Surfactant Effects on Particle Generation in Antibody Formulations in Pre-filled Syringes

肺表面活性物质 硅油 化学 吸附 粒子(生态学) 化学工程 色谱法 聚山梨酯 蛋白质吸附 硅酮 粒径 全内反射荧光显微镜 材料科学 有机化学 生物化学 物理化学 工程类 地质学 海洋学
作者
Alana Gerhardt,Aaron C. McUmber,Bao H. Nguyen,Rachael A. Lewus,Daniel K. Schwartz,John F. Carpenter,Theodore W. Randolph
出处
期刊:Journal of Pharmaceutical Sciences [Elsevier BV]
卷期号:104 (12): 4056-4064 被引量:41
标识
DOI:10.1002/jps.24654
摘要

Protein aggregation and particle formation have been observed when protein solutions contact hydrophobic interfaces, and it has been suggested that this undesirable phenomenon may be initiated by interfacial adsorption and subsequent gelation of the protein. The addition of surfactants, such as polysorbate 20, to protein formulations has been proposed as a way to reduce protein adsorption at silicone oil–water interfaces and mitigate the production of aggregates and particles. In an accelerated stability study, monoclonal antibody formulations containing varying concentrations of polysorbate 20 were incubated and agitated in pre-filled glass syringes (PFS), exposing the protein to silicone oil–water interfaces at the siliconized syringe walls, air–water interfaces, and agitation stress. Following agitation in siliconized syringes that contained an air bubble, lower particle concentrations were measured in the surfactant-containing antibody formulations than in surfactant-free formulations. Polysorbate 20 reduced particle formation when added at concentrations above or below the critical micelle concentration (CMC). The ability of polysorbate 20 to decrease particle generation in PFS corresponded with its ability to inhibit gelation of the adsorbed protein layer, which was assessed by measuring the interfacial diffusion of individual antibody molecules at the silicone oil–water interface using total internal reflectance fluorescence (TIRF) microscopy with single-molecule tracking.

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