Literature DB >> 18259986

Cytochrome P450 inactivation by pharmaceuticals and phytochemicals: therapeutic relevance.

William W Johnson1.   

Abstract

One of the major clinical concerns is possible drug interactions that can be the result of abrogation of the P450 pathway(s) of metabolism causing toxicity due to elevated exposures of other drugs metabolized by these pathways. When the P450 substrate is catalytically activated to a reactive intermediate, this transient molecule may react with available nucleophilic residues from the enzyme - thereby resulting in the inactivation of the P450. The effects of CYP inactivation on the pharmacokinetics of co-administered drugs or on the inactivator itself depend on complex factors involving the molecular entities, the kinetics of inactivation (K(I), k(inact)), the partition ratio, the zero-order synthesis rate of new enzyme, multiple pathways of metabolism (competing pathways), the dose or exposure, and specific patient characteristics. This review summarizes the catalytic efficiencies of many inactivator drugs along with any consequent clinical relevance. The chemical agents described have been ranked for the kinetic efficiency of inactivation and contrasted with the known clinically relevant drug interactions. This will allow judicious consideration of the many factors that influence the importance of CYP inactivation and their relative contribution to systemic clearance of co-administered drugs. This study allows an improved characterization and dissection of potential physiological interactions with various drugs and nutrients. Knowing more about selective inactivation of cytochrome P450 by common xenobiotics, drugs and phytochemicals allows better understanding of expected interactions with chemotherapeutics and other xenobiotics.

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Year:  2008        PMID: 18259986     DOI: 10.1080/03602530701836704

Source DB:  PubMed          Journal:  Drug Metab Rev        ISSN: 0360-2532            Impact factor:   4.518


  8 in total

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2.  A highly sensitive fluorogenic probe for cytochrome P450 activity in live cells.

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Authors:  Hsia-lien Lin; Haoming Zhang; Christine Medower; Paul F Hollenberg; William W Johnson
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4.  In vitro-in vivo extrapolation of zolpidem as a perpetrator of metabolic interactions involving CYP3A.

Authors:  Thomas M Polasek; Janani S Sadagopal; David J Elliot; John O Miners
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5.  Marinopyrrole A target elucidation by acyl dye transfer.

Authors:  Chambers C Hughes; Yu-Liang Yang; Wei-Ting Liu; Pieter C Dorrestein; James J La Clair; William Fenical
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Review 6.  Time-dependent enzyme inactivation: Numerical analyses of in vitro data and prediction of drug-drug interactions.

Authors:  Jaydeep Yadav; Erickson Paragas; Ken Korzekwa; Swati Nagar
Journal:  Pharmacol Ther       Date:  2019-12-11       Impact factor: 12.310

7.  The effect of piperine on midazolam plasma concentration in healthy volunteers, a research on the CYP3A-involving metabolism.

Authors:  Mohammad Mahdi Rezaee; Sohrab Kazemi; Mohammad Taghi Kazemi; Saeed Gharooee; Elham Yazdani; Hoda Gharooee; Mohammad Reza Shiran; Ali Akbar Moghadamnia
Journal:  Daru       Date:  2014-01-07       Impact factor: 3.117

Review 8.  Reconceptualization of Hormetic Responses in the Frame of Redox Toxicology.

Authors:  Zoi Skaperda; Fotios Tekos; Periklis Vardakas; Charitini Nepka; Demetrios Kouretas
Journal:  Int J Mol Sci       Date:  2021-12-21       Impact factor: 5.923

  8 in total

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