Abstract
A novel 2,6-naphthyridine was identified by high throughput screen (HTS) as a dual protein kinase C/D (PKC/PKD) inhibitor. PKD inhibition in the heart was proposed as a potential antihypertrophic mechanism with application as a heart failure therapy. As PKC was previously identified as the immediate upstream activator of PKD, PKD vs PKC selectivity was essential to understand the effect of PKD inhibition in models of cardiac hypertrophy and heart failure. The present study describes the modification of the HTS hit to a series of prototype pan-PKD inhibitors with routine 1000-fold PKD vs PKC selectivity. Example compounds inhibited PKD activity in vitro, in cells, and in vivo following oral administration. Their effects on heart morphology and function are discussed herein.
MeSH terms
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Active Transport, Cell Nucleus
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Administration, Oral
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Aminopyridines / chemical synthesis*
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Aminopyridines / pharmacokinetics
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Aminopyridines / pharmacology
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Animals
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Antihypertensive Agents / chemical synthesis
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Antihypertensive Agents / chemistry
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Antihypertensive Agents / pharmacology
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Blood Pressure / drug effects
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Cardiomegaly / drug therapy
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Cardiomegaly / pathology
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Cell Nucleus / metabolism
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Histone Deacetylases / metabolism
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Isoenzymes / antagonists & inhibitors
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Male
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Models, Molecular
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Muscle Cells / drug effects
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Muscle Cells / metabolism
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Muscle Cells / pathology
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Myocardium / metabolism
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Myocardium / pathology
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Naphthyridines / chemical synthesis*
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Naphthyridines / pharmacokinetics
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Naphthyridines / pharmacology
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Phosphorylation
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Protein Binding
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Protein Kinase C / antagonists & inhibitors*
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Rats
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Rats, Inbred Dahl
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Rats, Sprague-Dawley
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Structure-Activity Relationship
Substances
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Aminopyridines
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Antihypertensive Agents
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Isoenzymes
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Naphthyridines
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cyclohexyl-(4-(1-piperazin-1-yl(2,6)naphthyridin-3-yl)pyridin-2-yl)amine
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protein kinase D
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Protein Kinase C
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Histone Deacetylases