Influence of trastuzumab on epirubicin pharmacokinetics in metastatic breast cancer patients

doi:10.1093/annonc/mdg350

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Annals of Oncology 14:1222-1226, 2003
© 2003 European Society for Medical Oncology

Original Paper

Influence of trastuzumab on epirubicin pharmacokinetics in metastatic breast cancer patients

G. Lunardi¹, M. O. Vannozzi¹, C. Bighin², L. Del Mastro², I. Stevani², G. Schettini² and M. Venturini²^,+

¹ Department of Pharmacology–Pharmacotoxicology Laboratory, ² Department of Medical Oncology, Istituto Nazionale per la Ricerca sul Cancro, Genova, Italy

Received 10 December 2002; revised 20 March 2003; accepted 6 May 2003

Background:

Anthracycline cardiotoxicity is increased by the contemporaneousadministration of trastuzumab. The mechanism by which it occursis as yet unknown. The aim of this study was to evaluate whethertrastuzumab modifies the pharmacokinetics of epirubicin andits metabolites.

Patients and methods:

Women with HER2-positive metastatic breast cancer were treatedwith epirubicin 75 mg/m² i.v. bolus followed by docetaxel75 mg/m² in a 1-h infusion, every 3 weeks for six cycles, andtrastuzumab (once at 4 mg/m², then 2 mg/m² weekly thereafter)in a 30-min infusion. Epirubicin pharmacokinetic data of sevenpatients were evaluated at the first cycle of therapy (baseline,with trastuzumab administered 24 h after epirubicin), and atthe sixth cycle (i.e. 15 weeks after baseline, with trastuzumabadministered immediately before epirubicin).

Results:

No pharmacokinetic change in the parent compound epirubicinwas detected. The area under the plasma concentration–timecurve (AUC_{0–24 h}) was 1230 ± 318 [mean ±standard deviation (SD)] at the first cycle and 1287 ±385 h·µg/l at the sixth. The mean (±SD)maximum plasma concentration (C_max) and the terminal eliminationhalf-life at the first cycle (1303 ± 490 µg/l and12.5 ± 3.1 h, respectively) were similar to those obtainedat the sixth cycle (1229 ± 580 µg/l and 11.5 ±2.9 h, respectively). Pharmacokinetic data of epirubicin metabolitesevaluated at the first and sixth cycle of chemotherapy weresuperimposable without any statistical difference.

Conclusion:

Enhanced anthracycline cardiotoxicity related to trastuzumabadministration was not linked to pharmacokinetic interferenceswith epirubicin and its metabolites.

Key words: advanced breast cancer, epirubicin, pharmacokinetic, trastuzumab

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