UDP-Glucuronosyltransferases (UGTs) 2B7 and UGT2B17 Display Converse Specificity in Testosterone and Epitestosterone Glucuronidation, whereas UGT2A1 Conjugates Both Androgens Similarly

Sten, Taina; Bichlmaier, Ingo; Kuuranne, Tiia; Leinonen, Antti; Yli‐Kauhaluoma, Jari; Finel, Moshe

doi:10.1124/dmd.108.024844

Cited by 91 publications

(95 citation statements)

References 23 publications

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“…Steroid hormones are mainly metabolized via glucuronidation (James, 2011). In human, steroid hormones are predominantly glucuronidated by members of the UGT2 family (Sten et al, 2009). In zebrafish, however, they are mainly conjugated by members of the UGT5 family (Tables 2 and 3).…”

Section: Discussionmentioning

confidence: 99%

Characterization of the ZebrafishUgtRepertoire Reveals a New Class of Drug-Metabolizing UDP Glucuronosyltransferases

Wang¹,

Huang²,

Wu³

2014

Mol Pharmacol

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The zebrafish genome contains a gene superfamily of 40 Ugt genes that can be divided into Ugt1, Ugt2, and Ugt5 families. Because the encoded zebrafish UDP glucuronosyltransferase (UGT) proteins do not display orthologous relationships to any of the mammalian and avian UGT enzymes based on molecular phylogeny, it is difficult to predict their substrate specificity. Here, we mapped their tissue-specific expression patterns. We showed that the zebrafish UGT enzymes can be glycosylated. We determined their substrate specificity and catalytic activity toward diverse aglycone substrates. Specifically, we measured mRNA levels of each of the 40 zebrafish Ugt genes in 11 adult tissues and found that they are expressed in a tissue-specific manner. Moreover, functional analyses with the donor of UDP glucuronic acid (UDPGA) for each of the 40 zebrafish UGT proteins revealed their substrate specificity toward 10 important aglycones. In particular, UGT1A1, UGT1A7, and UGT1B1 displayed good glucuronidation activities toward most phenolic aglycones (4-methylumbelliferone, 4-nitrophenol, 1-naphthol, bisphenol A, and mycophenolic acid) and the two carboxylic acids (bilirubin and diclofenac). Importantly, some members of the UGT5, a novel UGT family identified recently, are capable of glucuronidating multiple aglycones with the donor cofactor of UDPGA. In particular, UGT5A5, UGT5B2, and UGT5E1 glucuronidate phenols and steroids with high specificity toward steroid hormones of estradiol and testosterone and estrogenic alkylphenols 4-tert-octylphenol. These results shed new insights into the mechanisms by which fish species defend themselves against vast numbers of xenobiotics via glucuronidation conjugations and may facilitate the establishment of zebrafish as a model vertebrate in toxicological, developmental, and pathologic studies.

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Section: Discussionmentioning

confidence: 99%

Characterization of the ZebrafishUgtRepertoire Reveals a New Class of Drug-Metabolizing UDP Glucuronosyltransferases

Wang¹,

Huang²,

Wu³

2014

Mol Pharmacol

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“…Other than UGTs, 17β‐HSD2, 5‐AR, CYP3A4, and sulfotransferases can also metabolize testosterone, however, the quantitative contribution of these enzymes in testosterone first‐pass metabolism is unknown 28, 29, 30. Dutasteride is a selective inhibitor of the type 1 and type 2 isoforms of the 5‐AR enzyme ( Figure 1).…”

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confidence: 99%

Effect of Dose and 5α‐Reductase Inhibition on the Circulating Testosterone Metabolite Profile of Men Administered Oral Testosterone

