Visani G, Milligan D, Leoni F, Chang J, Kelsey S, Marcus R, Powles R, Schey S, Covelli A, Isidori A, Litchman M, Piccaluga P P, Mayer H, Malagola M, Pfister C
Istituto di Ematologia e Oncologia Medica L & A Seragnoli, Università degli Studi di Bologna, Azienda Ospedaliera Policlinico Sant'Orsola-Malpighi, Italy.
Leukemia. 2001 May;15(5):764-71. doi: 10.1038/sj.leu.2402117.
PSC 833 (Valspodar) can reverse multidrug resistance (MDR) in patients with hematologic malignancies, but alters the pharmacokinetics of concomitant anticancer agents. A phase I, dose-finding study was initiated to define a safe and effective regimen of mitoxantrone, etoposide, and cytarabine (MEC) when administered with PSC 833 to patients with early relapsed or refractory acute myeloid leukemia (AML). Poor-prognosis AML patients refractory to first-line induction therapy or relapsing within 9 months of attaining complete remission (CR) were treated with cytarabine (1.0 g/m2/day), etoposide (30 mg/m2/day), and mitoxantrone at a dose of either 3.0 mg/m2/day (cohort 1) or 4.5 mg/m2/day (cohorts 2 and 3) for 6 days plus continuous-infusion PSC 833 (10 mg/kg/24 h with a 2.0 mg/kg loading dose) for 6 or 7 days each 21-day cycle. Patients achieving CR were given a 4-day MEC plus PSC 833 consolidation cycle. Twenty-three patients were enrolled (eight with primary refractory AML and 15 in relapse). Dose-limiting toxicity occurred in one of six patients in cohort 2 (grade 4 mucositis) and one of seven patients in cohort 3 (grade 4 hyperbilirubinemia). The maximum tolerated dose of mitoxantrone was defined as 4.5 mg/m2/day. Clinically significant grade 4 hyperbilirubinemia, possibly related to PSC 833, occurred in four patients. Hematologic toxicities were as expected in this patient population, but were not dose limiting. Mild to moderate cerebellar ataxia and paresthesia occurred in six (26%) and five (22%) patients, respectively, but were not dose limiting. Overall, six of 23 (26%) patients achieved CR, including five patients with demonstrated P-glycoprotein expression and/or function. The median overall survival was 4 months. All six patients with a CR were alive and four (17%) patients were disease free at 12 months. Blood levels of PSC 833 were well above the target level of 1000 ng/ml, a concentration that is known to reverse MDR in vitro. PSC 833 reduced the clearance of etoposide by approximately two-fold. No correlation was observed between the mitoxantrone or etoposide area under the curve and response. In conclusion, the MEC plus PSC 833 tested regimen was well tolerated and the 26% CR rate warrants further testing of this regimen in a randomized, phase III trial.
PSC 833(伐司朴达)可逆转血液系统恶性肿瘤患者的多药耐药性(MDR),但会改变同时使用的抗癌药物的药代动力学。开展了一项Ⅰ期剂量探索研究,以确定米托蒽醌、依托泊苷和阿糖胞苷(MEC)与PSC 833联合应用于早期复发或难治性急性髓系白血病(AML)患者时的安全有效方案。对一线诱导治疗难治或在达到完全缓解(CR)后9个月内复发的预后不良AML患者,给予阿糖胞苷(1.0 g/m2/天)、依托泊苷(30 mg/m2/天),米托蒽醌剂量为3.0 mg/m2/天(第1组)或4.5 mg/m2/天(第2组和第3组),持续6天,外加连续输注PSC 833(10 mg/kg/24 h,负荷剂量2.0 mg/kg),每21天周期持续6或7天。达到CR的患者接受为期4天的MEC加PSC 833巩固周期治疗。共入组23例患者(8例原发性难治性AML患者和15例复发患者)。第2组6例患者中有1例(4级粘膜炎)和第3组7例患者中有1例(4级高胆红素血症)发生剂量限制性毒性。米托蒽醌的最大耐受剂量确定为4.5 mg/m2/天。4例患者出现可能与PSC 833相关的具有临床意义的4级高胆红素血症。血液学毒性在该患者群体中符合预期,但并非剂量限制性毒性。分别有6例(26%)和5例(22%)患者出现轻度至中度小脑共济失调和感觉异常,但并非剂量限制性毒性。总体而言,23例患者中有6例(26%)达到CR,包括5例显示P-糖蛋白表达和/或功能的患者。中位总生存期为4个月。所有6例达到CR的患者均存活,4例(17%)患者在12个月时无疾病。PSC 833的血药浓度远高于1000 ng/ml的目标水平,该浓度在体外已知可逆转MDR。PSC 833使依托泊苷的清除率降低了约两倍。未观察到米托蒽醌或依托泊苷曲线下面积与反应之间的相关性。总之,所测试的MEC加PSC 833方案耐受性良好,26%的CR率值得在随机Ⅲ期试验中进一步测试该方案。
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