Synthesis and structure-activity relationships of (MeTyr1, MeArg7)-Dynorphin A(1-8)-OH analogues with substitution at position 8.
- 1 January 1990
- journal article
- research article
- Published by Pharmaceutical Society of Japan in CHEMICAL & PHARMACEUTICAL BULLETIN
- Vol. 38 (2), 404-406
- https://doi.org/10.1248/cpb.38.404
Abstract
A series of [MeTyr1, MeArg7]-Dynorphin A (Dyn)(1.sbd.8)-OH analogues, modified at position 8 with various amino acids, is described. Their biological activities were determined in the three bioassays [guinea pig ileum (GPI), mouse vas deferens (MVD), and rabbit vas deferens (RVD)] and in the mouse tail-pinch test after subcutaneous administration. None of the analogues tested displayed more potent .kappa.-opioid activity in the RVD than [MeTyr1, MeArg7, D-Leu8]-Dyn(1-8)-NHEt (1), which is a potent analgesic peptide with similar opioid receptor selectivity to that of Dyn. However, [MeTyr1, MeArg7, MeIle8]-Dyn(1.sbd.8)-OH (11) showed about a twofold more potent analgesic effect than 1. Based on the obtained results it is conceivable that in the case of Dyn(1-8)-OH analogues both a lipophilic L-amino acid in position 8 and an unchanged 7-8 amide bond are essential to maintain potent .kappa.-opioid activity.This publication has 14 references indexed in Scilit:
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