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首页> 外文期刊>European journal of pharmaceutical sciences >Viscosity of high concentration protein formulations of monoclonal antibodies of the IgG1 and IgG4 subclass - Prediction of viscosity through protein-protein interaction measurements
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Viscosity of high concentration protein formulations of monoclonal antibodies of the IgG1 and IgG4 subclass - Prediction of viscosity through protein-protein interaction measurements

机译:IgG1和IgG4亚类单克隆抗体的高浓度蛋白质制剂的粘度-通过蛋白质-蛋白质相互作用测量预测粘度

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The purpose of this work was to explore the relation between protein-protein interactions (PPIs) and solution viscosity at high protein concentration using three monoclonal antibodies (mAbs), two of the IgG 4 subclass and one of the IgG1 subclass. A range of methods was used to quantify the PPI either at low concentration (interaction parameter (kD) obtained from dynamic light scattering, DLS) or at high concentration (solution storage modulus (G′) from ultrasonic shear rheology). We also developed a novel method for the determination of PPI using the apparent radius of the protein at either low or high protein concentration determined using DLS. The PPI measurements were correlated with solution viscosity (measured by DLS using polystyrene nanospheres and ultrasonic shear rheology) as a function of pH (4-9) and ionic strength (10, 50 and 150 mM). Our measurements showed that the highest solution viscosity was observed under conditions with the most negative kD, the highest apparent radius and the lowest net charge. An increase in ionic strength resulted in a change in the nature of the PPI at low pH from repulsive to attractive. In the neutral to alkaline pH region the mAbs behaved differently with respect to increase in ionic strength. Two mAbs (A and B) showed little or no effect of increasing ionic strength, whereas mAb-C showed a remarkable decrease in attractive PPI and viscosity. Previous studies have mainly investigated mAbs of the IgG 1 and IgG2 subclass. We show here, for the first time, that mAbs of the IgG4 subclass behave similar as the other subclasses. By comparison of the three tested mAbs with mAbs investigated in other studies a clear linear trend emerges between the pH of strongest attractive PPI and highest solution viscosity. The determination of PPI using either kD or apparent radius is thus a useful prediction tool in the determination of solution conditions that favors low solution viscosity at high protein concentration of therapeutically used mAb molecules. The novel methodology using apparent radius is a simple and rapid alternative to determine relative PPI directly under formulation conditions. The method can potentially serve as a high-throughput screening tool in formulation development.
机译:这项工作的目的是使用三种单克隆抗体(mAb),两种IgG 4子类别和一种IgG1子类别,探索高蛋白浓度下蛋白质-蛋白质相互作用(PPI)与溶液粘度之间的关系。在低浓度(从动态光散射获得的相互作用参数(kD),DLS)或高浓度(从超声剪切流变学获得的溶液储能模量(G'))中,使用了多种方法来定量PPI。我们还开发了一种使用DLS测定的低或高蛋白浓度下的蛋白表观半径测定PPI的新方法。 PPI测量值与溶液粘度(通过使用聚苯乙烯纳米球和超声剪切流变学的DLS测量)的溶液粘度相关,该值随pH(4-9)和离子强度(10、50和150 mM)而变化。我们的测量表明,在最大负kD,最大表观半径和最低净电荷的条件下观察到最高溶液粘度。离子强度的增加导致低pH下PPI的性质从排斥变为吸引。在中性至碱性pH范围内,mAb随离子强度的增加而表现不同。两种mAb(A和B)几乎没有或没有提高离子强度的作用,而mAb-C却显示出有吸引力的PPI和粘度显着降低。先前的研究主要研究了IgG 1和IgG2亚类的mAb。我们首次在这里显示IgG4子类的mAb的行为与其他子类相似。通过将三种测试的mAb与其他研究中研究的mAb进行比较,在最强的吸引力PPI的pH和最高的溶液粘度之间出现了明显的线性趋势。因此,使用kD或表观半径确定PPI是确定溶液条件的有用预测工具,该条件有利于在治疗用mAb分子的高蛋白浓度下降低溶液粘度。使用表观半径的新颖方法是直接在配方条件下确定相对PPI的简单快捷方法。该方法可以潜在地用作制剂开发中的高通量筛选工具。

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