O'Rourke T J, Weiss G R, New P, Burris H A, Rodriguez G, Eckhardt J, Hardy J, Kuhn J G, Fields S, Clark G M
Hematology-Oncology Service, Brooke Army Medical Center, Fort Sam Houston, TX 78234-6200.
Anticancer Drugs. 1994 Oct;5(5):520-6. doi: 10.1097/00001813-199410000-00002.
Ormaplatin is a platinum analog that was developed because of an altered toxicity profile and non-cross resistance to cisplatin in both in vitro and in vivo models. To determine the toxicities and maximum tolerated dose of ormaplatin on a daily times five schedule, patients with refractory solid tumors received ormaplatin on five consecutive days at nine dose levels ranging from 1.0 to 15.0 mg/m2/day. A total of 35 patients received 70 cycles of therapy. Nausea and vomiting and myelosuppression were moderate and not dose-limiting. Dose-limiting neurotoxicity, consisting of a sensory peripheral neuropathy, was seen in all five patients who received cumulative doses greater than or equal to 165 mg/m2. This neurotoxicity was symptomatic in all patients and caused significant functional impairment in four patients with inability to walk in two patients. A sensitive atomic absorption spectroscopy analysis performed for one patient at the 13.0 mg/m2/day dose level showed a Cpmax of 163 ng/ml and a t1/2 of 10.9 min for free platinum. A phase II dose could not be determined due to the onset of peripheral neuropathy at low cumulative doses and not at absolute dose levels.
奥马铂是一种铂类类似物,因其在体外和体内模型中具有改变的毒性特征且对顺铂无交叉耐药性而被开发。为了确定奥马铂每日5次给药方案的毒性和最大耐受剂量,难治性实体瘤患者在9个剂量水平(范围为1.0至15.0mg/m²/天)下连续5天接受奥马铂治疗。共有35名患者接受了70个周期的治疗。恶心、呕吐和骨髓抑制程度中等,并非剂量限制性毒性。在所有接受累积剂量大于或等于165mg/m²的5名患者中均出现了剂量限制性神经毒性,表现为感觉性周围神经病变。所有患者的这种神经毒性均有症状,4名患者出现了严重功能障碍,2名患者无法行走。对一名接受13.0mg/m²/天剂量水平治疗的患者进行的灵敏原子吸收光谱分析显示,游离铂的Cpmax为163ng/ml,t1/2为10.9分钟。由于在低累积剂量而非绝对剂量水平时出现周围神经病变,因此无法确定II期剂量。
