Conformation-activity correlations for chemotactic tripeptide analogs incorporating dialkyl residues with linear and cyclic alkyl sidechains at position 2

Prasad, Sudhanand ; Rao, R .Balaji ; Bergstrand, Hakan ; Lundquist, Britta ; Becker, Elmer L. ; Balaram, P. (1996) Conformation-activity correlations for chemotactic tripeptide analogs incorporating dialkyl residues with linear and cyclic alkyl sidechains at position 2 International Journal of Peptide and Protein Research, 48 (4). pp. 312-318. ISSN 0367-8377

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Official URL: http://www3.interscience.wiley.com/journal/1216357...

Related URL: http://dx.doi.org/10.1111/j.1399-3011.1996.tb00847

Abstract

Five stereochemically constrained analogs of the chemotactic tripeptide incorporating l-aminocycloalkane-l-carboxylic acid (Acnc) and α, α-dialkylglycines (Deg, diethylglycine; Dpg, N, N-dipropylglycine and Dbg, N, N-dibutylglycine) at position 2 have been synthesized. NMR studies of peptides For-Met-Xxx-Phe-OMe (Xxx = Ac7c. I: Ac8c. II: Deg, III; Dpg, IV and Dbg, V; For, formyl) establish that peptides with cycloalkyl residues, I and II, adopt folded β-turn conformations in CDCl3, and (CD3)2SO. In contrast, analogs with linear alkyl sidechains, III-V, favour fully extended (C5) conformations in solution. Peptides I-V exhibit high activity in inducing β-glucosaminidase release from rabbit neutrophils, with ED50 values ranging from 1.4-8.0 × 10-11. M. In human neutrophils the Dxg peptides III-V have ED50 values ranging from 2.3 × 10-8 to 5.9 × 10-10 M, with the activity order being V>IV>III. While peptides I-IV are less active than the parent. For-Met-Leu-Phe-OH, in stimulating histamine release from human basophils, the Dbg peptide V is appreciably more potent, suggesting its potential utility as a probe for formyl peptide receptors.

Item Type:Article
Source:Copyright of this article belongs to Munksgaard International Publishers.
Keywords:Chemotactic Peptides; α α-dialkylated Residues; Peptide Conformation; β-turns
ID Code:4491
Deposited On:18 Oct 2010 07:42
Last Modified:16 May 2016 15:08

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