Inhibition Mechanism of UDP-Glucuronosyltransferase 1A6 by Xanthene Food Dyes
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概要
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We have reported that erythrosine (ET), a xanthene dye, inhibited uridine 5-diphosphate (UDP)-glucuronosyltransferase 1A6 (UGT1A6). In order to clarify the structure-inhibition relationships of these xanthene dyes, the inhibitory effect of xanthene dye on human UGT1A6 activity was investigated, such as acid red (AR), ET, phloxine (PL), and rose bengal (RB). ET, PL, and RB strongly inhibited human UGT1A6 activity, with IC_<50> values =0.05, 0.04, and 0.015 mM, respectively. Meanwhile, AR had almost no effect (IC_<50> value =1.7 mM). ET, PL and RB have four halogen atoms on their xanthene backbone, unlike AR. Meanwhile, some contrast media with high halogens on those aromatic compounds, such as ioxaglic acid, iodixanol, meglumine iotalamate, and diatriazole sodium, did not inhibit human UGT1A6 activity. These results suggest that halogens enhance the inhibitory effect of xanthene dyes. In this study, it was proved that xanthene dyes had an inhibitory effect on human UGT1A6 activity by the combination of xanthene structure and halogens on its. Part of this inhibition by xanthene dyes depends the reaction of ^1O_2 originated on xanthene dyes by light irradiation, because the inhibition was prevented by ^1O_2 quenchers, such as NaN_3 and histidine, and in the dark.
- 公益社団法人日本薬学会の論文
- 2006-10-01
著者
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Uesugi Noriko
Department Of Drug Metabolism And Disposition Graduate School Of Pharmaceutical Sciences Nagoya City
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Mizutani Takaharu
Department Of Drug Metabolism And Disposition Graduate School Of Pharmaceutical Sciences Nagoya City
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Mizutani Takaharu
Department Of Drug Metabolism And Disposition Faculty Of Pharmaceutical Sciences Nagoya City Univers
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Furumiya Kenji
Department of Drug Metabolism and Disposition, Graduate School of Pharmaceutical Sciences, Nagoya Ci
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Furumiya Kenji
Department Of Drug Metabolism And Disposition Graduate School Of Pharmaceutical Sciences Nagoya City
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