 14 个月。具有表型或功能 P-糖蛋白的患者在 ADC 治疗时的 CR 率高于 AD,但置信区间重叠。在这些序贯试验中,连续输注 AD 产生的 CR 率与推注柔红霉素相当。加用环孢素不会导致过度毒性,产生相似的 CR 率,可能改善无复发生存。进一步的相关分析并未确定亚组特别受益于加用环孢素。
