Pharmacogenomics of CYP2C9: Functional and Clinical Considerations.

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Daly AK, Rettie AE, Fowler DM, Miners JO

Pharmacogenomics of CYP2C9: Functional and Clinical Considerations.

J Pers Med. 2017 Dec 28;8(1). pii: jpm8010001. doi: 10.3390/jpm8010001.

PubMed ID

29283396 [ View in PubMed

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Abstract

CYP2C9 is the most abundant CYP2C subfamily enzyme in human liver and the most important contributor from this subfamily to drug metabolism. Polymorphisms resulting in decreased enzyme activity are common in the CYP2C9 gene and this, combined with narrow therapeutic indices for several key drug substrates, results in some important issues relating to drug safety and efficacy. CYP2C9 substrate selectivity is detailed and, based on crystal structures for the enzyme, we describe how CYP2C9 catalyzes these reactions. Factors relevant to clinical response to CYP2C9 substrates including inhibition, induction and genetic polymorphism are discussed in detail. In particular, we consider the issue of ethnic variation in pattern and frequency of genetic polymorphisms and clinical implications. Warfarin is the most well studied CYP2C9 substrate; recent work on use of dosing algorithms that include CYP2C9 genotype to improve patient safety during initiation of warfarin dosing are reviewed and prospects for their clinical implementation considered. Finally, we discuss a novel approach to cataloging the functional capabilities of rare 'variants of uncertain significance', which are increasingly detected as more exome and genome sequencing of diverse populations is conducted.

DrugBank Data that Cites this Article

Drug Enzymes

Drug	Enzyme	Kind	Organism	Pharmacological Action	Actions
Coumarin	Cytochrome P450 2C9	Protein	Humans	No	Substrate	Details
Estrone sulfate	Cytochrome P450 2C9	Protein	Humans	Unknown	Substrate Inhibitor	Details
Etodolac	Cytochrome P450 2C9	Protein	Humans	Unknown	Substrate	Details
Warfarin	Cytochrome P450 2C9	Protein	Humans	Unknown	Substrate Inducer	Details

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• Approved
• Vet approved
• Nutraceutical
• Illicit
• Withdrawn
• Investigational
• Experimental
• All Drugs

Drugs	Interaction
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Acenocoumarol Hydroxyprogesterone caproate	The metabolism of Acenocoumarol can be increased when combined with Hydroxyprogesterone caproate.
Axitinib Acetylsalicylic acid	The metabolism of Axitinib can be increased when combined with Acetylsalicylic acid.
Binimetinib Dexamethasone	The metabolism of Binimetinib can be increased when combined with Dexamethasone.
Binimetinib Aminoglutethimide	The metabolism of Binimetinib can be increased when combined with Aminoglutethimide.
Binimetinib Secobarbital	The metabolism of Binimetinib can be increased when combined with Secobarbital.