AI Article Synopsis
- The study highlights the importance of CYP3A4 in drug metabolism and its role in drug-drug interactions, underscoring the need for better predictive models during drug development.
- The research assesses the ability of human cryopreserved hepatocytes to predict the fraction of metabolism via CYP3A for different compounds, using ketoconazole to gauge intrinsic clearance rates.
- Findings reveal that variability in CYP3A metabolism for compounds with multiple metabolic pathways cannot be accurately predicted through inhibition experiments, suggesting that a broader approach using multiple hepatocyte batches is necessary for reliable estimations.
Article Abstract
1. It has previously been demonstrated that metabolism of drugs via a single enzymatic pathway, particularly CYP3A4, is associated with increased risk for drug-drug interactions (DDI). Quantitative experimental systems as well as integrated prediction models to assess such risk during the preclinical phase are highly warranted. 2. The present study was designed to systematically investigate the performance of human cryopreserved hepatocytes in suspension to predict fraction metabolized via CYP3A (fmCYP3A) by assessing the ketoconazole sensitive intrinsic clearance (CLint) for five prototypical CYP3A substrates with varying degree of CYP3A dependent CLint in twelve individual hepatocyte batches. 3. We demonstrate that in contrast to well predicted mean hepatic metabolic clearance (CLH) and mean fmCYP3A data, the variability in CYP3A contribution for compounds having multiple metabolic pathways cannot be predicted from inhibition experiments using ketoconazole as inhibitor. Instead, data in the present paper indicate that the variability is larger after inhibition of CYP3A for compounds having multiple metabolic pathways. 4. It is therefore recommended to estimate the average CLint and fmCYP3A for a given test compound in a series (n = 10) of individual human hepatocyte batches.
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| http://dx.doi.org/10.3109/00498254.2013.809617 | DOI Listing |
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