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流式细胞术:研究蛋白质制剂中硅油诱导颗粒形成的有前途的技术。

Flow cytometry: a promising technique for the study of silicone oil-induced particulate formation in protein formulations.

机构信息

University of Colorado Center for Pharmaceutical Biotechnology, Department of Chemical and Biological Engineering, University of Colorado, Boulder, CO 80309, USA.

出版信息

Anal Biochem. 2011 Mar 15;410(2):191-9. doi: 10.1016/j.ab.2010.12.008. Epub 2010 Dec 10.

Abstract

Subvisible particles in formulations intended for parenteral administration are of concern in the biopharmaceutical industry. However, monitoring and control of subvisible particulates can be complicated by formulation components, such as the silicone oil used for the lubrication of prefilled syringes, and it is difficult to differentiate microdroplets of silicone oil from particles formed by aggregated protein. In this study, we demonstrate the ability of flow cytometry to resolve mixtures comprising subvisible bovine serum albumin (BSA) aggregate particles and silicone oil emulsion droplets with adsorbed BSA. Flow cytometry was also used to investigate the effects of silicone oil emulsions on the stability of BSA, lysozyme, abatacept, and trastuzumab formulations containing surfactant, sodium chloride, or sucrose. To aid in particle characterization, the fluorescence detection capabilities of flow cytometry were exploited by staining silicone oil with BODIPY 493/503 and model proteins with Alexa Fluor 647. Flow cytometric analyses revealed that silicone oil emulsions induced the loss of soluble protein via protein adsorption onto the silicone oil droplet surface. The addition of surfactant prevented protein from adsorbing onto the surface of silicone oil droplets. There was minimal formation of homogeneous protein aggregates due to exposure to silicone oil droplets, although oil droplets with surface-adsorbed trastuzumab exhibited flocculation. The results of this study demonstrate the utility of flow cytometry as an analytical tool for monitoring the effects of subvisible silicone oil droplets on the stability of protein formulations.

摘要

用于注射给药制剂的亚可见颗粒是生物制药行业关注的问题。然而,由于制剂成分(如用于预填充注射器润滑的硅油)的存在,对亚可见颗粒的监测和控制可能会变得复杂,并且很难将硅油的微液滴与聚集的蛋白质形成的颗粒区分开来。在这项研究中,我们证明了流式细胞术能够分辨包含亚可见牛血清白蛋白(BSA)聚集体颗粒和吸附有 BSA 的硅油乳液滴的混合物。流式细胞术还用于研究硅油乳液对含有表面活性剂、氯化钠或蔗糖的 BSA、溶菌酶、abatacept 和曲妥珠单抗制剂稳定性的影响。为了辅助颗粒特征分析,通过用 BODIPY 493/503 对硅油进行染色以及用 Alexa Fluor 647 对模型蛋白进行染色,利用流式细胞术的荧光检测能力。流式细胞术分析表明,硅油乳液通过将蛋白质吸附到硅油液滴表面,导致可溶性蛋白质的损失。表面活性剂的添加阻止了蛋白质吸附到硅油液滴表面。尽管表面吸附有曲妥珠单抗的油滴表现出絮凝,但由于暴露于硅油滴,很少形成均匀的蛋白质聚集体。这项研究的结果表明,流式细胞术可作为一种分析工具,用于监测亚可见硅油滴对蛋白质制剂稳定性的影响。

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