Phase I study of the combination of topotecan and irinotecan in children with refractory solid tumors

Phase I study of the combination of topotecan and irinotecan in children with refractory solid tumors

We have shown in xenograft studies that the antitumor activities of topotecan and irinotecan are highly schedule- and dose-dependent, with a high frequency of response at low, protracted dose schedules. Preclinical and clinical data suggest that topotecan and irinotecan have different antitumor acti...

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Veröffentlicht in:Cancer chemotherapy and pharmacology 2006, Vol.57 (1), p.15-24
Hauptverfasser: RODRIGUEZ-GALINDO, Carlos, CREWS, Kristine R, STEWART, Clinton F, FURMAN, Wayne, PANETTA, J. Carl, DAW, Najat C, CAIN, Alvida, MING TAN, HOUGHTON, Peter H, SANTANA, Victor M
Format: Artikel
Sprache:eng
Schlagworte:
Adolescent
Antineoplastic agents
Antineoplastic Combined Chemotherapy Protocols - adverse effects
Antineoplastic Combined Chemotherapy Protocols - pharmacokinetics
Antineoplastic Combined Chemotherapy Protocols - therapeutic use
Biological and medical sciences
Camptothecin - adverse effects
Camptothecin - analogs & derivatives
Camptothecin - pharmacokinetics
Camptothecin - therapeutic use
Child
Child, Preschool
Drug Administration Schedule
Humans
Medical sciences
Neoplasms - drug therapy
Neoplasms - metabolism
Pharmacology. Drug treatments
Topotecan - adverse effects
Topotecan - pharmacokinetics
Topotecan - therapeutic use
Treatment Outcome
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Zusammenfassung:We have shown in xenograft studies that the antitumor activities of topotecan and irinotecan are highly schedule- and dose-dependent, with a high frequency of response at low, protracted dose schedules. Preclinical and clinical data suggest that topotecan and irinotecan have different antitumor activities and mechanisms of resistance, and non-overlapping toxicities, providing a rationale for their combination. Combining both agents may increase the amount of camptothecin delivered to the tumor, without additive toxicity. We conducted a phase I study in children with refractory solid tumors to determine the maximum tolerated dose (MTD) of irinotecan when administered with a targeted systemic exposure (TSE) of topotecan and to define the dose-limiting toxicity (DLT) of this combination. Irinotecan was administered IV over 60 min followed by topotecan over 30 min daily for 5 days for two consecutive weeks. We initially fixed the topotecan-TSE to 80+/-10 ng*h/ml and investigated the ability to escalate irinotecan (starting dose 16 mg/m2/d). Topotecan and irinotecan pharmacokinetics were determined. Eleven patients (median age 10 years) were enrolled. Owing to DLT, irinotecan was de-escalated to 12 (level -1; n = 3) and 9 (level -2; n = 3) mg/m2/day, and topotecan-TSE was reduced to 60+/-10 ng*h/ml (level -3; n = 2). DLTs were neutropenia (n = 8), typhlitis (n = 5), and skin rash (n = 1). MTD could not be reached. Median (range) irinotecan and topotecan lactone systemic clearances were 50.3 (16.6-76.2) l/h/m2 and 27.6 (14.7-55.9) l/h/m2, respectively. The pharmacokinetics profile of each agent was similar to that seen in previous single agent studies. One patient with neuroblastoma and one with rhabdomyosarcoma had a partial and a complete response, respectively. Despite promising antitumor activity, the combination of topotecan and irinotecan given on a protracted schedule does not warrant further development in children due to unacceptable toxicity.
ISSN:0344-5704
1432-0843
DOI:10.1007/s00280-005-0030-7