Benson A B, Trump D L, Koeller J M, Egorin M I, Olman E A, Witte R S, Davis T E, Tormey D C
Cancer Treat Rep. 1985 Jul-Aug;69(7-8):795-9.
Overcoming resistance to chemotherapy is an important goal in cancer treatment. In many systems, resistance to anthracyclines and vinca alkaloids correlates with a diminished intracellular content of drug. In P388 leukemia and Ehrlich ascites tumor, an active outward transport of anthracyclines and vinca alkaloids occurs. Calcium channel blockers, such as verapamil, inhibit this active outward transport and increase intracellular content of vinblastine and anthracyclines in cells resistant to vinca alkaloids and anthracyclines, respectively. We report a phase I trial of vinblastine (1.5 mg/m2 daily as iv continuous infusion X 5 days) in 17 patients and concurrent verapamil in escalating doses. Verapamil was administered as a loading dose (0.02-0.1 mg/kg) followed by a maintenance infusion (0.036-0.18 mg/kg/hour) for 5 1/2 days with continuous cardiac monitoring. There was no apparent augmentation of vinblastine toxicity when vinblastine and verapamil were given concurrently. ECG change was the dose-limiting toxicity. At 0.12 mg/kg/hour, five of nine patients developed first-degree heart block (mean P-R interval, 0.32 seconds; range, 0.23-0.52 seconds). Junctional rhythms were noted in two of 17 patients. Reversible nonspecific T-wave changes were seen in four of 17 patients. Blood pressure and left ventricular ejection fractions (ultrasonic) were not altered. Five of 17 patients had wbc count nadirs less than 2000/mm3, and two of 17 patients had platelet count nadirs less than 100,000/mm3. Four patients experienced neurotoxicity. A mean vinblastine concentration of 2.2 ng/ml (0.55 nM) and a mean verapamil concentration of 290 ng/ml (0.45 microM) were achieved with the concurrent 5-day infusion. The tolerable levels of verapamil obtained appear to be less than those which were reported to inhibit vinblastine efflux in vitro. Additional in vitro experiments at the tolerable doses of vinblastine and verapamil are recommended.
克服化疗耐药性是癌症治疗的一个重要目标。在许多系统中,对蒽环类药物和长春花生物碱的耐药性与细胞内药物含量减少相关。在P388白血病和艾氏腹水瘤中,存在蒽环类药物和长春花生物碱的主动外向转运。钙通道阻滞剂,如维拉帕米,可抑制这种主动外向转运,并分别增加对长春花生物碱和蒽环类药物耐药的细胞内长春碱和蒽环类药物的含量。我们报告了一项针对17例患者的长春碱(每日1.5mg/m²,静脉持续输注×5天)的I期试验以及同时给予递增剂量维拉帕米的情况。维拉帕米以负荷剂量(0.02 - 0.1mg/kg)给药,随后进行维持输注(0.036 - 0.18mg/kg/小时),持续5.5天,并持续进行心脏监测。当同时给予长春碱和维拉帕米时,长春碱的毒性没有明显增加。心电图改变是剂量限制性毒性。在0.12mg/kg/小时时,9例患者中有5例出现一度心脏传导阻滞(平均P - R间期,0.32秒;范围,0.23 - 0.52秒)。17例患者中有2例出现交界性心律。17例患者中有4例出现可逆性非特异性T波改变。血压和左心室射血分数(超声)未改变。17例患者中有5例白细胞计数最低点低于2000/mm³,17例患者中有2例血小板计数最低点低于100,000/mm³。4例患者出现神经毒性。在同时进行的5天输注中,长春碱的平均浓度为2.2ng/ml(0.55nM),维拉帕米的平均浓度为290ng/ml(0.45μM)。所获得的维拉帕米可耐受水平似乎低于据报道在体外抑制长春碱外排的水平。建议在长春碱和维拉帕米的可耐受剂量下进行额外的体外实验。
