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Pulsed Ultrafiltration Mass Spectrometry: A New Method for Screening Combinatorial Libraries

机译:脉冲超滤质谱:筛选组合库的新方法

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In response to the need for rapid screening of combinatorial libraries to identify new lead compounds during drug discovery., we have developed an on-line combination of ultrafiltration and electrospray mass spectrometry, called pulsed ultrafiltration mass spectrometry, which facilitates the identification of solution-phase ligands in library mixtures that bind to solution-phase receptors. After ligands contained in a library mixture were bound to a macromolecular receptor, e.g., human serum albumin or calf intestine adenosine deaminase, the ligand-receptor complexes were purified by ultrafiltration and then dissociated using methanol to elute the ligands into the electrospray mass spectrometer for detection. Ligands with dissociation constants in the micromolar to nanomolar range were successfully bound, released, and detected using this method, including warfarin, salicylate, furosemide, and thyroxine binding to human serum albumin, and erythro-9-(2-hydroxy-3-nonyl)adenine binding to calf intestine adenosine deaminase. Repetitive bind-and-release experiments demonstrated that the receptor could be reused. Thus, pulsed ultrafiltration mass spectrometry was shown to provide a simple and powerful new method for the screening of combinatorial libraries in support of new drug discovery.
机译:为响应在药物发现过程中需要快速筛选组合库以鉴定新的先导化合物的需求,我们开发了超滤和电喷雾质谱的在线组合,称为脉冲超滤质谱,可促进溶液相的鉴定库混合物中与溶液相受体结合的配体。将文库混合物中包含的配体与大分子受体(例如人血清白蛋白或小牛肠腺苷脱氨酶)结合后,通过超滤纯化配体-受体复合物,然后使用甲醇解离,将其洗脱到电喷雾质谱仪中进行检测。使用这种方法可以成功地结合,释放和检测具有离解常数在微摩尔至纳摩尔范围内的配体,包括华法林,水杨酸酯,呋塞米和甲状腺素与人血清白蛋白的结合以及erythro-9-(2-hydroxy-3-nonyl腺嘌呤与小牛肠腺苷脱氨酶的结合。重复的结合和释放实验表明该受体可以重复使用。因此,显示出脉冲超滤质谱法提供了一种简单而强大的新方法来筛选组合库,以支持新药的发现。

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