Hyatt_2006_Mol.Cancer.Ther_5_2281

Reference

Title : Intracellular inhibition of carboxylesterases by benzil: modulation of CPT-11 cytotoxicity - Hyatt_2006_Mol.Cancer.Ther_5_2281
Author(s) : Hyatt JL , Tsurkan L , Wierdl M , Edwards CC , Danks MK , Potter PM
Ref : Mol Cancer Ther , 5 :2281 , 2006
Abstract :

Carboxylesterases are ubiquitous proteins responsible for the detoxification of xenobiotics. However, these enzymes also activate prodrugs, such as the anticancer agents capecitabine and CPT-11. As a consequence, overexpression of carboxylesterases within tumor cells sensitizes these cells to CPT-11. We have recently identified two classes of carboxylesterase inhibitors based on either a benzil (diphenylethane-1,2-dione) or a benzene sulfonamide scaffold and showed that these compounds inhibit carboxylesterases with Kis in the low nanomolar range. Because both classes of inhibitors show reversible enzyme inhibition, conventional in vitro biochemical assays would not accurately reflect the in situ levels of carboxylesterase activity or inhibition. Therefore, we have developed a novel assay for the determination of intracellular carboxylesterase activity using 4-methylumbelliferone as a substrate. These studies show that benzil and a dimethylbenzil analogue efficiently enter cells and inhibit human intestinal carboxylesterase and rabbit liver carboxylesterase intracellularly. This inhibition results in reduced cytotoxicity to CPT-11 due to the lack of carboxylesterase-mediated conversion of the prodrug to SN-38. These results suggest that intracellular modulation of carboxylesterase activity with benzil or its analogues may be applied to minimize the toxicity of normal cells to CPT-11.

PubMedSearch : Hyatt_2006_Mol.Cancer.Ther_5_2281
PubMedID: 16985062

Related information

Inhibitor Benzil

Citations formats

Hyatt JL, Tsurkan L, Wierdl M, Edwards CC, Danks MK, Potter PM (2006)
Intracellular inhibition of carboxylesterases by benzil: modulation of CPT-11 cytotoxicity
Mol Cancer Ther 5 :2281

Hyatt JL, Tsurkan L, Wierdl M, Edwards CC, Danks MK, Potter PM (2006)
Mol Cancer Ther 5 :2281