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苯二氮䓬受体的光亲和标记导致激动剂 - 拮抗剂相互作用改变。

Photoaffinity labeling of benzodiazepine receptors causes altered agonist-antagonist interactions.

作者信息

Thomas J W, Tallman J F

出版信息

J Neurosci. 1983 Feb;3(2):433-40. doi: 10.1523/JNEUROSCI.03-02-00433.1983.

Abstract

Previous studies have shown that [3H]flunitrazepam forms irreversible cross-links with brain tissue when exposed to ultraviolet irradiation. Comparison of the amount of [3H]flunitrazepam irreversibly incorporated and the number of benzodiazepine binding sites blocked after photolabeling has indicated that several binding sites are inactivated for each molecule of [3H]flunitrazepam incorporated. To learn the cause of this discrepancy, binding to the benzodiazepine binding sites has been examined using several radiolabeled benzodiazepine antagonists. Binding of a beta-carboline ester, CGS-8216, and Ro 15-1788 was not altered by photolabeling; however, displacement studies revealed that photolabeling converted a homogeneous set of benzodiazepine binding sites into two subsets: one of high affinity (unaltered sites) and one of low affinity. The low affinity sites could be detected by displacement studies of antagonist binding by benzodiazepines, and conversion to a low affinity form accounts for the discrepancy observed after photolabeling using [3H]flunitrazepam as ligand.

摘要

先前的研究表明,[3H]氟硝西泮在受到紫外线照射时会与脑组织形成不可逆的交联。对[3H]氟硝西泮不可逆掺入量与光标记后被阻断的苯二氮䓬结合位点数量进行比较,结果表明,每掺入一个[3H]氟硝西泮分子,就有几个结合位点失活。为了探究这种差异的原因,已使用几种放射性标记的苯二氮䓬拮抗剂研究了与苯二氮䓬结合位点的结合情况。β-咔啉酯CGS-8216和Ro 15-1788的结合不受光标记的影响;然而,置换研究表明,光标记将一组均匀的苯二氮䓬结合位点转化为两个亚组:一个高亲和力亚组(未改变的位点)和一个低亲和力亚组。低亲和力位点可通过苯二氮䓬对拮抗剂结合的置换研究来检测,转化为低亲和力形式解释了使用[3H]氟硝西泮作为配体进行光标记后观察到的差异。

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