[二甲基色胺转运体1](Dmt1)DALDA与DAMGO在μ、δ和κ阿片受体结合及G蛋白激活方面的比较。
Comparison of [Dmt1]DALDA and DAMGO in binding and G protein activation at mu, delta, and kappa opioid receptors.
作者信息
Zhao Guo-Min, Qian Xuanxuan, Schiller Peter W, Szeto Hazel H
机构信息
Department of Pharmacology, Weill Medical College of Cornell University, 1300 York Ave., New York, NY 10021, USA.
出版信息
J Pharmacol Exp Ther. 2003 Dec;307(3):947-54. doi: 10.1124/jpet.103.054775. Epub 2003 Oct 8.
[Dmt1]DALDA (H-Dmt-d-Arg-Phe-Lys-NH2; Dmt = 2',6'-dimethyltyrosine) binds with high affinity and selectivity to the mu opioid receptor and is a surprisingly potent and long-acting analgesic, especially after intrathecal administration. In an attempt to better understand the unique pharmacological profile of [Dmt1]DALDA, we have prepared [3H][Dmt1]DALDA and compared its binding properties with that of [3H]DAMGO ([d-Ala2,N-Me-Phe4,Gly5-ol]-enkephalin). Kinetic studies revealed rapid association of [3H][Dmt1]DALDA when incubated with mouse brain membranes (K+1 = 0.155 nM(-1) min(-1)). Dissociation of [3H][Dmt1]DALDA was also rapid (K(-1) = 0.032 min(-1)) and indicated binding to a single site. [3H][Dmt1]DALDA binds with very high affinity to human mu opioid receptor (hMOR) (Kd = 0.199 nM), and Kd and Bmax were reduced by sodium but not Gpp(NH)p [guanosine 5'-(beta,gamma-imido)triphosphate]. Similar Kd values were obtained in brain and spinal cord tissues and SH-SY5Y cells. The hMOR:hDOR (human delta opioid receptor) selectivity of [Dmt1]DALDA ( approximately 10,000) is 8-fold higher than DAMGO. However, [Dmt1]DALDA is less selective than DAMGO against hKOR (human kappa opioid receptor) (26-versus 180-fold). The Ki values for a number of opioid ligands were generally higher when determined by competitive displacement binding against [3H][Dmt1]DALDA compared with [3H]DAMGO, with the exception of Dmt1-substituted peptide analogs. All Dmt1 analogs showed much higher affinity for the mu receptor than corresponding Tyr1 analogs. [35S]GTPgammaS (guanosine 5'-O -(3-[35S]thio)triphosphate) binding showed that [Dmt1]DALDA and DAMGO are full agonists at hMOR and hDOR but are only partial agonists at hKOR. The very high affinity and selectivity of [3H][Dmt1]DALDA for the mu receptor, together with its very low nonspecific binding (10-15%) and metabolic stability, make [3H][Dmt1]DALDA an ideal radioligand for labeling mu receptors.
[Dmt1]DALDA(H-Dmt-d-Arg-Phe-Lys-NH2;Dmt = 2',6'-二甲基酪氨酸)与μ阿片受体具有高亲和力和选择性结合,是一种出奇有效且长效的镇痛药,尤其是在鞘内给药后。为了更好地理解[Dmt1]DALDA独特的药理学特征,我们制备了[3H][Dmt1]DALDA,并将其结合特性与[3H]DAMGO([d-Ala2,N-Me-Phe4,Gly5-ol]-脑啡肽)的结合特性进行了比较。动力学研究表明,[3H][Dmt1]DALDA与小鼠脑膜孵育时结合迅速(K+1 = 0.155 nM(-1) min(-1))。[3H][Dmt1]DALDA的解离也很快(K(-1) = 0.032 min(-1)),表明其与单一位点结合。[3H][Dmt1]DALDA与人μ阿片受体(hMOR)具有非常高的亲和力(Kd = 0.199 nM),并且Kd和Bmax因钠而降低,但不因Gpp(NH)p[鸟苷5'-(β,γ-亚氨基)三磷酸]而降低。在脑和脊髓组织以及SH-SY5Y细胞中获得了相似的Kd值。[Dmt1]DALDA对hMOR:hDOR(人δ阿片受体)的选择性(约10,000)比DAMGO高8倍。然而,[Dmt1]DALDA对hKOR(人κ阿片受体)的选择性低于DAMGO(26倍对180倍)。与[3H]DAMGO相比,当通过与[3H][Dmt1]DALDA竞争置换结合来测定时,许多阿片样物质配体的Ki值通常更高,但Dmt1取代的肽类似物除外。所有Dmt1类似物对μ受体的亲和力都比相应的Tyr1类似物高得多。[35S]GTPγS(鸟苷5'-O-(3-[35S]硫代)三磷酸)结合表明,[Dmt1]DALDA和DAMGO在hMOR和hDOR上是完全激动剂,但在hKOR上只是部分激动剂。[3H][Dmt1]DALDA对μ受体具有非常高的亲和力和选择性,以及其非常低的非特异性结合(10 - 15%)和代谢稳定性,使得[3H][Dmt1]DALDA成为标记μ受体的理想放射性配体。
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