盐酸(4-(双(4-氟苯基)甲基)哌嗪-1-基)(环己基)甲酮(LDK1229):一种新型的二苯甲基哌嗪类似物类大麻素CB1受体反向激动剂。
(4-(Bis(4-fluorophenyl)methyl)piperazin-1-yl)(cyclohexyl)methanone hydrochloride (LDK1229): a new cannabinoid CB1 receptor inverse agonist from the class of benzhydryl piperazine analogs.
作者信息
Mahmoud Mariam M, Olszewska Teresa, Liu Hui, Shore Derek M, Hurst Dow P, Reggio Patricia H, Lu Dai, Kendall Debra A
机构信息
Department of Molecular and Cell Biology, University of Connecticut, Storrs, Connecticut (M.M.M.); Irma Lerma Rangel College of Pharmacy, Texas A&M Health Science Center, Kingsville, Texas (T.O., H. L., D.L.); Department of Chemistry and Biochemistry, University of North Carolina at Greensboro, Greensboro, North Carolina (D.M.S., D.P.H., P.H.R.); and Department of Pharmaceutical Sciences, University of Connecticut, Storrs, Connecticut (D.A.K.).
Department of Molecular and Cell Biology, University of Connecticut, Storrs, Connecticut (M.M.M.); Irma Lerma Rangel College of Pharmacy, Texas A&M Health Science Center, Kingsville, Texas (T.O., H. L., D.L.); Department of Chemistry and Biochemistry, University of North Carolina at Greensboro, Greensboro, North Carolina (D.M.S., D.P.H., P.H.R.); and Department of Pharmaceutical Sciences, University of Connecticut, Storrs, Connecticut (D.A.K.)
出版信息
Mol Pharmacol. 2015 Feb;87(2):197-206. doi: 10.1124/mol.114.095471. Epub 2014 Nov 19.
Some inverse agonists of cannabinoid receptor type 1 (CB1) have been demonstrated to be anorectic antiobesity drug candidates. However, the first generation of CB1 inverse agonists, represented by rimonabant (SR141716A), otenabant, and taranabant, are centrally active, with a high level of psychiatric side effects. Hence, the discovery of CB1 inverse agonists with a chemical scaffold distinct from these holds promise for developing peripherally active CB1 inverse agonists with fewer side effects. We generated a new CB1 inverse agonist, (4-(bis(4-fluorophenyl)methyl)piperazin-1-yl)(cyclohexyl)methanone hydrochloride (LDK1229), from the class of benzhydryl piperazine analogs. This compound binds to CB1 more selectively than cannabinoid receptor type 2, with a Ki value of 220 nM. Comparable CB1 binding was also observed by analogs 1-[bis(4-fluorophenyl)methyl]-4-cinnamylpiperazine dihydrochloride (LDK1203) and 1-[bis(4-fluorophenyl)methyl]-4-tosylpiperazine hydrochloride (LDK1222), which differed by the substitution on the piperazine ring where the piperazine of LDK1203 and LDK1222 are substituted by an alkyl group and a tosyl group, respectively. LDK1229 exhibits efficacy comparable with SR141716A in antagonizing the basal G protein coupling activity of CB1, as indicated by a reduction in guanosine 5'-O-(3-thio)triphosphate binding. Consistent with inverse agonist behavior, increased cell surface localization of CB1 upon treatment with LDK1229 was also observed. Although docking and mutational analysis showed that LDK1229 forms similar interactions with the receptor as SR141716A does, the benzhydryl piperazine scaffold is structurally distinct from the first-generation CB1 inverse agonists. It offers new opportunities for developing novel CB1 inverse agonists through the optimization of molecular properties, such as the polar surface area and hydrophilicity, to reduce the central activity observed with SR141716A.
一些1型大麻素受体(CB1)反向激动剂已被证明是厌食性抗肥胖药物候选物。然而,以利莫那班(SR141716A)、奥替那班和塔那那班为代表的第一代CB1反向激动剂具有中枢活性,伴有高水平的精神副作用。因此,发现具有与这些不同化学骨架的CB1反向激动剂有望开发出副作用更少的外周活性CB1反向激动剂。我们从二苯甲基哌嗪类似物类别中生成了一种新的CB1反向激动剂,盐酸(4-(双(4-氟苯基)甲基)哌嗪-1-基)(环己基)甲酮(LDK1229)。该化合物与CB1的结合比2型大麻素受体更具选择性,Ki值为220 nM。1-[双(4-氟苯基)甲基]-4-肉桂基哌嗪二盐酸盐(LDK1203)和1-[双(4-氟苯基)甲基]-4-甲苯磺酰基哌嗪盐酸盐(LDK1222)的类似物也观察到了类似的CB1结合,它们的区别在于哌嗪环上的取代基,其中LDK1203和LDK1222的哌嗪分别被烷基和甲苯磺酰基取代。LDK1229在拮抗CB1的基础G蛋白偶联活性方面表现出与SR141716A相当的效力,如鸟苷5'-O-(3-硫代)三磷酸结合减少所示。与反向激动剂行为一致,在用LDK1229处理后也观察到CB1的细胞表面定位增加。尽管对接和突变分析表明LDK1229与受体形成的相互作用与SR141716A相似,但二苯甲基哌嗪骨架在结构上与第一代CB1反向激动剂不同。它为通过优化分子性质(如极性表面积和亲水性)来开发新型CB1反向激动剂提供了新机会,以减少SR141716A所观察到的中枢活性。
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