Literature DB >> 21455238

Managing the challenge of chemically reactive metabolites in drug development.

B Kevin Park1, Alan Boobis, Stephen Clarke, Chris E P Goldring, David Jones, J Gerry Kenna, Craig Lambert, Hugh G Laverty, Dean J Naisbitt, Sidney Nelson, Deborah A Nicoll-Griffith, R Scott Obach, Philip Routledge, Dennis A Smith, Donald J Tweedie, Nico Vermeulen, Dominic P Williams, Ian D Wilson, Thomas A Baillie.   

Abstract

The normal metabolism of drugs can generate metabolites that have intrinsic chemical reactivity towards cellular molecules, and therefore have the potential to alter biological function and initiate serious adverse drug reactions. Here, we present an assessment of the current approaches used for the evaluation of chemically reactive metabolites. We also describe how these approaches are being used within the pharmaceutical industry to assess and minimize the potential of drug candidates to cause toxicity. At early stages of drug discovery, iteration between medicinal chemistry and drug metabolism can eliminate perceived reactive metabolite-mediated chemical liabilities without compromising pharmacological activity or the need for extensive safety evaluation beyond standard practices. In the future, reactive metabolite evaluation may also be useful during clinical development for improving clinical risk assessment and risk management. Currently, there remains a huge gap in our understanding of the basic mechanisms that underlie chemical stress-mediated adverse reactions in humans. This review summarizes our views on this complex topic, and includes insights into practices considered by the pharmaceutical industry.

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Year:  2011        PMID: 21455238     DOI: 10.1038/nrd3408

Source DB:  PubMed          Journal:  Nat Rev Drug Discov        ISSN: 1474-1776            Impact factor:   84.694


  88 in total

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Review 8.  Xenobiotic acyl glucuronides and acyl CoA thioesters as protein-reactive metabolites with the potential to cause idiosyncratic drug reactions.

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10.  Bioinformatic analysis of xenobiotic reactive metabolite target proteins and their interacting partners.

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  87 in total

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3.  Quantitative Chemical Proteomic Profiling of the in Vivo Targets of Reactive Drug Metabolites.

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8.  Screening reactive metabolites bioactivated by multiple enzyme pathways using a multiplexed microfluidic system.

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9.  Reversible inhibitors of regulators of G-protein signaling identified in a high-throughput cell-based calcium signaling assay.

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