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Merck

Phenylglycine as a novel P2 scaffold in hepatitis C virus NS3 protease inhibitors.

Bioorganic & medicinal chemistry (2006-11-23)
Pernilla Ortqvist, Shane D Peterson, Eva Kerblom, Thomas Gossas, Yogesh A Sabnis, Rebecca Fransson, Gunnar Lindeberg, U Helena Danielson, Anders Karlén, Anja Sandström
ABSTRAKT

Molecular modeling and inhibitory potencies of tetrapeptide protease inhibitors of HCV NS3 proposed phenylglycine as a new promising P2 residue. The results suggest that phenylglycine might be capable of interacting with the NS3 (protease-helicase/NTPase) in ways not possible for the common P2 proline-based inhibitors. Thus, a series of tripeptides, both linear and macrocyclic, based on p-hydroxy-phenylglycine in the P2 position were prepared and their inhibitory effect determined. When the p-hydroxy group was replaced by methoxy, isoquinolin-, or quinolinyloxy functions, inhibitors with improved potencies were obtained. The P2 phenylglycine-based inhibitors were further optimized by C-terminal extension to acyl sulfonamides and by P1-P3 cyclization, which gave products with inhibition constants in the nanomolar range ( approximately 75nM).

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Sigma-Aldrich
D−(−)-α-Phenylglycine, 99%
Sigma-Aldrich
2-Phenylglycine, 95%
Sigma-Aldrich
L−(+)-α-Phenylglycine, 99%