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一种荧光香豆素探针的协同转运将香豆素标记为有机阴离子转运多肽OATP3A1的药理学调节剂。

Synergistic transport of a fluorescent coumarin probe marks coumarins as pharmacological modulators of Organic anion-transporting polypeptide, OATP3A1.

作者信息

Bakos Éva, Tusnády Gábor E, Német Orsolya, Patik Izabel, Magyar Csaba, Németh Krisztina, Kele Péter, Özvegy-Laczka Csilla

机构信息

Membrane Protein Research Group, Institute of Enzymology, RCNS, H-1117 Budapest, Magyar tudósok krt. 2., Budapest, Hungary.

Bioinformatics Research Group, Institute of Enzymology, RCNS, H-1117 Budapest, Magyar tudósok krt. 2., Budapest, Hungary.

出版信息

Biochem Pharmacol. 2020 Dec;182:114250. doi: 10.1016/j.bcp.2020.114250. Epub 2020 Sep 28.

DOI:10.1016/j.bcp.2020.114250
PMID:32991865
Abstract

Organic anion-transporting polypeptide 3A1 (OATP3A1) is a membrane transporter mediating the cellular uptake of various hormones such as estrone-3-sulfate, prostaglandins E1 and E2 and thyroxine. OATP3A1 is widely expressed in the human body and its presence in tissue-blood barriers, neurons and muscle cells marks it as a potential pharmacological target. Herein we demonstrate that an otherwise membrane impermeant, zwitterionic fluorescent coumarin probe, bearing a sulfonate function is a potent substrate of human OATP3A1, thus readily transported into HEK-293-OATP3A1 cells allowing functional investigation and the screen of drug interactions of the OATP3A1 transporter. At the same time, dyes lacking either the sulfonate motif or the coumarin scaffold showed a dramatic decrease in affinity or even a complete loss of transport. Furthermore, we observed a distinct inhibition/activation pattern in the OATP3A1-mediated uptake of closely related fluorescent coumarin derivatives differing only in the presence of the sulfonate moiety. Additionally, we detected a synergistic effect between one of the probes tested and the endogenous OATP substrate estrone-3-sulfate. These data, together with docking results indicate the presence of at least two cooperative substrate binding sites in OATP3A1. Besides providing the first sensitive probe for testing OATP3A1 substrate/inhibitor interactions, our results also help to understand substrate recognition and transport mechanism of the poorly characterized OATP3A1. Moreover, coumarins are good candidates for OATP3A1-targeted drug delivery and as pharmacological modulators of OATP3A1.

摘要

有机阴离子转运多肽3A1(OATP3A1)是一种膜转运蛋白,介导多种激素的细胞摄取,如硫酸雌酮、前列腺素E1和E2以及甲状腺素。OATP3A1在人体中广泛表达,其在组织-血屏障、神经元和肌肉细胞中的存在使其成为一个潜在的药理学靶点。在此,我们证明了一种带有磺酸酯功能的两性离子荧光香豆素探针,尽管其原本不能透过细胞膜,但却是人OATP3A1的有效底物,因此能轻易转运到HEK-293-OATP3A1细胞中,从而允许对OATP3A1转运蛋白进行功能研究和药物相互作用筛选。同时,缺乏磺酸酯基序或香豆素支架的染料在亲和力上显著降低,甚至完全丧失转运能力。此外,我们观察到在OATP3A1介导的仅在磺酸酯部分存在差异的密切相关荧光香豆素衍生物摄取中存在明显的抑制/激活模式。此外,我们检测到所测试的一种探针与内源性OATP底物硫酸雌酮之间存在协同效应。这些数据与对接结果表明OATP3A1中至少存在两个协同底物结合位点。除了提供首个用于测试OATP3A1底物/抑制剂相互作用的灵敏探针外,我们的结果还有助于理解特性尚不明确的OATP3A1的底物识别和转运机制。此外,香豆素是OATP3A1靶向药物递送的良好候选物,也是OATP3A1的药理学调节剂。

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