Phase II Metabolism in Human Skin: Skin Explants Show Full Coverage for Glucuronidation, Sulfation, N-Acetylation, Catechol Methylation, and Glutathione Conjugation

Phase II Metabolism in Human Skin: Skin Explants Show Full Coverage for Glucuronidation, Sulfation, N-Acetylation, Catechol Methylation, and Glutathione Conjugation

Although skin is the largest organ of the human body, cutaneous drug metabolism is often overlooked, and existing experimental models are insufficiently validated. This proof-of-concept study investigated phase II biotransformation of 11 test substrates in fresh full-thickness human skin explants, a...

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Veröffentlicht in:Drug metabolism and disposition 2015-01, Vol.43 (1), p.126-139
Hauptverfasser: Manevski, Nenad, Swart, Piet, Balavenkatraman, Kamal Kumar, Bertschi, Barbara, Camenisch, Gian, Kretz, Olivier, Schiller, Hilmar, Walles, Markus, Ling, Barbara, Wettstein, Reto, Schaefer, Dirk J, Itin, Peter, Ashton-Chess, Joanna, Pognan, Francois, Wolf, Armin, Litherland, Karine
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Sprache:eng
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Acetylation
Adult
Aged
Biotransformation - physiology
Catechols - metabolism
Diclofenac - metabolism
Female
Glucuronides - metabolism
Glutathione - metabolism
Humans
Liver - metabolism
Male
Metabolic Detoxication, Phase II - physiology
Methylation
Middle Aged
Naphthols - metabolism
Skin - metabolism
Sulfates - metabolism
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container_end_page 139
container_issue 1
container_start_page 126
container_title Drug metabolism and disposition
container_volume 43
creator Manevski, Nenad
Swart, Piet
Balavenkatraman, Kamal Kumar
Bertschi, Barbara
Camenisch, Gian
Kretz, Olivier
Schiller, Hilmar
Walles, Markus
Ling, Barbara
Wettstein, Reto
Schaefer, Dirk J
Itin, Peter
Ashton-Chess, Joanna
Pognan, Francois
Wolf, Armin
Litherland, Karine
description Although skin is the largest organ of the human body, cutaneous drug metabolism is often overlooked, and existing experimental models are insufficiently validated. This proof-of-concept study investigated phase II biotransformation of 11 test substrates in fresh full-thickness human skin explants, a model containing all skin cell types. Results show that skin explants have significant capacity for glucuronidation, sulfation, N-acetylation, catechol methylation, and glutathione conjugation. Novel skin metabolites were identified, including acyl glucuronides of indomethacin and diclofenac, glucuronides of 17β-estradiol, N-acetylprocainamide, and methoxy derivatives of 4-nitrocatechol and 2,3-dihydroxynaphthalene. Measured activities for 10 μM substrate incubations spanned a 1000-fold: from the highest 4.758 pmol·mg skin–1·h–1 for p-toluidine N-acetylation to the lowest 0.006 pmol·mg skin–1·h–1 for 17β-estradiol 17-glucuronidation. Interindividual variability was 1.4- to 13.0-fold, the highest being 4-methylumbelliferone and diclofenac glucuronidation. Reaction rates were generally linear up to 4 hours, although 24-hour incubations enabled detection of metabolites in trace amounts. All reactions were unaffected by the inclusion of cosubstrates, and freezing of the fresh skin led to loss of glucuronidation activity. The predicted whole-skin intrinsic metabolic clearances were significantly lower compared with corresponding whole-liver intrinsic clearances, suggesting a relatively limited contribution of the skin to the body’s total systemic phase II enzyme-mediated metabolic clearance. Nevertheless, the fresh full-thickness skin explants represent a suitable model to study cutaneous phase II metabolism not only in drug elimination but also in toxicity, as formation of acyl glucuronides and sulfate conjugates could play a role in skin adverse reactions.
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subjects Acetylation
Adult
Aged
Biotransformation - physiology
Catechols - metabolism
Diclofenac - metabolism
Female
Glucuronides - metabolism
Glutathione - metabolism
Humans
Liver - metabolism
Male
Metabolic Detoxication, Phase II - physiology
Methylation
Middle Aged
Naphthols - metabolism
Skin - metabolism
Sulfates - metabolism
title Phase II Metabolism in Human Skin: Skin Explants Show Full Coverage for Glucuronidation, Sulfation, N-Acetylation, Catechol Methylation, and Glutathione Conjugation
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