Τόμος 9 (1995) – Τεύχος 2 & 3 – Άρθρο 9 – Επιθεώρηση Κλινικής Φαρμακολογίας και Φαρμακοκινητικής-Διεθνής Έκδοση – Volume 9 (1995) – Issue 2 & 3 – Article 9 – Epitheorese Klinikes Farmakologias και Farmakokinetikes-International Edition

By | | Emanuel Escher, Roger Bosse, Sylvain Gagnon, Άρθρο επισκόπησης - Review Article, Δημήτριος Θεοδωρόπουλος - Dimitrios Theodoropoulos, Εύη Μάνεση-Ζούπα - Evy Manessi-Zoupa, Ουρανία Μπέλτε - Urania Belte, Παύλος Κορδοπάτης - Paul Cordopatis, Πλήρες Κείμενο στα Αγγλικά - Full Text in English
Title Synthesis and biological activities of angiotensin II analogues containing α-aminoisobutyric acid
Authors Paul Cordopatis1, Urania Belte1, Evy Manessi-Zoupa2, Dimitrios Theodoropoulos2, Roger Bosse3, Sylvain Gagnon3 and Emanuel Escher3

1. Department of Pharmacy and

2. Department of Chemistry, University of Patras, 265 00 Patra, Greece

3. Department of Pharmacology, University of Sherbrooke, Quebec J1H 5N4, Canada
Citation Cordopatis, P., Belte, U., Manessi-Zoupa, E., Theodoropoulos, D., Bosse, R. et al.: Synthesis and biological activities of angiotensin II analogues containing α-aminoisobutyric acid, Epitheorese Klin. Farmakol. Farmakokinet. 9(2-3): 89-92 (1995)
Publication Date 1995
Full Text Language English
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Keywords Peptide synthesis, angiotensin II, α-aminoisobutyric acid analogues.
Other Terms review article
Summary Six analogues of angiotensin II (AT) were synthesized with modifications in position 1 and 7. Previous studies indicate that α,α dimethylation of Gly1 (aminoisobutyric acid, Aib) produced quite potent analogues, as did N-methylation of Gly1 (sarcosine). Combination of both, Cα and Nα méthylations to N-Me-Aib1 reduces, however, affinity in a drastic manner. Décyclisation of the Pro7-residue produced moderately active analogues with position 7N-methylation and inactive analogues if the N-alkylation was su-pressed. In order to investigate a possible interdependence of positions 1 and 7, a series of peptides with combinations of position 1 and 7 alkylations were investigated. The following analogues were prepared by solid phase synthesis: [Sar¹, Aib7]AT, [Sar1, Aib7, Leu8]AT, [Aib1,7 ]AT, [Aib1,7,Leu8]AT, [N-Me-Aib1,7, Leu8]AT. The biological properties of these peptides were assessed on the rabbit aorta preparation and their binding potencies were measured on bovine adrenal membranes. Both on agonistic and antagonistic analogues single Aib substitutions either in position 1 or 7 induced minor affinity modifications in both bioassays. Simultaneous Aib modifications in position 1 and 7 induced severe affinity loss in both bioassays. Agonistic Aib7 analogues have all reduced intrinsic activity, indicating an influence of this position on the activation mechanism of the AT receptor of the AT1 type.
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