Identification of Novel Substrates for Human Cytochrome P450 2J2

@article{Lee2010IdentificationON,
  title={Identification of Novel Substrates for Human Cytochrome P450 2J2},
  author={Caroline A. Lee and David Neul and Andrea Clouser-Roche and Deepak K. Dalvie and Michael R. Wester and Ying Jiang and J. Peter Jones and Sascha Freiwald and Michael A. Zientek and Rheem A. Totah},
  journal={Drug Metabolism and Disposition},
  year={2010},
  volume={38},
  pages={347 - 356}
}
Several antihistamine drugs including terfenadine, ebastine, and astemizole have been identified as substrates for CYP2J2. The overall importance of this enzyme in drug metabolism has not been fully explored. In this study, 139 marketed therapeutic agents and compounds were screened as potential CYP2J2 substrates. Eight novel substrates were identified that vary in size and overall topology from relatively rigid structures (amiodarone) to larger complex structures (cyclosporine). The substrates… 
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Identifying a Selective Substrate and Inhibitor Pair for the Evaluation of CYP2J2 Activity
TLDR
Amiodarone 4-hydroxylation was reported as a specific CYP2J2-catalyzed reaction with no CYP3A4, or other drug-metabolizing enzyme, involvement and enabled the determination of liver relative activity factor and intersystem extrapolation factor for CYP 2J2.
Discovery and Characterization of Novel, Potent, and Selective Cytochrome P450 2J2 Inhibitors
TLDR
A number of marketed drugs as potent and selective CYP2J2 inhibitors are discovered, including telmisartan and flunarizine, which are at least 10-fold more selective against all other major metabolizing CYPs.
PharmGKB summary: cytochrome P450, family 2, subfamily J, polypeptide 2: CYP2J2.
TLDR
This study found that the CYP2J2 substrates arachidonic acid (AA) and ebastine strongly inhibited astemizole O-demethylation in microsomes from human small intestines and in in-vitro experiments with recombinant CYP3A4.
Discovery and Characterization of Novel , Potent , and Selective Cytochrome P 450 2 J 2 Inhibitors
TLDR
A number of marketed drugs as potent and selective CYP2J2 inhibitors are discovered, and it is elucidated that telmisartan is a mixed-type inhibitor, and flunarizine competitively inhibits CYP1J2, one of the human CYPs involved in phase I xenobiotics metabolism.
Terfenadone is a strong inhibitor of CYP2J2 present in the human liver and intestinal microsomes.
Molecular determinant of substrate binding and specificity of cytochrome P450 2J2
TLDR
A new structural model of CYP2J2 is developed, and its sensitivity to substrate binding is explored by molecular dynamics simulations of the interactions with chemically similar fluorescent probes, showing that the induced-fit binding of these probes led to the preferred active poses ready for the catalysis by CYP1J2.
The development of novel cytochrome P450 2J2 (CYP2J2) inhibitor and the underlying interaction between inhibitor and CYP2J2
TLDR
Using a high-throughput screening approach based on enzymic activity of CYP2J2, a novel natural inhibitor is identified (Piperine, 9a) with IC50 value of 0.44 μM from 108 common herbal medicines and a series of its derivatives were designed and synthesised based on the underlying interactions of Piperine with CYP 2J2.
Characterization of the Active Site Properties of CYP4F12
TLDR
Overall, it appears that although CYP4F12 may be capable of binding similar ligands to other cytochrome P450 enzymes such as CYP3A4, the ability to achieve catalytically favorable orientations may be inherently more difficult because of the increased steric constraints of the CYP 4F12 active site.
CYP2J2 and CYP2C19 Are the Major Enzymes Responsible for Metabolism of Albendazole and Fenbendazole in Human Liver Microsomes and Recombinant P450 Assay Systems
TLDR
The data for the first time suggest that albendazole hydroxylation is primarily catalyzed by CYP2J2, whereas fen bendazoles hydroxyation is preferentially catalyzedBy CYP3A and flavin-containing monooxygenase, and the present data will be useful in understanding the pharmacokinetics and drug interactions of albENDazole and fenbendzole in vivo.
Cytochrome P450 2J2: distribution, function, regulation, genetic polymorphisms and clinical significance
Abstract Cytochrome P450 2J2 (CYP2J2) is an enzyme mainly found in human extrahepatic tissues, with predominant expression in the cardiovascular systems and lower levels in the intestine, kidney,
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References

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TLDR
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TLDR
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TLDR
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TLDR
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TLDR
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TLDR
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TLDR
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