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Molecular characterization of an enzyme that degrades neuromodulatory fatty-acid amides.

机译:降解神经调节性脂肪酸酰胺的酶的分子特征。

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Endogenous neuromodulatory molecules are commonly coupled to specific metabolic enzymes to ensure rapid signal inactivation. Thus, acetylcholine is hydrolysed by acetylcholine esterase and tryptamine neurotransmitters like serotonin are degraded by monoamine oxidases. Previously, we reported the structure and sleep-inducing properties of cis-9-octadecenamide, a lipid isolated from the cerebrospinal fluid of sleep-deprived cats. cis-9-Octadecenamide, or oleamide, has since been shown to affect serotonergic systems and block gap-junction communication in glial cells (our unpublished results). We also identified a membrane-bound enzyme activity that hydrolyses oleamide to its inactive acid, oleic acid. We now report the mechanism-based isolation, cloning and expression of this enzyme activity, originally named oleamide hydrolase, from rat liver plasma membranes. We also show that oleamide hydrolase converts anandamide, a fatty-acid amide identified as the endogenous ligand for the cannabinoid receptor, toarachidonic acid, indicating that oleamide hydrolase may serve as the general inactivating enzyme for a growing family of bioactive signalling molecules, the fatty-acid amides. Therefore we will hereafter refer to oleamide hydrolase as fatty-acid amide hydrolase, in recognition of the plurality of fatty-acid amides that the enzyme can accept as substrates.
机译:内源性神经调节分子通常与特定的代谢酶偶联,以确保快速的信号灭活。因此,乙酰胆碱酯酶会水解乙酰胆碱,单胺氧化酶会降解色胺素之类的色胺类神经递质。以前,我们报道了顺式9-十八烯酰胺(一种从睡眠不足的猫的脑脊液中分离出来的脂质)的结构和诱导睡眠的特性。自那以后,已证明顺式9-十八碳酰胺或油酰胺会影响血清素能系统并阻断神经胶质细胞中的间隙连接通讯(我们未发表的结果)。我们还确定了一种膜结合酶活性,该酶将油酰胺水解成其非活性酸油酸。现在,我们从大鼠肝脏质膜报道这种酶活性(最初称为油酰胺水解酶)的基于机制的分离,克隆和表达。我们还显示,油酰胺水解酶可将anandamide转化为一种脂肪酸酰胺,该脂肪酸酰胺被确定为大麻素受体toarachidonic acid的内源性配体,表明该油酰胺水解酶可能充当了生物活性信号分子不断增长的家族的一般失活酶,酰胺。因此,在下文中我们将油酰胺水解酶称为脂肪酸酰胺水解酶,因为该酶可以接受作为底物的多种脂肪酸酰胺。

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