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A deconvolution method for the separation of specific versus nonspecific interactions in noncovalent protein-ligand complexes analyzed by ESI-FT-ICR mass spectrometry.

机译:通过ESI-FT-ICR质谱分析的非卷积方法,用于分离非共价蛋白-配体复合物中的特异性和非特异性相互作用。

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摘要

A method to separate specific and nonspecific noncovalent interactions observed in ESI mass spectra between a protein and its ligands is presented. Assuming noncooperative binding, the specific ligand binding is modeled as a statistical distribution on identical binding sites. For the nonspecific fraction we assume a statistical distribution on a large number of "nonspecific" interacting sites. The model was successfully applied to the noncovalent interaction between the protein creatine kinase (CK) and its ligands adenosine diphosphate (ADP) and adenosine triphosphate (ATP) that both exhibit nonspecific binding in the mass spectrum. The two sequential dissociation constants obtained by applying our method are K(1,diss) = 11.8 +/- 1.5 microM and K(2,diss) = 48 +/- 6 microM for ADP. For ATP, the constants are K(1,diss) = 27 +/- 7 microM and K(2,diss) = 114 +/- 27 microM. All constants are in good correlation with reported literature values. The model should be valuable for systems with a large dissociation constant that require high ligand concentrations and thus have increased potential of forming nonspecific adducts.
机译:提出了一种分离蛋白质和其配体之间在ESI质谱图中观察到的特异性和非特异性非共价相互作用的方法。假定非合作结合,将特异性配体结合建模为相同结合位点上的统计分布。对于非特异性部分,我们假设大量“非特异性”相互作用位点的统计分布。该模型已成功应用于蛋白质肌酸激酶(CK)及其配体之间的非共价相互作用,后者在质谱中均表现出非特异性结合,二磷酸腺苷(ADP)和三磷酸腺苷(ATP)。通过应用我们的方法获得的两个顺序解离常数是ADP的K(1,diss)= 11.8 +/- 1.5 microM和K(2,diss)= 48 +/- 6 microM。对于ATP,常数为K(1,diss)= 27 +/- 7 microM和K(2,diss)= 114 +/- 27 microM。所有常数与报道的文献值具有良好的相关性。该模型对于具有高解离常数,需要高配体浓度并因此具有增加形成非特异性加合物的潜力的系统而言非常有价值。

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