Bifunctional pharmacophores. Biological activities of the peptide analog containing both casomorphine-like and substance P antagonist-like active elements.

A W Lipkowski, K Misterek
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引用次数: 0

Abstract

SP-antagonistic properties of a newly synthesized peptide Tyr-Pro-D-Phe-Phe-D-Phe-D-Trp-MetNH2 (AWL-60) were investigated both in vitro and in vivo. In vitro AWL-60 effectively antagonized the action of SP-agonist (SP6-11); however, this antagonism was non-competitive. Antagonistic properties of AWL-60 were also observed in vivo: in doses as low as 0.1 nmol/kg iv AWL-60 markedly attenuated the fall in blood pressure produced by [less than Glu]6SP6-11. Since AWL-60 exerts weak opioid agonistic properties (as a casomorphine analog) the possible involvement of an opioid agonistic component in their SP inhibitory action is considered.

双官能团的药效团。含有卡索啡样和P物质拮抗剂样活性成分的肽类似物的生物活性。
在体外和体内研究了新合成肽tyr1 - pro - d - phe - phe - d - phe - d - trp - metnh2 (AWL-60)的sp拮抗特性。AWL-60在体外能有效拮抗sp -激动剂(SP6-11)的作用;然而,这种对抗是非竞争性的。在体内也观察到AWL-60的拮抗特性:在低至0.1 nmol/kg的剂量下,AWL-60显著减弱[低于Glu]6SP6-11引起的血压下降。由于AWL-60具有较弱的阿片受体激动特性(作为卡啡啡类似物),因此考虑了阿片受体激动成分可能参与其SP抑制作用。
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