Etoposide admixed with cisplatin. Phase I clinical investigation of 72-hour infusion

Abstract

The compatibility of etoposide (VP-16-213) and cisplatin (CDDP) in an admixture solution was established by High Pressure Liquid Chromotography (HPLC) studies in vitro at room temperature. A Phase I dualdose escalation study of the admixture was subsequently carried out utilizing a 24-hour continuous infusion schedule administered for 3 consecutive days and repeated at 3 to 4 week intervals. Twenty-seven patients received a total of 42 treatment courses. The daily dose rates for VP-16-213 were 50, 75, and 100 mg/m²/day. Cisplatin was delivered at 20, 30, and 40 mg/m²/day for each dose level of VP-16-213. Doserate limiting toxicity was observed first at the VP-16 dose of 50 mg/m²/day and CDDP at 30 mg/m²/day. At 100 mg/m²/day for VP-16-213, six of 17 courses were associated with life-threatening leukopenia and four of six patients died with sepsis. All but one of the patients developing severe or life-threatening leukopenia had associated acute renal failure with serum creatinine levels greater than 2 mg/dl. The optimal dose rate of delivery for VP-16 and CDDP administered as a 72-hour infusion admixture is 75 mg/m²/day and 30 mg/m²/day, respectively.