Publication | Open Access
Acylguanidines as Small-Molecule β-Secretase Inhibitors
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Citations
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References
2006
Year
Protein AssemblyMolecular BiologyAmyloid Precursor ProteinChemical BiologyPharmaceutical ChemistryMolecular PharmacologyMedicinal ChemistryProtein FoldingProtein X-ray CrystallographySmall-molecule β-Secretase InhibitorsProtein MisfoldingMolecular RecognitionInhibitory ActivityPotent AnalogsBace1 IcBiochemistryDrug DevelopmentPharmacologyStructural BiologyNatural SciencesMedicineSmall MoleculesDrug Discovery
BACE1 is an aspartyl protease responsible for cleaving amyloid precursor protein to liberate Abeta, which aggregates leading to plaque deposits implicated in Alzheimer's disease. We have identified small-molecule acylguanidine inhibitors of BACE1. Crystallographic studies show that these compounds form unique hydrogen-bonding interactions with the catalytic site aspartic acids and stabilize the protein in a flap-open conformation. Structure-based optimization led to the identification of potent analogs, such as 10d (BACE1 IC(50) = 110 nM).
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