棕榈酰乙醇胺的同系物和类似物对内源性大麻素花生四烯乙醇胺失活的影响。
Effects of homologues and analogues of palmitoylethanolamide upon the inactivation of the endocannabinoid anandamide.
作者信息
Jonsson K O, Vandevoorde S, Lambert D M, Tiger G, Fowler C J
机构信息
Department of Pharmacology and Clinical Neuroscience, Umeå University, SE-901 87 Umeå, Sweden.
出版信息
Br J Pharmacol. 2001 Aug;133(8):1263-75. doi: 10.1038/sj.bjp.0704199.
Abstract
- The ability of a series of homologues and analogues of palmitoylethanolamide to inhibit the uptake and fatty acid amidohydrolase (FAAH)-catalysed hydrolysis of [(3)H]-anandamide ([(3)H]-AEA) has been investigated. 2. Palmitoylethanolamide and homologues with chain lengths from 12 - 18 carbon atoms inhibited rat brain [(3)H]-AEA metabolism with pI(50) values of approximately 5. Homologues with chain lengths < or = eight carbon atoms gave < 20% inhibition at 100 microM. 3. R-palmitoyl-(2-methyl)ethanolamide, palmitoylisopropylamide and oleoylethanolamide inhibited [(3)H]-AEA metabolism with pI(50) values of 5.39 (competitive inhibition), 4.89 (mixed type inhibition) and 5.33 (mixed type inhibition), respectively. 4. With the exception of oleoylethanolamide, the compounds did not produce dramatic inhibition of [(3)H]-WIN 55,212-2 binding to human CB(2) receptors expressed on CHO cells. Palmitoylethanolamide, palmitoylisopropylamide and R-palmitoyl-(2-methyl)ethanolamide had modest effects upon [(3)H]-CP 55,940 binding to human CB(1) receptors expressed on CHO cells. 5. Most of the compounds had little effect upon the uptake of [(3)H]-AEA into C6 and/or RBL-2H3 cells. However, palmitoylcyclohexamide (100 microM) and palmitoylisopropylamide (30 and 100 microM) produced more inhibition of [(3)H]-AEA uptake than expected to result from inhibition of [(3)H]-AEA metabolism alone. 6. In intact C6 cells, palmitoylisopropylamide and oleoylethanolamide inhibited formation of [(3)H]-ethanolamine from [(3)H]-AEA to a similar extent as AM404, whereas palmitoylethanolamide, palmitoylcyclohexamide and R-palmitoyl-(2-methyl)ethanolamide were less effective. 7. These data provide useful information upon the ability of palmitoylethanolamide analogues to act as 'entourage' compounds. Palmitoylisopropylamide may prove useful as a template for design of compounds that reduce the cellular accumulation and metabolism of AEA without affecting either CB(1) or CB(2) receptors.
摘要
- 已对一系列棕榈酰乙醇胺的同系物和类似物抑制[(3)H]-花生四烯乙醇胺([(3)H]-AEA)摄取及脂肪酸酰胺水解酶(FAAH)催化的水解作用进行了研究。2. 棕榈酰乙醇胺及链长为12 - 18个碳原子的同系物抑制大鼠脑[(3)H]-AEA代谢,其半数抑制浓度(pI(50))值约为5。链长≤8个碳原子的同系物在100微摩尔时抑制率<20%。3. R-棕榈酰-(2-甲基)乙醇胺、棕榈酰异丙胺和油酰乙醇胺抑制[(3)H]-AEA代谢,其pI(50)值分别为5.39(竞争性抑制)、4.89(混合型抑制)和5.33(混合型抑制)。4. 除油酰乙醇胺外,这些化合物对[(3)H]-WIN 55,212-2与CHO细胞上表达的人CB(2)受体的结合未产生显著抑制。棕榈酰乙醇胺、棕榈酰异丙胺和R-棕榈酰-(2-甲基)乙醇胺对[(3)H]-CP 55,940与CHO细胞上表达的人CB(1)受体的结合有适度影响。5. 大多数化合物对[(3)H]-AEA进入C6和/或RBL-2H3细胞的摄取影响很小。然而,棕榈酰环己酰胺(100微摩尔)和棕榈酰异丙胺(30和100微摩尔)对[(3)H]-AEA摄取的抑制作用比仅由抑制[(3)H]-AEA代谢所预期的更大。6. 在完整的C6细胞中,棕榈酰异丙胺和油酰乙醇胺抑制[(3)H]-AEA生成[(3)H]-乙醇胺的程度与AM404相似,而棕榈酰乙醇胺、棕榈酰环己酰胺和R-棕榈酰-(2-甲基)乙醇胺的效果较差。7. 这些数据为棕榈酰乙醇胺类似物作为“随从”化合物的能力提供了有用信息。棕榈酰异丙胺可能被证明是设计减少AEA细胞内蓄积和代谢而不影响CB(1)或CB(2)受体的化合物的有用模板。
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