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结合等温滴定量热法和时间分辨荧光法研究高亲和力抗体-配体相互作用的热力学和动力学。

Combination of isothermal titration calorimetry and time-resolved luminescence for high affinity antibody-ligand interaction thermodynamics and kinetics.

机构信息

Chemistry Department, University of California, Davis, CA 95616, USA.

出版信息

Methods. 2012 Feb;56(2):145-53. doi: 10.1016/j.ymeth.2011.09.011. Epub 2011 Sep 20.

Abstract

For experiments using synthetic ligands as probes for biological experiments, it is useful to determine the specificity and affinity of the ligands for their receptors. As ligands with higher affinities are developed (K(A)>10(8)M(-1); K(D)<10(-8)M), a new challenge arises: to measure these values accurately. Isothermal titration calorimetry measures heat produced or consumed during ligand binding, and also provides the equilibrium binding constant. However, as normally practiced, its range is limited. Displacement titration, where a competing weaker ligand is used to lower the apparent affinity of the stronger ligand, can be used to determine the binding affinity as well as the complete thermodynamic data for ligand-antibody complexes with very high affinity. These equilibrium data have been combined with kinetic measurements to yield the rate constants as well. We describe this methodology, using as an example antibody 2D12.5, which captures yttrium S-2-(4-aminobenzyl)-1, 4, 7, 10-tetraazacyclododecanetetraacetate.

摘要

对于使用合成配体作为生物实验探针的实验,确定配体与其受体的特异性和亲和力是很有用的。随着具有更高亲和力的配体的发展(K(A)>10(8)M(-1); K(D)<10(-8)M),出现了一个新的挑战:准确测量这些值。等温滴定量热法测量配体结合过程中产生或消耗的热量,并提供平衡结合常数。然而,按照通常的做法,其范围是有限的。置换滴定法,其中使用竞争较弱的配体来降低较强配体的表观亲和力,可用于确定结合亲和力以及具有非常高亲和力的配体-抗体复合物的完整热力学数据。这些平衡数据已经与动力学测量结合使用,以获得速率常数。我们使用抗体 2D12.5 作为示例描述了这种方法,该抗体可捕获钇 S-2-(4-氨基苄基)-1,4,7,10-四氮杂环十二烷四乙酸。

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