Boden P R, Higginbottom M, Hill D R, Horwell D C, Hughes J, Rees D C, Roberts E, Singh L, Suman-Chauhan N, Woodruff G N
Parke-Davis Neuroscience Research Centre, Addenbrookes Hospital Site, Cambridge, U.K.
J Med Chem. 1993 Mar 5;36(5):552-65. doi: 10.1021/jm00057a005.
The design, synthesis, and structure-activity relationships (SAR) for the development of selective dipeptoid ligands for both of the cholecystokinin (CCK) receptor subtypes CCK-A and CCK-B are described. The SAR developed is used to design a ligand with equal nanomolar binding affinity for both the CCK-A and CCK-B receptors. Example compounds such as [1R-[1 alpha[R*(R*)],2 beta]]-4-[[2-[[3-(1H-indol-3-yl)- 2-methyl-2-[[[(2-methylcyclohexyl)oxy]carbonyl]amino]-1- oxopropyl]-amino]-1-phenylethyl]amino]-4-oxo-butanoic acid (24c), (1R-trans)-N-[alpha-methyl-N-[[(2-methylcyclohexyl)oxy] carbonyl]-D-tryptophyl]-L-3-(phenylmethyl)-beta-alanine (28i), and N-[alpha-methyl-N-[(tricyclo[3.3.1.1]dec-2-yloxy) carbonyl]-D-tryptophanyl]-L-3-(phenylmethyl)-beta-alanine (30m) are CCK-B selective compounds having CCK-B binding affinities of IC50 = 3.9, 0.34, and 0.15 nM with a CCK-A/CCK-B ratio of 464, 53, and 170, respectively. Other compounds such as (1R-trans)-N-[alpha-methyl-N-[[(2-methylcyclohexyl)oxy]carbonyl]- L-tryptophyl]-D-3-(phenylmethyl)-beta-alanine (281) and N-(alpha-methyl-N-[(tricyclo[3.3.1.1]dec-2-yloxy)carbonyl]-L - tryptophyl]-D-3-(phenylmethyl)-beta-alanine (30p) are CCK-A-selective compounds having CCK-A binding affinities of IC50 = 7.9 and 2.82 nM with a CCK-A/CCK-B ratio of 0.007 and 0.01, respectively. Further to these, (1S-trans)-N-[alpha-methyl-N-[[(2-methylcyclohexyl)oxy] carbonyl]-D-tryptophyl]-L-3-(phenylmethyl)-beta-alanine (28h) is a mixed CCK-A/CCK-B ligand with a CCK-A binding affinity of IC50 = 3.9 nM and a CCK-B binding affinity of IC50 = 4.2, producing a CCK-A/CCK-B ratio of unity. The CCK-B selective compounds are shown to be antagonists in electrophysiological tests on the rat ventromedial nucleus of the hypothalamus with an equilibrium constant (Ke) value of 2.8 nM for 30m and are also shown to be anxiolytic in the mouse ligh/dark box test with a minimum effective dose of 0.01 mg/kg, sc, for 30m. The CCK-A selective compounds are also shown to be competitive antagonists by the inhibition of CCK-8S-evoked amylase secretion from pancreatic acinar cells with a Ke value of 16 nM for 30p. In electrophysiological tests on the rat dorsal raphé (an area rich in CCK-A receptors) 30p had a Ke value of 12.8 nM. The mixed CCK-A/CCK-B compound 28h showed antagonistic properties in both CCK-A and CCK-B models; thus it inhibited CCK-8S-evoked amylase secretion from pancreatic acinar cells and is anxiolytic in the light/dark box paradigm.(ABSTRACT TRUNCATED AT 400 WORDS)
本文描述了用于开发胆囊收缩素(CCK)受体亚型CCK - A和CCK - B的选择性二肽类配体的设计、合成及构效关系(SAR)。所建立的构效关系用于设计一种对CCK - A和CCK - B受体均具有纳摩尔级结合亲和力的配体。示例化合物如[1R - [1α[R*(R*)],2β]] - 4 - [[2 - [[3 - (1H - 吲哚 - 3 - 基)-2 - 甲基 - 2 - [[[(2 - 甲基环己基)氧基]羰基]氨基]-1 - 氧代丙基]-氨基]-1 - 苯乙基]氨基]-4 - 氧代丁酸(24c)、(1R - 反式)-N - [α - 甲基 - N - [[(2 - 甲基环己基)氧基]羰基]-D - 色氨酰]-L - 3 - (苯甲基)-β - 丙氨酸(28i)和N - [α - 甲基 - N - [(三环[3.3.1.1]癸 - 2 - 基氧基)羰基]-D - 色氨酰]-L - 3 - (苯甲基)-β - 丙氨酸(30m)是CCK - B选择性化合物,其CCK - B结合亲和力的IC50分别为3.9、0.34和0.15 nM,CCK - A/CCK - B比值分别为464、53和170。其他化合物如(1R - 反式)-N - [α - 甲基 - N - [[(2 - 甲基环己基)氧基]羰基]-L - 色氨酰]-D - 3 - (苯甲基)-β - 丙氨酸(281)和N - (α - 甲基 - N - [(三环[3.3.1.1]癸 - 2 - 基氧基)羰基]-L - 色氨酰]-D - 3 - (苯甲基)-β - 丙氨酸(30p)是CCK - A选择性化合物,其CCK - A结合亲和力的IC50分别为7.9和2.82 nM,CCK - A/CCK - B比值分别为0.007和0.01。此外,(1S - 反式)-N - [α - 甲基 - N - [[(2 - 甲基环己基)氧基]羰基]-D - 色氨酰]-L - 3 - (苯甲基)-β - 丙氨酸(28h)是一种CCK - A/CCK - B混合配体,其CCK - A结合亲和力的IC50为3.9 nM,CCK - B结合亲和力的IC50为4.2,CCK - A/CCK - B比值为1。在对大鼠下丘脑腹内侧核的电生理测试中,CCK - B选择性化合物显示为拮抗剂,30m的平衡常数(Ke)值为2.8 nM,并且在小鼠明暗箱试验中也显示为抗焦虑剂,30m的最小有效剂量为0.01 mg/kg,皮下注射。CCK - A选择性化合物通过抑制CCK - 8S诱导的胰腺腺泡细胞淀粉酶分泌也显示为竞争性拮抗剂,30p的Ke值为16 nM。在对大鼠背缝核(富含CCK - A受体的区域)的电生理测试中,30p的Ke值为12.8 nM。CCK - A/CCK - B混合化合物28h在CCK - A和CCK - B模型中均显示出拮抗特性;因此它抑制CCK - 8S诱导的胰腺腺泡细胞淀粉酶分泌,并且在明暗箱范式中是抗焦虑剂。(摘要截断于400字)
