2-萘磺酰基-L-天冬氨酰-(2-苯乙基)酰胺(2-NAP)——一种选择性胆囊收缩素CCKA受体拮抗剂。
2-Naphthalenesulphonyl L-aspartyl-(2-phenethyl)amide (2-NAP)--a selective cholecystokinin CCKA-receptor antagonist.
作者信息
Hull R A, Shankley N P, Harper E A, Gerkowitch V P, Black J W
机构信息
James Black Foundation, King's College School of Medicine & Dentistry, London.
出版信息
Br J Pharmacol. 1993 Mar;108(3):734-40. doi: 10.1111/j.1476-5381.1993.tb12870.x.
Abstract
- The in vitro pharmacological characterization of the sodium salt of 2-naphthalenesulphonyl 1-aspartyl-(2-phenethyl)amide [2-NAP], a hydrophilic compound derived from the C-terminal aspartate-phenylalanine dipeptide of cholecystokinin (CCK), is described. 2. 2-NAP behaved as a competitive antagonist of sulphated cholecystokinin octapeptide (CCK-8) at CCKA-receptors in both intact tissue bioassays (guinea-pig gall bladder, pancreas and ileum, human and rabbit gall bladder) and a radioligand displacement assay (guinea-pig pancreatic cells). The mean pKB, over assays, was 6.5. 3. Compared to the other assays, the rabbit gall bladder assay gave a significantly higher pKB estimate [7.0] for 2-NAP and a significantly lower estimate [8.9] for devazepide (formerly L-364,718 and MK-329), a well-characterized CCKA-receptor antagonist; these anomalous results suggest that a different class of CCKA-receptors may be involved. 4. 2-NAP, was found to be highly selective, having at least 300 fold greater affinity for CCKA-receptors than for 50 other pharmacological loci, including gastrin/CCKB, as estimated by bioassay or radioligand displacement.
摘要
- 本文描述了2-萘磺酰基-1-天冬氨酰-(2-苯乙基)酰胺钠盐[2-NAP]的体外药理学特性,它是一种由胆囊收缩素(CCK)的C末端天冬氨酸-苯丙氨酸二肽衍生而来的亲水性化合物。2. 在完整组织生物测定(豚鼠胆囊、胰腺和回肠、人和兔胆囊)以及放射性配体置换测定(豚鼠胰腺细胞)中,2-NAP在CCKA受体上表现为硫酸化胆囊收缩素八肽(CCK-8)的竞争性拮抗剂。各测定的平均pKB为6.5。3. 与其他测定相比,兔胆囊测定对2-NAP给出了显著更高的pKB估计值[7.0],而对已充分表征的CCKA受体拮抗剂地伐西匹(原L-364,718和MK-329)给出了显著更低的估计值[8.9];这些异常结果表明可能涉及另一类CCKA受体。4. 通过生物测定或放射性配体置换估计,发现2-NAP具有高度选择性,对CCKA受体的亲和力比对包括胃泌素/CCKB在内的其他50个药理学位点至少高300倍。
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