IQM-95,333的药理学评价，一种在动物模型中具有抗焦虑样活性的高选择性CCKA受体拮抗剂。

Pharmacological evaluation of IQM-95,333, a highly selective CCKA receptor antagonist with anxiolytic-like activity in animal models.

作者信息

Ballaz S, Barber A, Fortuño A, Del Río J, Martin-Martínez M, Gómez-Monterrey I, Herranz R, González-Muñiz R, García-López M T

机构信息

Department of Physiology and Pharmacology, University of Navarra, Pamplona, Spain.

出版信息

Br J Pharmacol. 1997 Jun;121(4):759-67. doi: 10.1038/sj.bjp.0701186.

DOI:10.1038/sj.bjp.0701186

PMID:9208145

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1564744/

Abstract

The pyridopyrimidine derivative IQM-95,333 ((4aS,5R)-2-benzyl-5-[N alpha-tert-butoxicarbonyl)L-tryptophyl] amino-1,3dioxoperhydropyrido[1,2-c]pyrimidine), a new non-peptide antagonist of cholecystokinin type A (CCKA) receptors, has been evaluated in vitro and in vivo in comparison with typical CCKA and CCKB receptor antagonists, such as devazepide, lorglumide, L-365,260 and PD-135,158. 2. IQM-95,333 displaced [3H]-CCK-8S binding to CCKA receptors from rat pancreas with a high potency in the nanomolar range. Conversely, the affinity of this new compound at brain CCKB receptors was negligible (IC50 > 10 microM). IQM-95,333 was a more selective CCKA receptor ligand than devazepide and other CCKA receptor antagonists. 3. Like devazepide, IQM-95,333 was a more potent antagonist of CCK-8S- than of CCK-4-induced contraction of the longitudinal muscle from guinea-pig ileum, suggesting selective antagonism at CCKA receptors. 4. IQM-95,333 and devazepide were also potent inhibitors of CCK-8S-stimulated amylase release from isolated pancreatic acini, a CCKA receptor-mediated effect. The drug concentrations required (IC50s around 20 nM) were higher than in binding studies to pancreas homogenates. 5. Low doses (50-100 micrograms kg-1, i.p.) of IQM-95,333 and devazepide, without any intrinsic effect on food intake or locomotion, blocked the hypophagia and the hypolocomotion induced by systemic administration of CCK-8S, two effects associated with stimulation of peripheral CCKA receptors. 6. IQM-95,333 showed an anxiolytic-like profile in the light/dark exploration test in mice over a wide dose range (10-5,000 micrograms kg-1). Typical CCKA and CCKB antagonists, devazepide and L-365,260 respectively, were only effective within a more limited dose range. 7. In a classical conflict paradigm for the study of anxiolytic drugs, the punished-drinking test, IQM-95,333, devazepide and L-365,260 were effective within a narrow dose range. The dose-response curve for the three drugs was biphasic, suggesting that other mechanisms are operative at higher doses. 8. In conclusion, IQM-95,333 is a potent and selective CCKA receptor antagonist both in vitro and in vivo with an anxiolytic-like activity in two different animal models, which can only be attributed to blockade of this CCK receptor subtype.

摘要

吡啶并嘧啶衍生物IQM - 95,333（(4aS,5R)-2-苄基-5-[Nα-叔丁氧羰基）L-色氨酰]氨基-1,3-二氧代全氢吡啶并[1,2 - c]嘧啶），一种新型的A 型胆囊收缩素（CCKA）受体非肽拮抗剂，已与典型的CCKA和CCKB受体拮抗剂（如地伐西匹、氯谷胺、L - 365,260和PD - 135,158）进行了体外和体内评估。2. IQM - 95,333以纳摩尔范围内的高效力取代[3H]-CCK - 8S与大鼠胰腺CCKA受体的结合。相反，这种新化合物对脑CCKB受体的亲和力可忽略不计（IC50＞10μM）。IQM - 95,333是比地伐西匹和其他CCKA受体拮抗剂更具选择性的CCKA受体配体。3. 与地伐西匹一样，IQM - 95,333对CCK - 8S诱导的豚鼠回肠纵肌收缩的拮抗作用比对CCK - 4诱导的收缩更强，表明对CCKA受体具有选择性拮抗作用。4. IQM - 95,333和地伐西匹也是CCK - 8S刺激离体胰腺腺泡淀粉酶释放的有效抑制剂，这是一种CCKA受体介导的效应。所需药物浓度（IC50约为20 nM）高于与胰腺匀浆结合研究中的浓度。5. 低剂量（50 - 100μg kg-1，腹腔注射）的IQM - 95,333和地伐西匹对食物摄入或运动没有任何内在影响，但能阻断全身注射CCK - 8S诱导的食欲减退和运动减少，这两种效应与外周CCKA受体的刺激有关。6. 在小鼠明暗探索试验中，IQM - 95,333在很宽的剂量范围（10 - 5,000μg kg-1）内呈现出抗焦虑样特征。典型的CCKA和CCKB拮抗剂，即地伐西匹和L - 365,260，仅在更有限的剂量范围内有效。7. 在用于研究抗焦虑药物的经典冲突范式即罚饮试验中，IQM - 95,333、地伐西匹和L -

365,260在狭窄的剂量范围内有效。这三种药物的剂量反应曲线是双相的，表明在较高剂量下有其他机制起作用。8. 总之，IQM - 95,333在体外和体内都是一种强效且选择性的CCKA受体拮抗剂，在两种不同的动物模型中具有抗焦虑样活性，这只能归因于对该CCK受体亚型的阻断。