Design, Synthesis and Docking Studies of Hydroxyethylamine and Hydroxyethylsulfide BACE-1 Inhibitors

Luca      Rizzi; Nadia      Vaiana; Francesca      Sagui; Eva      Genesio; Elena      Pilli; Valentina      Porcari; Sergio      Romeo

Protein & Peptide Letters

Author(s): Luca Rizzi, Nadia Vaiana, Francesca Sagui, Eva Genesio, Elena Pilli, Valentina Porcari and Sergio Romeo

DOI: 10.2174/092986609787049439

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Design, Synthesis and Docking Studies of Hydroxyethylamine and Hydroxyethylsulfide BACE-1 Inhibitors

Page: [86 - 90] Pages: 5

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Abstract

Both stereoisomer of hydroxyethylamine (HEA) and hydroxyethylsulfide (HES) transition-state isostere inhibitors of BACE-1 were synthesized. The syn-HEA epimer resulted always more active than the anti stereoisomer independently from the P1 and the P1 substituents. On the contrary, the anti epimer of the HES isostere resulted more active than the syn stereoisomer. The change of stereopreference was studied by molecular modelling.

Keywords: Alzheimer, hydrolases, BACE-1, inhibitors, hydroxyethylamine, hydroxyethylsulfide

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