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From peptide libraries to optimized nonpeptide ligands in the search for S‐farnesyltransferase inhibitors

Jean‐Michel Henlin, Nathalie Kucharczyk, C. Desmet‐Beaufort, Armelle Loynel, Annie Genton, Gordon C. Tucker, Ghanem Atassi, Jean‐Luc Fauchère, Jean A. Boutin, Marc Bertrand

发表年份
2001
引用次数
3

摘要

A complete 331,776-member library of tetrapeptides made of 24 amino acid building blocks was synthesized robotically on solid phase and subjected to a deconvolution based on the inhibitory potency of the sublibraries in a HPLC assay of the S-farnesyltransferase activity in vitro. One of the non-natural peptide and noncysteine-containing leads Nip-Trp-Phe-His (Nip=p-nitrophenyl-L-alanine) was optimized chemically to give a proteolytically stable pseudopeptide with a 200-fold potency compared with the original lead. The final compound was converted to the C-terminal ethyl ester: p-F-C6H4-CO(CH2)2-CO-Bta-D-Phepsi[CH2NH]His-OEt (Bta = benzothienyl-L-alanine) and shown to behave as a prodrug which was hydrolyzed back to the C-terminal acid following cell penetration. The method confirmed that several structurally original leads can be discovered in large libraries when deconvolution relies upon a highly specific assay and that these leads can be optimized by chemical modification to impart the final compound the desired pharmacological and pharmacokinetic properties.

关键词

FarnesyltransferaseChemistryProdrugPeptideStereochemistryCombinatorial chemistryAlanineAmino acidBiochemistryEnzyme

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