Phase I Study of Paclitaxel by Three‐hour Infusion: Hypotension Just after Infusion Is One of the Major Dose‐limiting Toxicities

The primary objectives of this study were to determine the maximum tolerated dose (MTD) of paclitaxel administered by 3‐h infusion to patients with solid tumors, and to characterize the pharmacokinetics of a 3‐h infusion in comparison with those of a 24‐h infusion. Twenty‐seven patients each received one of six levels of paclitaxel, 105, 135, 180, 210, 240 and 270 mg/m(2), with premedication. Two patients given 240 mg/m(2) and one patient given 270 mg/m(2) unexpectedly had grade 3/4 hypotension just after finishing the paclitaxel infusion. Peripheral neuropathy was also dose‐limiting at 270 mg/m(2). Although granulocytopenia was significantly less severe than with a 24‐h infusion, more than half of the patients experienced grade 4 toxicity at doses of 240 or 270 mg/m(2). Severe hypersensitivity reactions (HSRs) were not observed. Pharmacokinetic studies using high performance liquid chromatography demonstrated proportionally greater increases in the peak plasma concentration and area under the curve, and decreases in clearance and volume of distribution with increasing dose, suggesting non‐linear pharmacokinetics of paclitaxel when given by 3‐h infusion. The MTD of paclitaxel given as a 3‐h infusion was determined to be 240 mg/m(2) with dose‐limiting toxicities of granulocytopenia, peripheral neuropathy and hypotension. Hypotension just after infusion, induced by 3‐h infusion of paclitaxel, is a new observation which has not been reported previously. The recommended dose for phase II study is 210 mg/m(2). Although hypotension was observed as an unexpected toxic effect, paclitaxel could be administered safely over 3 h with premedication and proper monitoring, resulting in reduced myelotoxicity and with no increase in the incidence of HSRs as compared with a 24‐h infusion.