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蛋白A树脂上的多克隆和单克隆IgG结合——竞争性结合效应的证据。

Polyclonal and monoclonal IgG binding on protein A resins-Evidence of competitive binding effects.

作者信息

Weinberg Justin, Zhang Shaojie, Crews Gillian, Healy Edward, Carta Giorgio, Przybycien Todd

机构信息

Department of Chemical Engineering, Carnegie Mellon University, 5000 Forbes Avenue, Pittsburgh, Pennsylvania 15213.

Department of Chemical Engineering, University of Virginia, 102 Engineers' Way, Charlottesville, Virginia 22904.

出版信息

Biotechnol Bioeng. 2017 Aug;114(8):1803-1812. doi: 10.1002/bit.26286. Epub 2017 Jun 6.

DOI:10.1002/bit.26286
PMID:28294302
Abstract

Protein A (ProA) chromatography is used extensively in the biopharmaceutical industry for the selective capture of both polyclonal and monoclonal antibodies (mAbs). This work provides a comparison of the adsorptive behavior of a highly heterogeneous polyclonal hIgG versus that of a mAb as well as the behavior of their mixtures on representative ProA resins. Both pH gradient elution and frontal loading experiments using human polyclonal IgG (hIgG) reveal a distribution of IgG-ProA binding strengths likely associated with multiple IgG subclasses and the heterogeneity of the variable region. pH gradient analysis of fractions collected along the breakthrough curve demonstrate a clear progression from weaker binding (higher pH eluting) to stronger binding (lower pH eluting) IgG species leaving the column suggesting the possibility of stronger binding species displacing the weaker binding ones. Displacement is directly observed by visualizing the adsorption of fluorescently labeled mAb and hIgG using confocal laser scanning microscopy (CLSM). Here, the displacement of hIgG results in a broad adsorption front compared to the sharp, "shrinking core" behavior typically observed with mAbs. Sequential CLSM adsorption experiments with a mAb and hIgG confirm that stronger or equivalent-binding hIgG species are able to displace and desorb bound mAb molecules. These phenomena are examined using a variety of ProA resins including CaptivA PriMAB, MabSelect, and MabSelect SuRe to understand the effect of different ligand properties on binding strength and competition among different IgG species. The results of these comparisons suggest that the competition kinetics are slower with ligands that have a single-point covalent attachment to the base matrix compared to a multi-point attachment. Biotechnol. Bioeng. 2017;114: 1803-1812. © 2017 Wiley Periodicals, Inc.

摘要

蛋白A(ProA)色谱法在生物制药行业中被广泛用于选择性捕获多克隆抗体和单克隆抗体(mAb)。这项工作比较了高度异质的多克隆人IgG与单克隆抗体的吸附行为,以及它们在代表性ProA树脂上的混合物行为。使用人多克隆IgG(hIgG)进行的pH梯度洗脱和前沿加载实验均表明,IgG与ProA的结合强度分布可能与多种IgG亚类以及可变区的异质性有关。沿穿透曲线收集的馏分的pH梯度分析表明,离开色谱柱的IgG种类从较弱结合(较高pH洗脱)到较强结合(较低pH洗脱)有明显的变化,这表明较强结合的种类有可能取代较弱结合的种类。通过共聚焦激光扫描显微镜(CLSM)观察荧光标记的单克隆抗体和hIgG的吸附情况,直接观察到了取代现象。在这里,与通常观察到的单克隆抗体的尖锐“收缩核”行为相比,hIgG的取代导致了较宽的吸附前沿。用单克隆抗体和hIgG进行的连续CLSM吸附实验证实,较强或等效结合的hIgG种类能够取代并解吸结合的单克隆抗体分子。使用多种ProA树脂(包括CaptivA PriMAB、MabSelect和MabSelect SuRe)对这些现象进行了研究,以了解不同配体性质对结合强度以及不同IgG种类之间竞争的影响。这些比较结果表明,与多点连接的配体相比,与基础基质单点共价连接的配体的竞争动力学较慢。《生物技术与生物工程》2017年;114:1803 - 1812。©2017威利期刊公司

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