Continued exploration of the triazolopyridine scaffold as a platform for p38 MAP kinase inhibition

Continued exploration of the triazolopyridine scaffold as a platform for p38 MAP kinase inhibition

The structure based drug design, synthesis and structure–activity relationship of a series of C6 sulfur linked triazolopyridine based p38 inhibitors are described. The metabolic deficiencies of this series were overcome through changes in the C6 linker from sulfur to methylene, which was predicted b...

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Veröffentlicht in:Bioorganic & medicinal chemistry letters 2010-01, Vol.20 (2), p.469-473
Hauptverfasser: Jerome, Kevin D., Rucker, Paul V., Xing, Li, Shieh, Huey S., Baldus, John E., Selness, Shaun R., Letavic, Michael A., Braganza, John F., McClure, Kim F.
Format: Artikel
Sprache:eng
Schlagworte:
Animals
BASIC BIOLOGICAL SCIENCES
Benzamides - chemical synthesis
Benzamides - chemistry
Benzamides - pharmacology
Binding Sites
Biological and medical sciences
Bones, joints and connective tissue. Antiinflammatory agents
Bridged Bicyclo Compounds, Heterocyclic - chemical synthesis
Bridged Bicyclo Compounds, Heterocyclic - chemistry
Bridged Bicyclo Compounds, Heterocyclic - pharmacology
Crystallography, X-Ray
DESIGN
Drug Design
ETHYLENE
EXPLORATION
GENERAL AND MISCELLANEOUS//MATHEMATICS, COMPUTING, AND INFORMATION SCIENCE
Humans
Kinase
Medical sciences
Microsomes, Liver - metabolism
Models, Chemical
Models, Molecular
ORIENTATION
p38
p38 Mitogen-Activated Protein Kinases - antagonists & inhibitors
p38 Mitogen-Activated Protein Kinases - metabolism
Pharmacology. Drug treatments
PHOSPHOTRANSFERASES
Protein Kinase Inhibitors - chemical synthesis
Protein Kinase Inhibitors - chemistry
Protein Kinase Inhibitors - pharmacology
Pyrimidines - chemical synthesis
Pyrimidines - chemistry
Pyrimidines - pharmacology
Rats
SIMULATION
Structure-Activity Relationship
STRUCTURE-ACTIVITY RELATIONSHIPS
SULFUR
SYNTHESIS
Triazoles - chemical synthesis
Triazoles - chemistry
Triazoles - pharmacology
Triazolopyridines
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Zusammenfassung:The structure based drug design, synthesis and structure–activity relationship of a series of C6 sulfur linked triazolopyridine based p38 inhibitors are described. The metabolic deficiencies of this series were overcome through changes in the C6 linker from sulfur to methylene, which was predicted by molecular modeling to be bioisosteric. X-ray of the ethylene linked compound 61 confirmed the predicted binding orientation of the scaffold in the p38 enzyme. The structure based drug design, synthesis and structure–activity relationship of a series of C6 sulfur linked triazolopyridine based p38 inhibitors are described. The metabolic deficiencies of this series were overcome through changes in the C6 linker from sulfur to methylene, which was predicted by molecular modeling to be bioisosteric. X-ray of the ethylene linked compound 61 confirmed the predicted binding orientation of the scaffold in the p38 enzyme.
ISSN:0960-894X
1464-3405
DOI:10.1016/j.bmcl.2009.11.114