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Capture compound mass spectrometry: a technology for the investigation of small molecule protein interactions.

机译:捕获化合物质谱法:一种研究小分子蛋白质相互作用的技术。

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摘要

One of the major hurdles in the post-genomic era is to understand the function of genes and the interplay of many different cellular proteins. This is especially important for drug development. Capture compound mass spectrometry (CCMS) addresses this challenge by selectively reducing the complexity of the proteome. Capture compounds are trifunctional molecules: a selectivity function reversibly interacts via affinity with proteins; a reactivity function irreversibly forms a covalent bond outside the affinity binding site; and a sorting/pullout function allows the captured protein(s) to be isolated from cellular lysate for mass spectrometric analysis and characterization by database queries. In the present study, we demonstrate the use of a CCMS capture compound with a sulfonamide drug analog as its selectivity function, isolating an expected target protein from cell lysates containing a large excess of other "non-target" proteins. A future application of CCMS is to define or confirm drug target proteins and their mechanisms of drug action, or to discover off-target proteins that cause side effects, enabling subsequent drug structure optimization.
机译:后基因组时代的主要障碍之一是了解基因的功能以及许多不同细胞蛋白的相互作用。这对于药物开发尤其重要。捕获化合物质谱法(CCMS)通过选择性降低蛋白质组的复杂性来应对这一挑战。捕获化合物是三功能分子:选择性功能通过与蛋白质的亲和力可逆地相互作用;反应功能在亲和结合位点外不可逆地形成共价键;排序/提取功能可将捕获的蛋白质从细胞裂解物中分离出来,以通过数据库查询进行质谱分析和鉴定。在本研究中,我们证明了使用具有磺酰胺药物类似物的CCMS捕获化合物作为其选择性功能,可以从含有大量过量其他“非目标”蛋白质的细胞裂解物中分离出预期的目标蛋白质。 CCMS的未来应用是定义或确认药物靶蛋白及其药物作用机制,或发现引起副作用的脱靶蛋白,从而实现后续的药物结构优化。

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