Comparison of in Vitro Preparations for Semi-Quantitative Prediction of in Vivo Drug Metabolism

Introduction. Since drug interactions may result in serious adverse effects or failure of therapy, it is of huge importance that health professionals base their decisions about drug prescription, dispensing and administration on reliable research evidence, taking into account the hierarchy of data sources for evaluation. Clinical Significance of Potential Interactions - Information Sources. The sources of data regarding drug interactions are numerous, beginning with various drug reference books. However, they are far from uniformity in the way of choosing and presenting putative clinically relevant interactions. Clinical Significance of Potential Interactions - Interpretation of Information. The difficulties in interpretation of drug interactions are illustrated through the analysis of a published example involving assessment made by two different groups of health professionals. Systematic Evaluation of Drug-Drug Interaction. The potential for interactions is mainly investigated before marketing a drug. Generally, the in vitro, followed by in vivo studies are to be performed. The major metabolic pathways involved in the metabolism of a new molecular entity, as well as the potential of induction of human enzymes involved in drug metabolism are to be examined. In the field of interaction research it is possible to make use of the population pharmacokinetic studies as well as of the pharmacodynamic assessment, and also the postregistration monitoring of the reported adverse reactions and other literature data. Conclusion. In vitro and in vivo drug metabolism and transport studies should be conducted to elucidate the mechanisms and potential for drug-drug interactions. The assessment of their clinical significance should be based on well-defined and validated exposure-response data.

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Evaluation of rat brain subcellular fractions for the prediction of in vivo drug metabolism in brain

Drug Metabolism and Pharmacokinetics ◽

10.1016/j.dmpk.2017.11.259 ◽

2018 ◽

Vol 33 (1) ◽

pp. S79 ◽

Cited By ~ 1

Author(s):

Mohammad Shadid ◽

Ying Liu ◽

Elvana Veizaj ◽

Jiansheng Huang ◽

Josh Johnson ◽

...

Keyword(s):

Drug Metabolism ◽

Rat Brain ◽

Subcellular Fractions ◽

In Vivo Drug Metabolism

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Correlations between in Vivo and in Vitro Studies in Human Drug Metabolism

Molecular and Applied Aspects of Oxidative Drug Metabolizing Enzymes ◽

10.1007/978-1-4615-4855-3_6 ◽

1999 ◽

pp. 81-90

Author(s):

Michel Eichelbaum

Keyword(s):

Drug Metabolism ◽

In Vitro Studies

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Nitric Oxide Mediates Hepatic Cytochrome P450 Dysfunction Induced by Endotoxin

Anesthesiology ◽

10.1097/00000542-199606000-00020 ◽

1996 ◽

Vol 84 (6) ◽

pp. 1435-1442 ◽

Cited By ~ 39

Author(s):

Claudia M. Muller ◽

Annette Scierka ◽

Richard L. Stiller ◽

Yong-Myeong Kim ◽

Ryan D. Cook ◽

...

Keyword(s):

Nitric Oxide ◽

Cytochrome P450 ◽

Drug Metabolism ◽

Sprague Dawley ◽

Cytochrome P450 Content ◽

Nitrate Concentrations ◽

Hypnotic Drugs ◽

Plasma Nitrite

Background Animals subjected to immunostimulatory conditions (sepsis) exhibit decreased total cytochrome P450 content and decreased P450-dependent drug metabolism. Cytochrome P450 function is of clinical significance because it mediates the metabolism of some opioid and hypnotic drugs. The authors tested the hypothesis that reduced P450 function and decreased drug metabolism in sepsis are mediated by endotoxin-enhanced synthesis of nitric oxide. Methods Hepatic microsomes were prepared from male Sprague-Dawley rats in nontreated rats, rats pretreated with phenobarbital and rats receiving aminoguanidine or NG-L-monomethyl-arginine alone. Nitric oxide synthesis was augmented for 12 h with a single injection of bacterial lipopolysaccharides. Nitric oxide synthase was inhibited with aminoguanidine or N(G)-L-monomethyl-arginine during the 12 h of endotoxemia in some animals. Plasma nitrite and nitrate concentrations were measured in vivo, and total microsomal P450 content, and metabolism of ethylmorphine and midazolam in vitro. Results Administration of endotoxin increased plasma nitrite and nitrate concentrations, decreased total cytochrome P450 content, and decreased metabolism of ethylmorphine and midazolam. Inhibition of nitric oxide formation by aminoguanidine or N(G)-L-monomethyl-arginine partially prevented the endotoxin-induced effects in the nontreated and phenobarbital-treated groups. Aminoguanidine or N(G)-L-monomethyl-arginine alone did not have an effect on either total cytochrome P450 content or P450-dependent drug metabolism. Plasma nitrite and nitrate concentrations correlated significantly negatively with P450 content (nontreated r = -0.88, phenobarbital r = -0.91), concentrations of formed formaldehyde (nontreated r = -0.87, phenobarbital r = -0.95), and concentrations of midazolam metabolites (4-OH midazolam nontreated r = -0.88, phenobarbital r = -0.93, and 1'-OH midazolam nontreated r = -0.88, phenobarbital r = -0.97). Conclusions Altered hepatic microsomal ethylmorphine and midazolam metabolism during sepsis is mediated in large part by nitric oxide.

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The effect of cimetidine on in vitro and in vivo microsomal drug metabolism in the rat

Biochemical Pharmacology ◽

10.1016/0006-2952(80)90448-7 ◽

1980 ◽

Vol 29 (22) ◽

pp. 3075-3080 ◽

Cited By ~ 108

Author(s):

Olavi Pelkonen ◽

Juhani Puurunen

Keyword(s):

Drug Metabolism ◽

Microsomal Drug Metabolism

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