内源性大麻素转运体和脂肪酸酰胺水解酶抑制剂的药理学特性
Pharmacological characterization of endocannabinoid transport and fatty acid amide hydrolase inhibitors.
作者信息
Dickason-Chesterfield Amy K, Kidd Stephanie R, Moore Steven A, Schaus John M, Liu Bin, Nomikos George G, Felder Christian C
机构信息
Eli Lilly & Company, Lilly Research Laboratories, Lilly Corporate Center, Indianapolis, Indiana 46285, USA.
出版信息
Cell Mol Neurobiol. 2006 Jul-Aug;26(4-6):407-23. doi: 10.1007/s10571-006-9072-6. Epub 2006 May 31.
: 1. The mechanism of anandamide uptake and disposal has been an issue of considerable debate in the cannabinoid field. Several compounds have been reported to inhibit anandamide uptake or fatty acid amide hydrolase (FAAH; the primary catabolic enzyme of anandamide) activity with varying degrees of potency and selectivity. We recently reported the first evidence of a binding site involved in the uptake of endocannabinoids that is independent from FAAH. There are no direct comparisons of purported selective inhibitory compounds in common assay conditions measuring anandamide uptake, FAAH activity and binding activity. 2. A subset of compounds reported in the literature were tested in our laboratory under common assay conditions to measure their ability to (a) inhibit [(14)C]-anandamide uptake in cells containing (RBL-2H3) or cells lacking (HeLa) FAAH, (b) inhibit purified FAAH hydrolytic activity, and (c) inhibit binding to a putative binding site involved in endocannabinoid transport in both RBL and HeLa cell membranes. 3. Under these conditions, nearly all compounds tested inhibited (a) uptake of [(14)C]-anandamide, (b) enzyme activity in purified FAAH preparations, and (c) radioligand binding of [(3)H]-LY2183240 in RBL and HeLa plasma membrane preparations. General rank order potency was preserved within the three assays. However, concentration response curves were right-shifted for functional [(14)C]-anandamide uptake in HeLa (FAAH(-/-)) cells. 4. A more direct comparison of multiple inhibitors could be made in these three assay systems performed in the same laboratory, revealing more information about the selectivity of these compounds and the relationship between the putative endocannabinoid transport protein and FAAH. At least two separate proteins appear to be involved in uptake and degradation of anandamide. The most potent inhibitory compounds were right-shifted when transport was measured in HeLa (FAAH(-/-)) cells suggesting a requirement for a direct interaction with the FAAH protein to maintain high affinity binding of anandamide or inhibitors to the putative anandamide transport protein.
- 花生四烯乙醇胺的摄取和代谢机制一直是大麻素领域中一个备受争议的问题。据报道,几种化合物能以不同程度的效力和选择性抑制花生四烯乙醇胺的摄取或脂肪酸酰胺水解酶(FAAH;花生四烯乙醇胺的主要分解代谢酶)的活性。我们最近报道了首个与内源性大麻素摄取相关的独立于FAAH的结合位点的证据。在测量花生四烯乙醇胺摄取、FAAH活性和结合活性的常见实验条件下,尚未对所谓的选择性抑制化合物进行直接比较。2. 文献中报道的一部分化合物在我们实验室的常见实验条件下进行了测试,以测定它们的以下能力:(a) 抑制含有(RBL - 2H3)或缺乏(HeLa)FAAH的细胞中[¹⁴C] - 花生四烯乙醇胺的摄取,(b) 抑制纯化的FAAH水解活性,以及(c) 抑制RBL和HeLa细胞膜中与内源性大麻素转运相关的假定结合位点的结合。3. 在这些条件下,几乎所有测试的化合物都抑制了:(a) [¹⁴C] - 花生四烯乙醇胺的摄取,(b) 纯化的FAAH制剂中的酶活性,以及(c) RBL和HeLa质膜制剂中[³H] - LY2183240的放射性配体结合。在这三种测定中,一般的效价顺序得以保留。然而,HeLa(FAAH(-/-))细胞中功能性[¹⁴C] - 花生四烯乙醇胺摄取的浓度 - 反应曲线向右移动。4. 在同一实验室进行的这三种测定系统中,可以对多种抑制剂进行更直接的比较,从而揭示有关这些化合物选择性以及假定的内源性大麻素转运蛋白与FAAH之间关系的更多信息。至少有两种不同的蛋白质似乎参与了花生四烯乙醇胺的摄取和降解。当在HeLa(FAAH(-/-))细胞中测量转运时,最有效的抑制化合物的曲线向右移动,这表明需要与FAAH蛋白直接相互作用,以维持花生四烯乙醇胺或抑制剂与假定的花生四烯乙醇胺转运蛋白的高亲和力结合。
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