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  • POPULATION PHARMACOKINETICS AND PHARMACODYNAMICS OF DOXORUBICIN AND CYCLOPHOSPHAMIDE IN BREAST CANCER PATIENTS: A STUDY BY THE EORTC-PAMM-NDDG.

Population pharmacokinetics and pharmacodynamics of doxorubicin and cyclophosphamide in breast cancer patients: a study by the EORTC-PAMM-NDDG.

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  • Markus Joerger
  • Alwin D R Huitema
  • Dick J Richel
  • Christian Dittrich
  • Nikolas Pavlidis
  • Evangelos Briasoulis
  • Jan B Vermorken
  • Elena Strocchi
  • Andrea Martoni
  • Roberto Sorio
  • Henk P Sleeboom
  • Miguel A Izquierdo
  • Duncan I Jodrell
  • Régine Féty
  • Ernst de Bruijn
  • Georg Hempel
  • Mats Karlsson
  • Brigitte Tranchand
  • Ad H G J Schrijvers
  • Chris Twelves
  • Jos H Beijnen
  • Jan H M Schellens

Abstract

PATIENTS AND METHODS

Sixty-five female patients with early or advanced breast cancer received doxorubicin 60 mg/m(2) over 15 minutes followed by cyclophosphamide 600 mg/m(2) over 15 minutes. The plasma concentration-time data of both drugs were measured, and the relationship between drug pharmacokinetics and neutrophil counts was evaluated using nonlinear mixed-effect modelling. Relationships were explored between drug exposure (the area under the plasma concentration-time curve [AUC]), toxicity and tumour response.

AIMS

To investigate the population pharmacokinetics and pharmacodynamics of doxorubicin and cyclophosphamide in breast cancer patients.

RESULTS

Fifty-nine patients had complete pharmacokinetic and toxicity data. In 50 patients with measurable disease, the objective response rate was 60%, with complete responses in 6% of patients. Both doxorubicin and cyclophosphamide pharmacokinetics were associated with neutrophil toxicity. Cyclophosphamide exposure (the AUC) was significantly higher in patients with at least stable disease (n = 44) than in patients with progressive disease (n = 6; 945 micromol . h/L [95% CI 889, 1001] vs 602 micromol . h/L [95% CI 379, 825], p = 0.0002). No such correlation was found for doxorubicin. Body surface area was positively correlated with doxorubicin clearance; AST and patient age were negatively correlated with doxorubicin clearance; creatinine clearance was positively correlated with doxorubicinol clearance; and occasional concurrent use of carbamazepine was positively correlated with cyclophosphamide clearance.

CONCLUSIONS

The proposed inhibitory population pharmacokinetic-pharmacodynamic model adequately described individual neutrophil counts after administration of doxorubicin and cyclophosphamide. In this patient population, exposure to cyclophosphamide, as assessed by the AUC, might have been a predictor of the treatment response, whereas exposure to doxorubicin was not. A prospective study should validate cyclophosphamide exposure as a predictive marker for the treatment response and clinical outcome in this patient group.

More about this publication

Clinical pharmacokinetics
  • Volume 46
  • Issue nr. 12
  • Pages 1051-68
  • Publication date 22-11-2007
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