Identifying the Reactive Metabolites of Tyrosine Kinase Inhibitor Pexidartinib In Vitro Using LC–MS-Based Metabolomic Approaches

Qin, Xuan; Wang, Yong; MacKenzie, Kevin R.; Hakenjos, John M.; Chen, Si; Khalil, Saleh M.; Jung, Sung Yun; Young, Damian W.; Guo, Lei; Li, Feng

doi:10.1021/acs.chemrestox.3c00164

Cited by 4 publications

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References 26 publications

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“…One SA is facile formation of a 3-methylene(aza)indole and the other an imine methide on the pyridine, both originating from the same methylene group. Formation of a large range of GSH and methoxyamine adducts was recently established; metabolism in addition involved cleavage of the pyrrole ring …”

Section: Work To Extend and Improve The Sarm Conceptmentioning

confidence: 99%

Use of Structural Alerts for Reactive Metabolites in the Application SpotRM

Claesson

2024

Chem. Res. Toxicol.

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Reactive metabolite (RM) formation is widely accepted as playing a crucial role in causing idiosyncratic adverse drug reactions (IADRs), where the liver is most affected. An important goal of drug design is to avoid selection of drug candidates giving rise to RMs and therefore risk causing problems later on involving IADRs. The simplest, initial approach is to avoid test structures that have substructures known or strongly suspected to be associated with IADRs. However, as is evident from the many case reports of IADRs, in most cases a clear association with any (bio)chemical mechanism is lacking, which makes it hard to establish any structure-toxicity relationship. Separate studies of RM formation, in vitro and in vivo, have led to likely evidence and to establishing many structural alerts (SAs) that can be used for fast selection/deselection of planned test compounds. As a background to a discussion of the concept, 25 kinase inhibitor drugs with known problems of hepatotoxicity were probed against a set of SAs contained in the application SpotRM. A clear majority of the probed drugs show liabilities as evident by being flagged by more than one of the fairly established types of SAs. At the same time, no clear SAs were found in three drugs, which is discussed in the broader context of usefulness and selection tactics of SAs in drug design.

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Section: Work To Extend and Improve The Sarm Conceptmentioning

confidence: 99%