Pharmacokinetic properties of toceranib phosphate (Palladia, SU11654), a novel tyrosine kinase inhibitor, in laboratory dogs and dogs with mast cell tumors.

[cutaneous mastocytosis]

Toceranib phosphate (Palladia , SU 11654 ), an oral tyrosine-kinase inhibitor , is under investigation for the treatment of mast cell tumors in dogs . The pharmacokinetics of toceranib phosphate has been characterized in dogs . Means of the following pharmacokinetic parameters were estimated following a 1 .0 mg /kg i .v . dose to laboratory beagles : plasma clearance of 1 .45 L /kg /h , volume of distribution of 29 .7 L /kg , and terminal half -life of 17 .7 h . Following single oral doses of 3 .25 mg /kg administered to laboratory beagles , mean C (max ) estimates ranged from 68 .6 ng /mL to 112 ng /mL with t (max ) ranging from 5 .3 h and 9 .3 h postdose . Terminal half -life was estimated at 31 h . Oral bioavailability was 76 .9 %. There were no statistically significant (P > 0 .05 ) differences with any pharmacokinetic parameter due to fed /fasted state or with time during 13 weeks of every-other-day dosing at 3 .25 mg /kg . Toceranib concentrations were proportional with dose over the range of 2 .0 to 6 .0 mg /kg . The pharmacokinetics of toceranib in client-owned dogs of a variety of pure and mixed breeds with mast cell tumors was similar to that in healthy laboratory dogs . In summary , toceranib phosphate exhibited moderate clearance , a high volume of distribution , and a moderate elimination half -life . After a single oral dose at 3 .25 mg /kg , the concentration vs . time curve showed broad , sustained exposure with measurable concentrations for more than 48 h . These pharmacokinetic parameters support every-other-day administration of toceranib phosphate at an initial dose of 3 .25 mg /kg for the treatment of mast cell tumors in dogs .