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Bioorganic and Medicinal Chemistry Letters 2006-Nov

Inhibitory effect of carboxylic acid group on hERG binding.

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Bing-Yan Zhu
Zhaozhong J Jia
Penglie Zhang
Ting Su
Wenrong Huang
Erick Goldman
Daniel Tumas
Vic Kadambi
Priya Eddy
Uma Sinha

Keywords

Abstract

Drug-induced QT prolongation arising from drugs' blocking of hERG channel activity presents significant challenges in drug development. Many, but not all, of our benzamidine-containing factor Xa inhibitors were found to have high hERG binding propensity. However, incorporation of a carboxylic acid group into these benzamidine molecules generally leads to hERG inactive compounds regardless where the carboxyl group is tethered within the molecules. The inhibitory effect of a carboxylic acid group on hERG binding has also been observed in many series of diverse structural scaffolds (including non-amidines). These findings suggest that the negatively charged carboxylate group causes unfavorable interaction within hERG channel binding cavity by electrostatic interaction.

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