Interpretation of in Vitro Metabolic Stability Studies for Racemic Mixtures.

ACS medicinal chemistry letters(2018)

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摘要
In early drug discovery, where chiral syntheses may not yet have been elucidated or enantiomeric separation is not feasible, screening of racemates in metabolic stability assays may offer a pragmatic approach. To assess the risk of incorrectly deprioritizing enantiomers due to misclassification of apparent intrinsic clearance (CLint), we evaluated (1) theoretical simulations; (2) literature on enantiomeric CLint differences; (3) historic MSD data; and (4) new data on enantiomers with high eudysmic ratios and low predicted three-dimensional similarity. Overall, the results suggested minimal risk of not progressing an enantiomer due to an appreciably different (>3-fold) racemate CLint.
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关键词
Intrinsic clearance,enantiomers,drug discovery,hepatocytes
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