Abstract
Zibotentan (ZD4054) is an oral-specific endothelin A receptor antagonist in development for the treatment of castration-resistant prostate cancer.
In a number of preclinical studies, the disposition and metabolism of zibotentan were investigated in mice, rats and dogs.
Following oral and intravenous administration, zibotentan was slowly absorbed (maximal concentration at approximately 4 h) and rapidly excreted, with the majority being eliminated by 48 h. The main route of elimination was via the urine in dogs and female rats, but via the faeces in male rats and mice of both sexes. Zibotentan was moderately bound to plasma proteins of all species examined (55–95%), and widely distributed throughout all tissues with the highest concentrations seen in the organs of excretion. Zibotentan was moderately metabolised.
Zibotentan was well absorbed, moderately bound to plasma proteins, widely distributed and excreted predominantly via the urine.
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Acknowledgements
Thanks to Michael Warwick, formerly of AstraZeneca, for his involvement in these studies. Thanks to staff at the following research facilities for conducting the animal studies: Covance Laboratories Ltd, Harrogate, UK; Huntingdon Life Sciences, Huntingdon, UK, and Inveresk, Tranent, UK. We also thank Juliet Fawcett PhD of Mudskipper who provided editorial assistance funded by AstraZeneca.
Declaration of interest
Primary employment by AstraZeneca and share ownership (all authors).