Literature DB >> 20739906

Cerivastatin in vitro metabolism by CYP2C8 variants found in patients experiencing rhabdomyolysis.

Rüdiger Kaspera1, Suresh B Naraharisetti, Bani Tamraz, Tariku Sahele, Matthew J Cheesman, Pui-Yan Kwok, Kristin Marciante, Susan R Heckbert, Bruce M Psaty, Rheem A Totah.   

Abstract

OBJECTIVES: Cerivastatin, a 3-hydroxy-3-methylglutaryl-coenzyme A reductase inhibitor withdrawn from the market because of serious adverse effects, is metabolized primarily by CYP2C8. The occurrence of associated myotoxicity and rhabdomyolysis were attributed to altered cerivastatin pharmacokinetics on account of gemfibrozil-inhibition or genetic variations in CYP2C8 and drug transporters involved in cerivastatin clearance. However, the effect of CYP2C8 genetic variation on cerivastatin metabolism has not been fully elucidated.
METHODS: In this study, patients (n=126) with confirmed cases of rhabdomyolysis after cerivastatin administration had their CYP2C8 gene resequenced and the metabolism of cerivastatin by the discovered CYP2C8 variants was assessed in proteins expressed in Escherichia coli.
RESULTS: In this unique patient population, 12 novel single nucleotide polymorphisms were discovered of which six were exclusively found in patients not using gemfibrozil. Three rare exonic variants resulted in amino acid substitutions and a frame shift deletion (V472fsL494 generating a defective mostly heme-free CYP2C8 protein). A particular promoter located deletion (-635_-634delTA) was tightly linked to CYP2C8*3. Heterologously expressed CYP2C8.3 and CYP2C8.4 displayed an increase in cerivastatin metabolic clearance of up to six-fold compared with the wild-type enzyme. Similarly, an independent sample of microsomes from human livers carrying the CYP2C8*3 and CYP2C8*4 alleles exhibited a 2-fold to 14-fold increase in normalized cerivastatin intrinsic clearance, compared with microsomes from livers carrying only the wild type allele.
CONCLUSION: Gain or loss of catalytic function found in the CYP2C8 gene could certainly alter cerivastatin pharmacokinetics and may influence, at least in part, susceptibility to the development of myotoxicity.

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Year:  2010        PMID: 20739906      PMCID: PMC2993694          DOI: 10.1097/FPC.0b013e32833ecace

Source DB:  PubMed          Journal:  Pharmacogenet Genomics        ISSN: 1744-6872            Impact factor:   2.089


  41 in total

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2.  Expression and characterization of CYP4V2 as a fatty acid omega-hydroxylase.

Authors:  Mariko Nakano; Edward J Kelly; Allan E Rettie
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3.  Glucuronidation converts gemfibrozil to a potent, metabolism-dependent inhibitor of CYP2C8: implications for drug-drug interactions.

Authors:  Brian W Ogilvie; Donglu Zhang; Wenying Li; A David Rodrigues; Amy E Gipson; Jeff Holsapple; Paul Toren; Andrew Parkinson
Journal:  Drug Metab Dispos       Date:  2005-11-18       Impact factor: 3.922

Review 4.  Pharmacokinetic and pharmacodynamic alterations of 3-hydroxy-3-methylglutaryl coenzyme A (HMG-CoA) reductase inhibitors: drug-drug interactions and interindividual differences in transporter and metabolic enzyme functions.

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5.  Benzylic oxidation of gemfibrozil-1-O-beta-glucuronide by P450 2C8 leads to heme alkylation and irreversible inhibition.

Authors:  Brian R Baer; Robert Kirk DeLisle; Andrew Allen
Journal:  Chem Res Toxicol       Date:  2009-07       Impact factor: 3.739

6.  Cytochrome P450 2C8 pharmacogenetics: a review of clinical studies.

Authors:  Elizabeth B Daily; Christina L Aquilante
Journal:  Pharmacogenomics       Date:  2009-09       Impact factor: 2.533

7.  Role of cytochrome P450 2C8 and 2J2 genotypes in calcineurin inhibitor-induced chronic kidney disease.

Authors:  Helen E Smith; J P Jones; Thomas F Kalhorn; Federico M Farin; Patricia L Stapleton; Connie L Davis; James D Perkins; David K Blough; Mary F Hebert; Kenneth E Thummel; Rheem A Totah
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8.  Characterization of novel CYP2C8 haplotypes and their contribution to paclitaxel and repaglinide metabolism.

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  12 in total

1.  Drug metabolism by CYP2C8.3 is determined by substrate dependent interactions with cytochrome P450 reductase and cytochrome b5.

Authors:  Rüdiger Kaspera; Suresh B Naraharisetti; Eric A Evangelista; Kristin D Marciante; Bruce M Psaty; Rheem A Totah
Journal:  Biochem Pharmacol       Date:  2011-06-24       Impact factor: 5.858

2.  OATP1B1-related drug-drug and drug-gene interactions as potential risk factors for cerivastatin-induced rhabdomyolysis.

Authors:  Bani Tamraz; Hisayo Fukushima; Alan R Wolfe; Rüdiger Kaspera; Rheem A Totah; James S Floyd; Benjamin Ma; Catherine Chu; Kristin D Marciante; Susan R Heckbert; Bruce M Psaty; Deanna L Kroetz; Pui-Yan Kwok
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Review 3.  Individualized risk for statin-induced myopathy: current knowledge, emerging challenges and potential solutions.

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4.  A screening study of drug-drug interactions in cerivastatin users: an adverse effect of clopidogrel.

Authors:  J S Floyd; R Kaspera; K D Marciante; N S Weiss; S R Heckbert; T Lumley; K L Wiggins; B Tamraz; P-Y Kwok; R A Totah; B M Psaty
Journal:  Clin Pharmacol Ther       Date:  2012-03-14       Impact factor: 6.875

5.  Cerivastatin, genetic variants, and the risk of rhabdomyolysis.

Authors:  Kristin D Marciante; Jon P Durda; Susan R Heckbert; Thomas Lumley; Ken Rice; Barbara McKnight; Rheem A Totah; Bani Tamraz; Deanna L Kroetz; Hisayo Fukushima; Rüdiger Kaspera; Joshua C Bis; Nicole L Glazer; Guo Li; Thomas R Austin; Kent D Taylor; Jerome I Rotter; Cashell E Jaquish; Pui-Yan Kwok; Russell P Tracy; Bruce M Psaty
Journal:  Pharmacogenet Genomics       Date:  2011-05       Impact factor: 2.089

6.  Variability of CYP2C8 Polymorphisms in Three Jordanian Populations: Circassians, Chechens and Jordanian-Arabs.

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7.  The genetic landscape of major drug metabolizing cytochrome P450 genes-an updated analysis of population-scale sequencing data.

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Review 8.  PharmGKB summary: very important pharmacogene information for cytochrome P450, family 2, subfamily C, polypeptide 8.

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Journal:  Pharmacogenet Genomics       Date:  2013-12       Impact factor: 2.089

9.  In vitro metabolism of exemestane by hepatic cytochrome P450s: impact of nonsynonymous polymorphisms on formation of the active metabolite 17β-dihydroexemestane.

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Review 10.  Pharmacogenetics of Statin-Induced Myotoxicity.

Authors:  Ping Siu Kee; Paul Ken Leong Chin; Martin A Kennedy; Simran D S Maggo
Journal:  Front Genet       Date:  2020-10-16       Impact factor: 4.599

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