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Novel Chalcone-Based Fluorescent Human Histamine H3 Receptor Ligands as Pharmacological Tools

机译:新型基于查尔酮的荧光人组胺H3受体配体作为药理学工具

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摘要

Novel fluorescent chalcone-based ligands at human histamine H3 receptors (hH3R) have been designed, synthesized, and characterized. Compounds described are non-imidazole analogs of ciproxifan with a tetralone motif. Tetralones as chemical precursors and related fluorescent chalcones exhibit affinities at hH3R in the same concentration range like the reference antagonist ciproxifan (hH3R pKi value of 7.2). Fluorescence characterization of our novel ligands shows emission maxima about 570 nm for yellow fluorescent chalcones and ≥600 nm for the red fluorescent derivatives. Interferences to cellular autofluorescence could be excluded. All synthesized chalcone compounds could be used to visualize hH3R proteins in stably transfected HEK-293 cells using confocal laser scanning fluorescence microscopy. These novel fluorescent ligands possess high potential to be used as pharmacological tools for hH3R visualization in different tissues.
机译:已经设计,合成和表征了在人类组胺H3受体(hH3R)上基于荧光查尔酮的新型配体。所描述的化合物是具有四氢萘酮基序的非诺咪唑西非昔芬类似物。四氢萘酮作为化学前体和相关的荧光查耳酮在hH3R处的亲和力与参考拮抗剂ciproxifan相同,且浓度范围相同(hH3R pKi值为7.2)。我们的新型配体的荧光特性显示,黄色荧光查耳酮的发射最大值约为570 nm,红色荧光衍生物的发射最大值约为≥600nm。可以排除对细胞自发荧光的干扰。使用共聚焦激光扫描荧光显微镜,所有合成的查尔酮化合物均可用于在稳定转染的HEK-293细胞中可视化hH3R蛋白。这些新颖的荧光配体具有很高的潜力,可用作在不同组织中可视化hH3R的药理学工具。

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