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Cell-membrane coated iron oxide nanoparticles for isolation and specific identification of drug leads from complex matrices

机译:细胞膜包覆的纳米氧化铁隔离和特定药物的识别从复杂的矩阵

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摘要

The lack of suitable tools for the identification of potential drug leads from complex matrices is a bottleneck in drug discovery. Here, we report a novel method to screen complex matrices for new drug leads targeting transmembrane receptors. Using (34) nicotinic receptors as a model system, we successfully demonstrated the ability of this new tool for the specific identification and effective extraction of binding compounds from complex mixtures. The formation of cell-membrane coated nanoparticles was confirmed by transmission electron microscopy. In particular, we have developed a direct tool to evaluate the presence of functional (34) nicotinic receptors on the cell membrane. The specific ligand binding to (34) nicotinic receptors was examined through ligand fishing experiments and confirmed by high-performance liquid chromatography coupled with diode-array detection and electrospray ionization mass spectrometry. This tool has a great potential to transform the drug discovery process focusing on identification of compounds targeting transmembrane proteins, as more than 50% of all modern pharmaceuticals use membrane proteins as prime targets.
机译:缺乏合适的工具来识别潜在的药物先导物从复杂的矩阵一个瓶颈在药物发现。小说屏幕复杂矩阵的新方法药物先导物针对跨膜受体。使用尼古丁受体(34)作为一个模型系统,我们成功地展示了这样的能力具体的识别和新工具结合化合物的有效提取复杂的混合物。证实了涂层纳米颗粒透射电子显微镜。我们已经开发出一种直接评估工具功能(34)烟碱受体的存在在细胞膜上。(34)烟碱受体是通过检查配体实验,证实了钓鱼高效液相色谱法耦合与二极管阵列检测和电喷射电离质谱分析。巨大的潜力将药物发现过程关注化合物的识别针对跨膜蛋白,如超过50%的所有现代制药使用膜蛋白质作为首要目标。

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