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某些内源性和合成 TSPO 配体与 rs6971 多态性的结合亲和力。

Binding Affinity of Some Endogenous and Synthetic TSPO Ligands Regarding the rs6971 Polymorphism.

机构信息

Division of Nuclear Medicine, Department of Biomedical Imaging and Image-guided Therapy, Medical University of Vienna, 1090 Vienna, Austria.

Department of Inorganic Chemistry, University of Vienna, 1090 Vienna, Austria.

出版信息

Int J Mol Sci. 2019 Jan 29;20(3):563. doi: 10.3390/ijms20030563.

DOI:10.3390/ijms20030563
PMID:30699908
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6387295/
Abstract

An intriguing target involved in several pathophysiological processes is the 18 kDa translocator protein (TSPO), of which exact functions remained elusive until now. A single nucleotide polymorphism in the gene influences the binding affinity of endogenous and synthetic TSPO ligands by facilitating a lower-affinity conformation, which modifies a potential ligand binding site, ultimately leading to a binding profile classification according to each genotype. For instance, some clinical effects of the distinctive binding affinity profile of cholesterol toward the TSPO of individuals with different genotypes have been extensively discussed. Therefore, we conducted an investigation based on a radioligand binding assay, to determine the inhibition constants of some reported endogenous TSPO ligands (diazepam binding inhibitor and protoporphyrin IX), as well as synthetic ligands (disulfiram and derivatives). We observed no dependency of the polymorphism on the binding affinity of the evaluated endogenous ligands, whereas a high dependency on the binding affinity of the tested synthetic ligands was evident.

摘要

一个涉及多种病理生理过程的有趣靶点是 18kDa 转位蛋白(TSPO),其确切功能至今仍不清楚。 基因中的单核苷酸多态性通过促进低亲和力构象来影响内源性和合成 TSPO 配体的结合亲和力,从而改变潜在的配体结合位点,最终根据每种基因型进行结合谱分类。 例如,已经广泛讨论了不同基因型个体的胆固醇对 TSPO 的独特结合亲和力谱的一些临床影响。 因此,我们进行了一项基于放射性配体结合测定的研究,以确定一些报道的内源性 TSPO 配体(地西泮结合抑制剂和原卟啉 IX)以及合成配体(戒酒硫和衍生物)的抑制常数。 我们没有观察到多态性与评估的内源性配体的结合亲和力之间的依赖性,而对于测试的合成配体的结合亲和力则存在高度依赖性。

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