Opioid peptides. Synthesis and biological properties of dermorphin related hexapeptides

## Abstract Two tris‐alkoxycarbonyl homoarginine derivatives, Boc‐Har{ω,ω′‐[Z(2Br)]~2~}‐OH and Boc‐Har{ω,ω′‐[Z(2Cl)]~2~}‐OH, were prepared by guanidinylation of Boc‐Lys‐OH, and used for the synthesis of neo‐endorphins and dynorphins. The results were compared with that obtained in the synthesis in

## Abstract The syntheses of [D‐Ala^2^, Car^4^, Leu^5^]‐enkephalin, its amide, and of [D‐Ala^2^, Car^4^, Met^5^]‐enkephalin amide are described in detail. The three compounds show pronounced morphine‐like potencies in certain bio‐assays, and were used to investigate the influence of electronic, ste

## Abstract The syntheses of seven [D‐ala‐^2^]‐enkephalin analogues, H‐Tyr‐ala‐Gly‐X‐Y, with X‐Y = Phe‐Ada‐OH, Phe‐ada‐OH, Phe‐Ada‐NH~2~, Phe‐ada‐NH~2~, Ada‐Leu‐OH, Ada‐Leu‐NH~2~, and Ada‐Ada‐NH~2~ are described. The compounds with Y = Ada (= L‐Ada) or ada (= D‐Ada) show pronounced morphine‐like ac

The synthesis of the first all-aza-amino acid analogue (2) of a peptidic renin inhibitor is described. The X-ray structural analysis and molecular modelling investigations of this novel compound reveal interesting conformational features which have a significant impact on its biological activity. In