A Laboratory-Specific Scaling Factor to Predict the In Vivo Human Clearance of Aldehyde Oxidase Substrates

Mailys De Sousa Mendes; Alexandra L Orton; Helen E Humphries; Barry Jones; Iain Gardner; Sibylle Neuhoff; Venkatesh Pilla Reddy

doi:10.1124/dmd.120.000082

A Laboratory-Specific Scaling Factor to Predict the In Vivo Human Clearance of Aldehyde Oxidase Substrates

Drug Metab Dispos. 2020 Nov;48(11):1231-1238. doi: 10.1124/dmd.120.000082. Epub 2020 Sep 6.

Authors

Mailys De Sousa Mendes¹, Alexandra L Orton¹, Helen E Humphries¹, Barry Jones¹, Iain Gardner¹, Sibylle Neuhoff¹, Venkatesh Pilla Reddy²

Affiliations

¹ Certara UK Limited, Simcyp Division, Sheffield, United Kingdom (M.D.S.M., H.E.H., I.G., S.N.) and Oncology DMPK Research & Early Development (A.O., B.J.) and Modelling and Simulation, Research & Early Development (V.P.R.), Oncology R&D, AstraZeneca, Cambridge, United Kingdom.
² Certara UK Limited, Simcyp Division, Sheffield, United Kingdom (M.D.S.M., H.E.H., I.G., S.N.) and Oncology DMPK Research & Early Development (A.O., B.J.) and Modelling and Simulation, Research & Early Development (V.P.R.), Oncology R&D, AstraZeneca, Cambridge, United Kingdom venkatesh.reddy@astrazeneca.com.

PMID: 32893186
DOI: 10.1124/dmd.120.000082

Abstract

Aldehyde oxidase (AO) efficiently metabolizes a range of compounds with N-containing heterocyclic aromatic rings and/or aldehydes. The limited knowledge of AO activity and abundance (in vitro and in vivo) has led to poor prediction of in vivo systemic clearance (CL) using in vitro-to-in vivo extrapolation approaches, which for drugs in development can lead to their discontinuation. We aimed to identify appropriate scaling factors to predict AO CL of future new chemical entities (NCEs). The metabolism of six AO substrates was measured in human liver cytosol (HLC) and S9 fractions. Measured blood-to-plasma ratios and free fractions (in the in vitro system and in plasma) were used to develop physiologically based pharmacokinetic models for each compound. The impact of extrahepatic metabolism was explored, and the intrinsic clearance required to recover in vivo profiles was estimated and compared with in vitro measurements. Using HLC data and assuming only hepatic metabolism, a systematic underprediction of clearance was observed (average fold underprediction was 3.8). Adding extrahepatic metabolism improved the accuracy of the results (average fold error of 1.9). A workflow for predicting metabolism of an NCE by AO is proposed, and an empirical (laboratory-specific) scaling factor of three on the predicted intravenous CL allows a reasonable prediction of the available clinical data. Alternatively, considering also extrahepatic metabolism, an scaling factor of 6.5 applied on the intrinsic clearance could be used. Future research should focus on the impact of the in vitro study designs and the contribution of extrahepatic metabolism to AO-mediated clearance to understand the mechanisms behind the systematic underprediction. SIGNIFICANCE STATEMENT: This works describes the development of scaling factors to allow in vitro-in vivo extrapolation of the clearance of compounds by aldehyde oxidase metabolism in humans. In addition, physiologically based pharmacokinetic models were developed for each of the aldehyde oxidase substrate compounds investigated.

MeSH terms

Administration, Intravenous
Aldehyde Oxidase / metabolism*
Biological Availability
Female
Humans
Liver / cytology
Liver / enzymology*
Male
Metabolic Clearance Rate
Microsomes, Liver
Models, Biological*
Oxidation-Reduction

Substances

Aldehyde Oxidase