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Dynamic titration: Determination of dissociation constants for noncovalent complexes in multiplexed format using HPLC-ESI-MS

机译:动态滴定:使用HPLC-ESI-MS测定多重形式的非共价复合物的解离常数

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摘要

With recent growth in fields such as life sciences and supramolecular chemistry, there has been an ever increasing need for high-throughput methods that would permit determination of binding affinities for noncovalent complexes of various host-guest systems. These are traditionally measured by titration experiments where concentration-dependent signals of species participating in solution-based binding equilibria are monitored by methods such as UV-vis spectrophotometry, calorimetry, or nuclear magnetic resonance spectrometry. Here we present a new titration technique that unifies and allows chromatographic separation of guests with determination of dissociation constants by electrospray mass spectrometry in a multiplexed format. A theoretical model has been derived that describes the complex formation for the guests eluted from a chromatographic column. when hosts are admixed postcolumn. The model takes possible competition equilibria into account; i.e., it can deal with unresolved peaks of guests with the possible addition of multiple hosts in one experiment. This on-line workflow makes determination of binding affinities for large libraries of compounds possible. The potential of the method is demonstrated on the determination of dissociation constants for complexes of beta- and gamma-cyclodextrins with nonsteroidal antiinflammatory drugs ibuprofen, naproxen, and flurbiprofen.
机译:随着诸如生命科学和超分子化学等领域的最新发展,对高通量方法的需求不断增长,该方法可以确定各种宿主-客体系统的非共价复合物的结合亲和力。传统上,这些是通过滴定实验来测量的,其中通过诸如紫外可见分光光度法,量热法或核磁共振波谱法等方法来监测参与基于溶液的结合平衡的物种的浓度依赖性信号。在这里,我们介绍了一种新的滴定技术,该技术可通过电喷雾质谱法以多路形式统一并允许客人进行色谱分离,并确定解离常数。已经得到了一个理论模型,该模型描述了从色谱柱上洗脱下来的客体的复杂形成。当宿主混合后柱。该模型考虑了可能的竞争均衡。也就是说,它可以通过在一个实验中添加多个主机来处理来宾未解决的高峰。这种在线工作流程使确定大型化合物库的结合亲和力成为可能。该方法的潜力在测定β-和γ-环糊精与非甾体抗炎药布洛芬,萘普生和氟比洛芬的复合物的解离常数时得到了证明。

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