The importance of residues 2 (arginine) and 6 (histidine) in high-affinity angiotensin II antagonists
- 1 April 1988
- journal article
- research article
- Published by American Chemical Society (ACS) in Journal of Medicinal Chemistry
- Vol. 31 (4) , 737-741
- https://doi.org/10.1021/jm00399a008
Abstract
The structure-antagonist activity relationship is described for analogues of [Sar1,Ile8]angiotensin II substituted in position 2 (arginine) and position 6 (histidine). An extreme sensitivity of potency to alterations in these positions was observed, suggesting that both residues are important for binding. Evidence is presented suggesting that the position 6 histidine side chain in angiotensin II (AII) is not involved in receptor stimulation. The structure-activity relationship is also explored for both [des-Asp1]AII (AIII) and [des-Asp1,Ile8]AII analogues substituted in position 2 (arginine). The substitution of D-N-methylalanine, D-(NMe)Ala, into position 2 of both [des-Asp1]AII and [des-Asp1, Ile8]AII gives analogues 39 and 40 that appear to be more potent than the native [Arg2]peptides and that are the most potent AIII agonists and antagonists described to date.This publication has 2 references indexed in Scilit:
- Synthesis of angiotensin II antagonists by incorporating .alpha.-methylalanine or O-methylthreonine residues in angiotensin II analogsJournal of Medicinal Chemistry, 1977
- Facile synthesis of amino acid and peptide esters under mild conditions via cesium saltsThe Journal of Organic Chemistry, 1977