Abstract

We have previously reported that amifostine potentiates the anti-tumour activity of carboplatin in mice. The present study was carried out in well-established human ovarian cancer xenografts OVCAR-3, A2780 and FMa grown subcutaneously in the nude mouse. It was found that a single dose of amifostine resulted in a higher increase in the anti-tumour activity of carboplatin than three doses of amifostine. A single dose of amifostine increased the AUC (area under the curve) values of total platinum in plasma ultrafiltrate (30.1 vs 18.2 microM x h), liver (307.7 vs 236.4 nmol g(-1) x h), kidney (500.8 vs 368.3 nmol g(-1) x h) and OVCAR-3 tumour tissue (184.0 vs 146.8 nmol g(-1) x h). Despite this increase in total platinum, a decrease in platinum (Pt)-DNA adduct levels was observed in liver, kidney and bone marrow, which was significant in liver. In tumour tissue an insignificant increase in Pt-DNA adduct levels, specifically the Pt-GG adduct, was observed after treatment with a single dose of amifostine, which may explain the increase in anti-tumour activity. The increase in the AUC of total platinum was probably caused by a reduction in body temperature, which was most severe after three doses of amifostine. The extreme hypothermia may be the reason that three doses of amifostine resulted in less potentiation of the efficacy of carboplatin.

Highlights

  • Single dose of amifostine increased the Area under the curve (AUC) values of total platinum in plasma ultrafiltrate (30.1 vs 18.2 gM X h), liver (307.7 vs 236.4 nmol g-1 x h), kidney (500.8 vs 368.3 nmol g-' x h) and OVCAR-3 tumour tissue (184.0 vs 146.8 nmol g-' x h)

  • In the present experiments we investigated the influence of multiple doses of amifostine on the efficacy of carboplatin in tumour-bearing nude mice

  • We investigated the influence of one and three doses of amifostine on the pharmacokinetics of carboplatin and the formation of Pt-DNA adducts in order to interpret the efficacy of carboplatin in the presence of amifostine

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Summary

Introduction

Single dose of amifostine increased the AUC (area under the curve) values of total platinum in plasma ultrafiltrate (30.1 vs 18.2 gM X h), liver (307.7 vs 236.4 nmol g-1 x h), kidney (500.8 vs 368.3 nmol g-' x h) and OVCAR-3 tumour tissue (184.0 vs 146.8 nmol g-' x h). Despite this increase in total platinum, a decrease in platinum (Pt)-DNA adduct levels was observed in liver, kidney and bone marrow, which was significant in liver. The extreme hypothermia may be the reason that three doses of amifostine resulted in less potentiation of the efficacy of carboplatin

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