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一种新型速激肽结合位点在大鼠脑中被鉴定,其特征为一种标记的伊索肽衍生物的特异性结合。

A new type of tachykinin binding site in the rat brain characterized by specific binding of a labeled eledoisin derivative.

作者信息

Beaujouan J C, Torrens Y, Viger A, Glowinski J

出版信息

Mol Pharmacol. 1984 Sep;26(2):248-54.

PMID:6207421
Abstract

A new ligand for investigating tachykinin-binding site subtypes was synthesized by coupling the 125I-Bolton and Hunter reagent to eledoisin (125I-BHE). Using a synaptosomal preparation (P2 fraction) of rat cerebral cortex, 125I-BHE was shown to bind with apparent high affinity (apparent Kd = 15.3 nM). When concentrations of up to 30 nM 125I-BHE were used, 125I-BHE binding was specific, saturable, reversible, and temperature-dependent. In contrast to [3H]dopamine, 125I-BHE was not taken up within synaptosomes by an ouabain-sensitive process. Eledoisin, kassinin, and substance P were examined for their ability to inhibit specific 125I-BHE binding to cortical synaptosomes. Eledoisin and kassinin were considerably more potent than substance P, in contrast to the order of potency observed for specific 125I-Bolton-Hunter substance P (125I-BHSP) binding. Specific 125I-BHE binding was highest in the cerebral cortex and hypothalamus; intermediate in the hippocampus, striatum, and thalamus; low in the mesencephalon, septum, and substantia nigra; and absent in the cerebellum. Comparison of these data with those previously obtained for 125I-BHSP binding to synaptosomes indicated that 125I-BHE-labeled binding sites differ markedly from those of 125I-BHSP-labeled binding sites. Therefore, tachykinin receptors other than substance P receptors seem to be present in the central nervous system.

摘要

通过将125I-博尔顿和亨特试剂与伊氏缩胆囊肽(125I-BHE)偶联,合成了一种用于研究速激肽结合位点亚型的新型配体。使用大鼠大脑皮层的突触体制剂(P2组分),结果显示125I-BHE以明显的高亲和力结合(表观Kd = 15.3 nM)。当使用高达30 nM的125I-BHE浓度时,125I-BHE的结合具有特异性、饱和性、可逆性且依赖温度。与[3H]多巴胺不同,125I-BHE不是通过哇巴因敏感过程被摄取到突触体内。检测了伊氏缩胆囊肽、卡辛宁和P物质抑制125I-BHE与皮层突触体特异性结合的能力。与特异性125I-博尔顿-亨特P物质(125I-BHSP)结合所观察到的效力顺序相反,伊氏缩胆囊肽和卡辛宁的效力比P物质强得多。特异性125I-BHE结合在大脑皮层和下丘脑最高;在海马、纹状体和丘脑居中;在中脑、隔区和黑质较低;在小脑中不存在。将这些数据与先前获得的125I-BHSP与突触体结合的数据进行比较表明,125I-BHE标记的结合位点与125I-BHSP标记的结合位点明显不同。因此,中枢神经系统中似乎存在除P物质受体之外的速激肽受体。

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