Strong uterotonic inhibitors – analogs of 1-deamino-8-D-homoarginine-vasopressin with <i>p</i>-substituted phenylalanine in position 2

Žertová, Miroslava; Procházka, Zdenko; Barth, Tomislav; Slaninová, Jiřina; Škopková, Jana; Bláha, Ivo; Lebl, Michal

doi:10.1135/cccc19911761

CCCC > Archive > 1991, Volume 56 > Issue 8 > p. 1761

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Strong uterotonic inhibitors – analogs of 1-deamino-8-D-homoarginine-vasopressin with p-substituted phenylalanine in position 2

Miroslava Žertová, Zdenko Procházka, Tomislav Barth, Jiřina Slaninová, Jana Škopková, Ivo Bláha and Michal Lebl

Institute of Organic Chemistry and Biochemistry, Czechoslovak Academy of Sciences, 166 10 Prague 6

Abstract

Solid phase methodology on benzhydrylamine or p-methylbenzhydrylamine resin was used for the synthesis of five analogs of deamino-vasopressin with non-coded amino acids. D-homoarginine, in position 8 and p-substituted D- or L-phenylalanine in position 2. Besides the mother analog, [Mpr¹, D-Har⁸]vasopressin (I), [Mpr¹, L-Phe(p-Me)², D-Har⁸]vasopressin (II), [Mpr¹, D-Phe(p-Me)²,D-Har⁸]vasopressin (III), [Mpr¹, L-Phe(p-Et)², D-Har⁸]vasopressin (IV) and [Mpr¹, D-Phe(p-Et)², D-Har⁸]vasopressin (V) were synthesized. All analogs have very low antidiuretic and pressor activities. Analogs containing p-methylphenylalanine of L-configuration and p-ethylphenylalanine of both D- and L-configuration are pressor inhibitors. All analogs substituted in position 2 were found to act as the uterotonic inhibitors, the most potent being [Mpr¹, D-Phe(p-Et)², D-Har⁸]vasopressin (V) with pA₂ = 8.30.

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Strong uterotonic inhibitors – analogs of 1-deamino-8-D-homoarginine-vasopressin with p-substituted phenylalanine in position 2

Abstract