<i>N</i>-{3-[2-(4-Alkoxyphenoxy)thiazol-5-yl]-1-methylprop-2-ynyl}carboxy Derivatives as Acetyl-CoA Carboxylase InhibitorsImprovement of Cardiovascular and Neurological Liabilities via Structural Modifications - Concepedia

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<i>N</i>-{3-[2-(4-Alkoxyphenoxy)thiazol-5-yl]-1-methylprop-2-ynyl}carboxy Derivatives as Acetyl-CoA Carboxylase InhibitorsImprovement of Cardiovascular and Neurological Liabilities via Structural Modifications

DOI Full Paper Access

30

Citations

9

References

2007

Year

Yu Gu, Moshe Weitzberg, Richard F. Clark, Xiangdong Xu, Qun Li, Nathan L. Lubbers, Yi Yang, David W. A. Beno, D. L. Widomski, Tianyuan Zhang,

Journal of Medicinal Chemistry

Bioorganic ChemistryImmunologyCardiovascular PharmacologyPharmacotherapyCardiovascular ToxicityPharmaceutical ChemistryMolecular PharmacologyMedicinal ChemistryAcc2 InhibitorAcc InhibitorsDerivativesBiochemistryNeuropharmacologyVascular BiologyDrug DevelopmentPharmacologyNatural SciencesRational Drug DesignStructural ModificationsCarboxy DerivativesAlkyne LinkerNeurological LiabilitiesMedicineDrug Discovery

Abstract

A preliminary safety evaluation of ACC2 inhibitor 1-(S) revealed serious neurological and cardiovascular liabilities of this chemotype. A systematic structure-toxicity relationship study identified the alkyne linker as the key motif responsible for these adverse effects. Toxicogenomic studies in rats showed that 1-(R) and 1-(S) induced gene expression patterns similar to that seen with several known cardiotoxic agents such as doxorubicin. Replacement of the alkyne with alternative linker groups led to a new series of ACC inhibitors with drastically improved cardiovascular and neurological profiles.

References

	Year	Citations

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