Characterization of the metabolism of benzaldehyde dimethane sulfonate (NSC 281612, DMS612)

苯甲醛二甲烷磺酸盐 (NSC 281612, DMS612) 代谢的表征

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作者:Robert A Parise, Julie L Eiseman, Dana M Clausen, Kimberly P Kicielinski, Pamela A Hershberger, Merrill J Egorin, Jan H Beumer

Conclusion

The activating conversion of BEN to BA is mediated not by CYP450 enzymes or aldehyde oxidase, but by ALDH1A1. This enzyme, a potential stem cell marker, may be a candidate biomarker for clinical activity of BEN.

Methods

Human red blood cells (RBC) were used to characterize kinetics and susceptibility to enzyme-specific inhibitors. Recombinant enzymes were used to confirm metabolism of BEN to BA. Analytes were quantitated with established LC-MS/MS methods.

Results

Average apparent Vmax and Km were 68 ng/mL min(-1) [10% RBC](-1) and 373 ng/mL, respectively. The conversion of BEN to BA in RBC was not inhibited by carbon monoxide, nitrogen gas, or menadione, an inhibitor of aldehyde oxidase. The conversion was inhibited by disulfiram, an inhibitor of ALDH. Of available ALDH isoforms ALDH1A1, ALDH3A1, ALDH2, and ALDH5A1, only ALDH1A1 converted BEN to BA.

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