Plasma pharmacokinetics and oral bioavailability of the 3,4,5,6- tetrahydrouridine (THU) prodrug, triacetyl-THU (taTHU), in mice

Jan H. Beumer,Julie L. Eiseman,Judith A. Gilbert,Julianne L. Holleran,Archibong E. Yellow-Duke,Dana M. Clausen,David Z. D'Argenio,Matthew M. Ames,Pamela A. Hershberger,Robert A. Parise,Lihua Bai,Joseph M. Covey,Merrill J. Egorin

Plasma pharmacokinetics and oral bioavailability of the 3,4,5,6- tetrahydrouridine (THU) prodrug, triacetyl-THU (taTHU), in mice

2011

Jan H. Beumer
Julie L. Eiseman
Judith A. Gilbert
Julianne L. Holleran
Archibong E. Yellow-Duke
Dana M. Clausen
David Z. D'Argenio
Matthew M. Ames
Pamela A. Hershberger
Robert A. Parise
Lihua Bai
Joseph M. Covey
Merrill J. Egorin

Purpose Cytidine drugs, such as gemcitabine, undergo rapid catabolism and inactivation by cytidine deaminase (CD). 3,4,5,6-tetrahydrouridine (THU), a potent CD inhibitor, has been applied preclinically and clinically as a modulator of cytidine analogue metabolism. However, THU is only 20% orally bioavailable, which limits its preclinical evaluation and clinical use. Therefore, we characterized THU pharmacokinetics after the administration to mice of the more lipophilic pro-drug triacetyl-THU (taTHU).

Keywords:

Biochemistry
Pharmacology
Tetrahydrouridine
Cytidine
Bioavailability
Deoxycytidine
Cytidine deaminase
Gemcitabine
Prodrug
Medicine
Pharmacokinetics

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