Abstract
Preventing entry of HIV into human host cells has emerged as an attractive approach to controlling viral replication. Maraviroc 1 is an approved antagonist of the human CCR5 receptor which prevents the entry of HIV. Herein, we report the design and discovery of a series of imidazopiperidine CCR5 antagonists which retain the attractive antiviral profile and window over hERG activity of maraviroc 1, combined with improved absorption profiles in rat and dog. Furthermore, this series of compounds has been shown to retain activity against a laboratory generated maraviroc-resistant HIV-1 strain, which indicates an alternative resistance profile to that of maraviroc 1. Compound 41f (PF-232798) was selected as a clinical candidate from the imidazopiperidine series and is currently in phase II clinical trials.
MeSH terms
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Animals
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Anti-HIV Agents / chemical synthesis*
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Anti-HIV Agents / chemistry
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Anti-HIV Agents / pharmacology
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Azabicyclo Compounds / chemical synthesis*
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Azabicyclo Compounds / chemistry
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Azabicyclo Compounds / pharmacology
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CCR5 Receptor Antagonists*
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Cell Line
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Cricetinae
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Cyclohexanes / pharmacology
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Dogs
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Drug Resistance, Viral
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ERG1 Potassium Channel
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Ether-A-Go-Go Potassium Channels / metabolism
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HIV-1 / drug effects*
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HIV-1 / isolation & purification
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Humans
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Imidazoles / chemical synthesis*
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Imidazoles / chemistry
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Imidazoles / pharmacology
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Leukocytes, Mononuclear / drug effects
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Leukocytes, Mononuclear / virology
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Maraviroc
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Models, Molecular
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Protein Binding
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Rats
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Stereoisomerism
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Structure-Activity Relationship
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Triazoles / pharmacology
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Tropanes
Substances
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Anti-HIV Agents
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Azabicyclo Compounds
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CCR5 Receptor Antagonists
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Cyclohexanes
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ERG1 Potassium Channel
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Ether-A-Go-Go Potassium Channels
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Imidazoles
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KCNH2 protein, human
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Triazoles
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Tropanes
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PF 232798
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Maraviroc