Identification of the cytosolic carboxylesterase catalyzing the 5'-deoxy-5-fluorocytidine formation from capecitabine in human liver

doi:10.1124/dmd.104.000554

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Drug Metabolism and Disposition Fast Forward
First published on July 21, 2004; DOI: 10.1124/dmd.104.000554

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Received for publication May 17, 2004.
Revised July 8, 2004.
Accepted for publication July 12, 2004.

Identification of the cytosolic carboxylesterase catalyzing the 5'-deoxy-5-fluorocytidine formation from capecitabine in human liver

Toshiki TABATA ¹, Miki KATOH ¹, Shogo TOKUDOME ², Miki NAKAJIMA ¹, Tsuyoshi YOKOI ¹^*

¹ Kanazawa University ² Dokkyo University School of Medicine

^* Address correspondence to: E-mail: tyokoi{at}kenroku.kanazawa-u.ac.jp

Abstract

Capecitabine, a prodrug of 5-fluorouracil, is first metabolizedto 5'-deoxy-5-fluorocytidine (5'-DFCR) by carboxylesterase (CES),which is mainly expressed in microsomes. Recently, we clarifiedthat 5'-DFCR formation was catalyzed by the enzyme in cytosolas well as microsomes in human liver. In the present study,the cytosolic enzyme involved in 5'-DFCR formation from capecitabinewas identified. This enzyme in the cytosolic preparation waspurified by ammonium sulfate precipitation, Sephacryl S-300gel filtration, Mono P chromatofocusing, and Superdex 200 gelfiltration. The purified enzyme was identified by the aminoacid sequence analysis to be a CES1A1 or a CES1A1 precursor. Based on the result of the N-terminal amino acid sequence analysis,the purified enzyme has no putative signal peptide, indicatingthat it was CES1A1. The apparent K_m and V_max values of 5'-DFCRformation were 19.2 mM and 88.3 nmol/min/mg protein, respectively. The 5'-DFCR formation catalyzed by the purified enzyme wasinhibited by both DFP and BNPP in a concentration-dependentmanner. SN-38 formation from irinotecan also occurred in thepurified enzyme, cytosol, and microsomes. In conclusion, thecytosolic enzyme involved in 5'-DFCR formation from capecitabinewould be CES1A1. It is suggested that the cytosolic CES hassignificant hydrolysis activity and plays an important roleas the microsomal CES in drug metabolism. It is worthy to investigatethe metabolic enzyme in cytosol involved in the activation ofester-type prodrugs such as capecitabine.

Key words: anticancer agents, bioactivation, carboxylesterases, metabolite kinetics, prodrugs

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