Thio TEPA pharmacokinetics during intravesical chemotherapy and the influence of Tween 80 |
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| Authors: | John R. W. Masters Barbara J. McDermott Wendy E. A. Jenkins Elizabeth Fenwick P. Julian R. Shah Anthony R. Mundy Paul M. Loadman Michael C. Bibby |
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| Affiliation: | (1) University College London, Institute of Urology, St Pauls Hospital, 24 Endell Street, WC2H 9AE London, UK;(2) Department of Therapeutics and Pharmacology, The Queen's University of Belfast, The Whitla Medical Building, BT9 7BL Belfast, Northern Ireland, UK;(3) Clinical Oncology Unit, University of Bradford, BD7 1DP, West Yorkshire, UK |
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| Abstract: | Summary A pharmacokinetic study of randomised crossover design was carried out in which eight patients with recurrent stage pTa or pT1 transitional cell carcinoma of the bladder were given thio TEPA (30 mg) in distilled water or in 10% (v/v) Tween 80 (30 ml) intravesically for 2 h, followed 3 months later by the alternative treatment. Thio TEPA and its primary metabolite, TEPA, were measured in plasma and urine using a sensitive and specific chromatographic assay. Large differences between patients were observed in the proportion of thio TEPA absorbed, ranging from 20%–78%. Peak plasma levels of thio TEPA were observed within 1 h of intravesical administration. By 2 h after administration the plasma levels of TEPA were similar to those of thio TEPA and, in contrast to those of the parent compound, remained at a similar level over the next 4 h. The rate of absorption of thio TEPA was not influenced by Tween 80, but it did cause statistically significant increases in mean peak plasma levels (from 101 to 154 ng/ml) and mean AUC values (from 0.376 to 0.496  g h per ml) and a decrease in the mean half-life (from 1.83 to 1.25 h). To obtain plasma levels similar to those achieved after instillation with thio TEPA alone, the dose should be reduced with Tween 80. |
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