Phase I clinical trial combining imatinib mesylate and IL-2 in refractory cancer patients: IL-2 interferes with the pharmacokinetics of imatinib mesylate.

[systemic capillary leak syndrome]

Imatinib mesylate (IM ) is a small molecule inhibitor of protein tyrosine kinases . In addition to its direct effect on malignant cells , it has been suggested IM may activate of natural killer (NK ) cells , hence exerting immunomodulatory functions . In preclinical settings , improved antitumor responses have been observed when IM and interleukin-2 (IL -2 ), a cytokine that enhances NK cells functions , were combined . The goals of this study were to determine the maximum tolerated dose (MTD ) of IL -2 combined with IM at a constant dose of 400 mg , the pharmacokinetics of IM and IL -2 , as well as toxicity and clinical efficacy of this immunotherapeutic regimen in patients affected by advanced tumors . The treatment consisted in 50 mg /day cyclophosphamide from 21 d before the initiation of IM throughout the first IM cycle (from D-21 to D 14 ), 400 mg /day IM for 14 d (D 1 to D 14 ) combined with escalating doses of IL -2 (3 , 6 , 9 and 12 MIU /day ) from days 10 to 14 . This treatment was administered at three week intervals to 17 patients . Common side effects of the combination were mild to moderate , including fever , chills , fatigue , nausea and hepatic enzyme elevation . IL -2 dose level II , 6 MIU /day , was determined as the MTD with the following dose-limiting toxicities : systemic capillary leak syndrome , fatigue and anorexia . Pharmacokinetic studies revealed that the area under the curve and the maximum concentration of IM and its main metabolite CGP 74588 increased significantly when IM was concomitantly administered with IL -2 . In contrast , IM did not modulate IL -2 pharmacokinetics . No objective responses were observed . The best response obtained was stable disease in 8 /17 (median duration : 12 weeks ). Finally , IL -2 augmented the impregnation of IM and its metabolite . The combination of IM (400 mg /day ) and IL -2 (6 MIU /day ) in tumors that express IM targets warrants further investigation .