Basit

Amory

Prasad

2018

Clinical Translational Sci

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Development of an oral testosterone therapy has proven extremely challenging because of extensive and variable first‐pass metabolism. We investigated the in vivo metabolism of testosterone with increasing oral doses of testosterone, both alone and with the co‐administration of dutasteride (5α‐reductase inhibitor) by liquid‐chromatography tandem mass spectrometry (LC‐MS/MS). In eugonadal men prior to dosing, the circulating concentration of testosterone, androstenedione, etiocholanolone‐glucuronide, and androsterone‐glucuronide was 8.6, 20.9, 9.1, and 55.3%, respectively, of the total testosterone‐related species, whereas testosterone‐glucuronide was ∼1%. When testosterone was dosed orally to men with experimental hypogonadism, a proportion of testosterone‐glucuronide increased to 13%. Dutasteride treatment significantly decreased levels of androsterone and its metabolites. This work reveals extensive metabolism of orally dosed testosterone to androsterone glucuronide via androstenedione, with testosterone‐glucuronide appearing to be the second most important metabolite. This information is of importance in the development of an effective oral testosterone therapy and may have implications for testosterone doping research.

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“…1) was designed to reveal information on the activity of many individual UGTs, and care was taken to ensure that the majority of the compounds in this collection are not substrates for UGT1A6. For example, epitestosterone and AZT are markers for UGT2B7 (Court et al, 2003;Sten et al, 2009), ethinylestradiol is mainly for UGT1A1 (Soars et al, 2003), oxazepam is for UGT2B15 (S-oxazepam glucuronide) (Court et al, 2002), propofol is for UGT1A9 (and UGT1A10 to some extent) (Court, 2005; M. Kurkela and M. Finel, unpublished observation from our laboratory), testosterone is mainly for UGT2B17, and TFP is for UGT1A4 (Uchaipichat et al, 2006). The marker substrate for UGT1A6 was 1-naphthol, a compound that is also glucuronidated by many other UGTs, but at much lower rates than by UGT1A6.…”

Section: Compoundsmentioning

confidence: 99%

Effects of Cell Differentiation and Assay Conditions on the UDP-Glucuronosyltransferase Activity in Caco-2 Cells

Zhang¹,

Tolonen²,

Rousu³

et al. 2010

Drug Metab Dispos

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ABSTRACT:Cell differentiation increases UDP-glucuronosyltransferase (UGT) gene expression in Caco-2 cells. Glucuronidation of 13 UGT substrates, 1-naphthol, diclofenac, epitestosterone, estradiol, ethinylestradiol, indomethacin, oxazepam, R-and S-propranolol, propofol, testosterone, trifluoperazine, and zidovudine, were studied to derive a broad view on the effect of cell differentiation on the glucuronidation activities of different human UGTs. In parallel, the glucuronidation of these compounds in human liver microsomes (HLM) and human intestinal microsomes (HIM) was analyzed. Because many of the substrates are highly lipophilic, the effects of dimethyl sulfoxide (DMSO) concentrations in the reaction mixture on glucuronidation rates were tested, as well as the effect of alamethicin, a pore-forming peptide. Large differences were observed in the effects of DMSO and alamethicin between recombinant UGTs and Caco-2 cells and HLM and HIM, and, therefore, the activity assays were performed under multiple conditions. Regardless of the assay conditions, however, the results clearly indicated that although differentiation increases glucuronidation activity, the rates in Caco-2 cells are mostly very low, much lower than those in either HLM or HIM. One clear exception was observed: substrates of UGT1A6, such as 1-naphthol, were glucuronidated at very high rates in both undifferentiated and differentiated Caco-2 cells. It may thus be concluded that Caco-2 cells, even differentiated ones, do not provide a good model system to assess first-pass drug glucuronidation in the intestine.

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UDP-Glucuronosyltransferases (UGTs) 2B7 and UGT2B17 Display Converse Specificity in Testosterone and Epitestosterone Glucuronidation, whereas UGT2A1 Conjugates Both Androgens Similarly

Cited by 91 publications

References 23 publications

Characterization of the ZebrafishUgtRepertoire Reveals a New Class of Drug-Metabolizing UDP Glucuronosyltransferases

Characterization of the ZebrafishUgtRepertoire Reveals a New Class of Drug-Metabolizing UDP Glucuronosyltransferases

Effect of Dose and 5α‐Reductase Inhibition on the Circulating Testosterone Metabolite Profile of Men Administered Oral Testosterone

Effects of Cell Differentiation and Assay Conditions on the UDP-Glucuronosyltransferase Activity in Caco-2 Cells

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