Design, synthesis, and modeling of novel cyclic thrombin receptor-derived peptide analogues of the Ser42-Phe-Leu-Leu-Arg46 motif sequence with fixed conformations of pharmacophoric groups: Importance of a Phe/Arg/NH2 cluster for receptor activa

Citation:

Alexopoulos, K. ; Panagiotopoulos, D. ; Mavromoustakos, T. ; Fatseas, P. ; Paredes-Carbajal, M. C. ; Mascher, D. ; Mihailescu, S. ; Matsoukas, J. Design, Synthesis, And Modeling Of Novel Cyclic Thrombin Receptor-Derived Peptide Analogues Of The Ser42-Phe-Leu-Leu-Arg46 Motif Sequence With Fixed Conformations Of Pharmacophoric Groups: Importance Of A Phe/arg/nh2 Cluster For Receptor Activa. Journal of Medicinal Chemistry 2001, 44, 328 - 339.

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Cited By :20Export Date: 23 August 2017

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Thomas Mavromoustakos

Professor, Chemistry

Design, synthesis, and modeling of novel cyclic thrombin receptor-derived peptide analogues of the Ser42-Phe-Leu-Leu-Arg46 motif sequence with fixed conformations of pharmacophoric groups: Importance of a Phe/Arg/NH2 cluster for receptor activa

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Notes:

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