Mitigating hERG Inhibition: Design of Orally Bioavailable CCR5 Antagonists as Potent Inhibitors of R5 HIV-1 Replication

Renato Skerlj; Gary Bridger; Yuanxi Zhou; Elyse Bourque; Ernest McEachern; Sanjay Danthi; Jonathan Langille; Curtis Harwig; Duane Veale; Bryon Carpenter; Tuya Ba; Michael Bey; Ian Baird; Trevor Wilson; Markus Metz; Ron MacFarland; Renee Mosi; Veronique Bodart; Rebecca Wong; Simon Fricker; Dana Huskens; Dominique Schols

doi:10.1021/ml2002604

Mitigating hERG Inhibition: Design of Orally Bioavailable CCR5 Antagonists as Potent Inhibitors of R5 HIV-1 Replication

ACS Med Chem Lett. 2012 Jan 25;3(3):216-21. doi: 10.1021/ml2002604. eCollection 2012 Mar 8.

Authors

Renato Skerlj¹, Gary Bridger², Yuanxi Zhou², Elyse Bourque¹, Ernest McEachern², Sanjay Danthi¹, Jonathan Langille², Curtis Harwig², Duane Veale², Bryon Carpenter², Tuya Ba², Michael Bey², Ian Baird², Trevor Wilson², Markus Metz¹, Ron MacFarland², Renee Mosi², Veronique Bodart², Rebecca Wong², Simon Fricker¹, Dana Huskens³, Dominique Schols³

Affiliations

¹ Genzyme Corporation , 153 Second Avenue, Waltham, Massachusetts 02451, United States.
² Anormed Inc. , 200-20353 64th Avenue, Langley, British Columbia, V2Y 1N5 Canada.
³ Rega Institute for Medical Research, Katholieke Universitett Leuven , Minderbroedersstraat 10, B-3000, Belgium.

Abstract

A series of CCR5 antagonists representing the thiophene-3-yl-methyl ureas were designed that met the pharmacological criteria for HIV-1 inhibition and mitigated a human ether-a-go-go related gene (hERG) inhibition liability. Reducing lipophilicity was the main design criteria used to identify compounds that did not inhibit the hERG channel, but subtle structural modifications were also important. Interestingly, within this series, compounds with low hERG inhibition prolonged the action potential duration (APD) in dog Purkinje fibers, suggesting a mixed effect on cardiac ion channels.

Keywords: CCR5; HIV-1; chemokine receptor; hERG.