Journal article
Nontargeted Identification of Reactive Metabolite Protein Adducts
MG Leeming, WA Donald, RAJ O'Hair
Analytical Chemistry | AMER CHEMICAL SOC | Published : 2017
Abstract
Metabolic bioactivation of many different chemicals results in the formation of highly reactive compounds (chemically reactive metabolites, CRMs) that can lead to toxicity via binding to macromolecular targets (e.g., proteins or DNA). There is a need to develop robust, rapid, and nontargeted analytical techniques to determine the identity of the protein targets of CRMs and their sites of modification. Here, we introduce a nontargeted methodology capable of determining both the identity of a CRM formed from an administered compound as well as the protein targets modified by the reactive metabolite in a single experiment without prior information. Acetaminophen (N-acetyl-p-aminophenol, APAP) a..
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Awarded by Australian Research Council
Funding Acknowledgements
Financial support from the University of Melbourne Interdisciplinary Seed Grant program is gratefully acknowledged. M.G.L. thanks the Elizabeth and Vernon Puzey Foundation for the award of a Ph.D. scholarship and The University of Melbourne for a Norma Hilda Schuster scholarship. W.A.D. thanks the Australian Research Council for a Discovery Early Career Researcher Award (DE130100424) and a Discovery Project (DP160102681). We gratefully acknowledge helpful discussions with Ching-Seng Ang. We thank James Ziogas, Andrew Isaac, Bernard Pope, and David Perkins for useful discussions.