Role and Clinical Consequences of Human<scp>UDP</scp>‐Glucuronosyltransferases

Dalvie, Deepak; Loi, Cho‐Ming

doi:10.1002/9780470921920.edm122

Cited by 2 publications

(4 citation statements)

References 132 publications

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“…UGT1A1 plays a pivotal role in the metabolic elimination and detoxification of many endogenous (such as bilirubin, β‐estradiol and bile acids) and xenobiotic compounds (such as buprenorphine, etoposide, carvedilol, and ethinylestradiol) . UGT1A1 has the capacity to glucuronidate many structurally diverse substrates with different skeleton.…”

Section: Non‐fluorescent Probes For Human Ugtsmentioning

confidence: 99%

“…UGT1A4 prefers catalysing N‐glucuronidation of primary, secondary, tertiary, and aromatic amines . Trifluoperazine (TFP), a tertiary amine, has been confirmed to be a highly selective substrate for UGT1A4.…”

Section: Non‐fluorescent Probes For Human Ugtsmentioning

confidence: 99%

“…UGT1A9, one of the most important UGT isoforms abundantly expressed in human liver and kidney, is implicated in the metabolism of endogenous estrogen and thyroidhormones, as well as a variety of therapeutic drugs, such as entacapone, propofol, and mycophenolic acid . Propofol, an anesthetic drug, could serve as a good probe substrate for UGT1A9 in HLM and has gained wide acceptance for users in in vitro glucuronidation studies (Table S4, Supporting Information).…”

Section: Non‐fluorescent Probes For Human Ugtsmentioning

confidence: 99%

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Chemical Probes for Human UDP‐Glucuronosyltransferases: A Comprehensive Review

Zhang

Hou

et al. 2018

Biotechnology Journal

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UGTs play crucial roles in the metabolism and detoxification of both endogenous and xenobiotic compounds. The key roles of UGTs in human health have garnered great interest in the design and development of specific probes for human UGTs. However, in contrast to other human enzymes, the probe substrates for human UGTs are rarely reported, owing to the highly overlapping substrate specificities of UGTs and the lack of the integrated crystal structures of UGTs. Over the past decades, many efforts are made to develop specific probe substrates for UGTs and use them in both basic research and drug discovery. This review focuses on recent progress in the development of probe substrates for UGTs and their biomedical applications. A long list of chemical probes for UGTs, including non-fluorescent and fluorescent probes along with their structural information and kinetic parameters, are prepared and analyzed. Additionally, challenges and future directions in this field are highlighted in the final section. All information and knowledge presented in this review provide practical tools/methods for measuring UGT activities in complex biological samples, which will be very helpful for rapid screening and characterization of UGT modulators, and for exploring the relevance of UGT enzymes to human diseases.

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Section: Non‐fluorescent Probes For Human Ugtsmentioning

confidence: 99%

Section: Non‐fluorescent Probes For Human Ugtsmentioning

confidence: 99%

Section: Non‐fluorescent Probes For Human Ugtsmentioning

confidence: 99%

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Chemical Probes for Human UDP‐Glucuronosyltransferases: A Comprehensive Review

Zhang

Hou

et al. 2018

Biotechnology Journal

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“…Glucuronidation of carboxylic acid drugs such as nonsteroidal anti-inflammatory drugs (NSAIDs) is a major conjugation reaction catalyzed by multiple UDP-glucuronosyltransferases (UGTs). − The resultant 1-β- O -acyl glucuronides (AGs) are of great importance not only in drug metabolism and excretion but also because of their toxicological consequences. AGs are chemically reactive, electrophilic metabolites that undergo degradation reactions (hydrolysis and intramolecular migration of the 1-β- O -acyl linkage) , as well as covalent binding to cellular macromolecules and thus may be implicated in adverse drug reactions (ADRs) such as drug-induced liver injury − and intestinal injury. − Some NSAIDs have been withdrawn from the market because of ADRs, including liver and renal toxicities and anaphylaxis. ,− Since a pioneering study on the excellent correlation between the extents of covalent binding of AGs to albumin and their degradation rate constants, there have been several thorough studies on the structure–rate constant relationships of AGs as well as prediction and evaluation studies of the toxicological risks posed by AGs. − The mechanism of the covalent binding of AGs to and the binding sites on albumin have been reported, − and the modification of albumin has been demonstrated to proceed via both the direct acylation and the Schiff base-mediated glycation mechanisms.…”

Section: Introductionmentioning

confidence: 99%

Chemo-Enzymatic Synthesis, Structural and Stereochemical Characterization, and Intrinsic Degradation Kinetics of Diastereomers of 1-β-O-Acyl Glucuronides Derived from Racemic 2-{4-[(2-Methylprop-2-en-1-yl)amino]phenyl}propanoic Acid

et al. 2018

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Alminoprofen, ( RS )-2-{4-[(2-methylprop-2-en-1-yl)amino]phenyl}propanoic acid (ALP) 1 , is a racemic drug categorized as a 2-arylpropanoic acid-class nonsteroidal anti-inflammatory drug. Pharmacokinetic studies of 1 in patients have revealed that the corresponding acyl glucuronide 5 is a major urinary metabolite, but little is known about the structure and stereochemistry of 5 . The present work describes the synthesis of a diastereomeric mixture of 1-β- O -acyl glucuronides (2 RS )- 5 from 1 and methyl 2,3,4-tri- O -acetyl-1-bromo-1-deoxy-α- d -glucopyranuronate 2 using our chemo-enzymatic method that has complete specificity for the β-configuration. The structure of (2 RS )- 5 was characterized by 1 H and 13 C NMR spectroscopy and high-resolution mass spectrometry as well as by complete hydrolysis by β-glucuronidase. The absolute stereochemistry of (2 RS )- 5 was determined by comparison with (2 R )- 5 synthesized alternatively from (2 R )- 1 and 2 . Compound (2 R )- 1 was prepared in two steps starting from chiral ( R )-2-(4-nitrophenyl)propanoic acid (2 R )- 6 . Chiral resolution of (2 RS )- 1 was achieved using a chiral high-performance liquid chromatography column, and its stereochemistry was determined by comparison with (2 R )- 1 . The intrinsic degradation rate constant of (2 R )- 5 was 0.405 ± 0.002 h –1 , which is approximately twice that of (2 S )- 5 (the k value was 0.226 ± 0.002 h –1 ) under physiological conditions (pH 7.40, 37 °C).

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Role and Clinical Consequences of HumanUDP‐Glucuronosyltransferases

Cited by 2 publications

References 132 publications

Chemical Probes for Human UDP‐Glucuronosyltransferases: A Comprehensive Review

Chemical Probes for Human UDP‐Glucuronosyltransferases: A Comprehensive Review

Chemo-Enzymatic Synthesis, Structural and Stereochemical Characterization, and Intrinsic Degradation Kinetics of Diastereomers of 1-β-O-Acyl Glucuronides Derived from Racemic 2-{4-[(2-Methylprop-2-en-1-yl)amino]phenyl}propanoic Acid

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