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内源性大麻素转运蛋白:用于研究固醇载体蛋白-2的工具的发现。

Endocannabinoid Transport Proteins: Discovery of Tools to Study Sterol Carrier Protein-2.

作者信息

Hillard Cecilia J, Huang Huan, Vogt Caleb D, Rodrigues Beatriz E, Neumann Terrence S, Sem Daniel S, Schroeder Friedhelm, Cunningham Christopher W

机构信息

Medical College of Wisconsin, Milwaukee, WI, United States.

Texas A&M University, TVMC, College Station, TX, United States.

出版信息

Methods Enzymol. 2017;593:99-121. doi: 10.1016/bs.mie.2017.06.017. Epub 2017 Jul 17.

Abstract

The endocannabinoid (eCB) neurotransmitter system regulates diverse neurological functions including stress and anxiety, pain, mood, and reward. Understanding the mechanisms underlying eCB regulation is critical for developing targeted pharmacotherapies to treat these and other neurologic disorders. Cellular studies suggest that the arachidonate eCBs, N-arachidonoylethanolamine (AEA) and 2-arachidonoylglycerol (2-AG), are substrates for intracellular binding and transport proteins, and several candidate proteins have been identified. Initial evidence from our laboratory indicates that the lipid transport protein, sterol carrier protein 2 (SCP-2), binds to the eCBs and can regulate their cellular concentrations. Here, we present methods for evaluating SCP-2 binding of eCBs and their application to the discovery of the first inhibitor lead molecules. Using a fluorescent probe displacement assay, we found SCP-2 binds the eCBs, AEA (K=0.68±0.05μM) and 2-AG (K=0.37±0.02μM), with moderate affinity. A series of structurally diverse arachidonate analogues also bind SCP-2 with K values between 0.82 and 2.95μM, suggesting a high degree of tolerance for arachidonic acid head group modifications in this region of the protein. We also report initial structure-activity relationships surrounding previously reported inhibitors of Aedis aegypti SCP-2, and the results of an in silico high-throughput screen that identified structurally novel SCP-2 inhibitor leads. The methods and results reported here provide the basis for a robust probe discovery effort to fully elucidate the role of facilitated transport mediated by SCP-2 in eCB regulation and function.

摘要

内源性大麻素(eCB)神经递质系统调节多种神经功能,包括应激和焦虑、疼痛、情绪及奖赏。了解eCB调节的潜在机制对于开发针对性的药物疗法以治疗这些及其他神经系统疾病至关重要。细胞研究表明,花生四烯酸eCBs、N-花生四烯酰乙醇胺(AEA)和2-花生四烯酰甘油(2-AG)是细胞内结合和转运蛋白的底物,并且已经鉴定出几种候选蛋白。我们实验室的初步证据表明,脂质转运蛋白、固醇载体蛋白2(SCP-2)与eCBs结合,并可调节其细胞浓度。在此,我们介绍评估SCP-2与eCBs结合的方法及其在发现首个抑制剂先导分子中的应用。使用荧光探针置换试验,我们发现SCP-2以中等亲和力结合eCBs、AEA(K=0.68±0.05μM)和2-AG(K=0.37±0.02μM)。一系列结构多样的花生四烯酸类似物也以0.82至2.95μM之间的K值结合SCP-2,这表明该蛋白区域对花生四烯酸头部基团修饰具有高度耐受性。我们还报告了围绕先前报道的埃及伊蚊SCP-2抑制剂的初步构效关系,以及计算机高通量筛选的结果,该筛选鉴定出了结构新颖的SCP-2抑制剂先导物。本文报道的方法和结果为全面阐明SCP-2介导的促进转运在eCB调节和功能中的作用的强大探针发现工作提供了基础。

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