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微流控压力装置可分离切变力和界面协同作用对抗体聚集的影响。

Microfluidic Stress Device to Decouple the Synergistic Effect of Shear and Interfaces on Antibody Aggregation.

机构信息

Department of Chemistry and Applied Biosciences, Institute for Chemical and Bioengineering, ETH Zurich, Zurich, Switzerland.

Janssen Cilag AG, Schaffhausen, Switzerland.

出版信息

J Pharm Sci. 2024 Aug;113(8):2161-2169. doi: 10.1016/j.xphs.2024.05.024. Epub 2024 May 25.

DOI:10.1016/j.xphs.2024.05.024
PMID:38801973
Abstract

Protein denaturation and aggregation resulting from the effects of interfacial stress, often enhanced by flow and shear stress, pose significant challenges in the production of therapeutic proteins and monoclonal antibodies. The influence of flow on protein stability is closely intertwined with interfacial effects. In this study, we have developed a microfluidic device capable of exposing low volume (< 320 µL) protein solutions to highly uniform shear. To disentangle the synergistic impact of flow and interfaces on protein aggregation, we fabricated two devices composed of different materials, namely poly(methyl methacrylate) (PMMA) and stainless steel. Upon application of shear, we observed formation of protein particles in the micron-size range. Notably, The number of particles generated in the steel devices was ∼ 3.5 fold lower than in the PMMA device, hinting at an interface-mediated effect. With increasing the protein concentration from 1 to 50 mg/mL we observed a saturation in the amount of aggregates, further confirming the key role of solid-liquid interfaces in inducing particle formation. Introduction of non-ionic surfactants prevented protein aggregation, even at the highest tested protein concentration and low surfactant concentrations of 0.05 mg/mL. Overall, our findings corroborate the synergistic impact of shear and interface effects on protein aggregation. The device developed in this study offers a small-scale platform for assessing the stability of antibody formulations throughout various stages of the development and manufacturing process.

摘要

蛋白质的变性和聚集是由于界面应力的影响,常常受到流动和切应力的增强,这给治疗性蛋白质和单克隆抗体的生产带来了重大挑战。流动对蛋白质稳定性的影响与界面效应密切相关。在这项研究中,我们开发了一种微流控装置,能够使低体积(<320μL)的蛋白质溶液暴露于高度均匀的剪切力下。为了厘清流动和界面协同作用对蛋白质聚集的影响,我们制造了两种由不同材料组成的装置,即聚甲基丙烯酸甲酯(PMMA)和不锈钢。在施加剪切力后,我们观察到蛋白质颗粒在微米级范围内形成。值得注意的是,在不锈钢装置中生成的颗粒数量比在 PMMA 装置中少约 3.5 倍,这暗示了界面介导的效应。随着蛋白质浓度从 1mg/mL 增加到 50mg/mL,我们观察到聚集物的数量达到饱和,进一步证实了固液界面在诱导颗粒形成中的关键作用。引入非离子表面活性剂即使在最高测试蛋白质浓度和低表面活性剂浓度(0.05mg/mL)下也能防止蛋白质聚集。总的来说,我们的研究结果证实了剪切力和界面效应协同作用对蛋白质聚集的影响。本研究中开发的装置提供了一个小规模的平台,可用于评估抗体配方在开发和制造过程的各个阶段的稳定性。

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