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环氧乙烷从灭菌塑料容器中的释放动力学模型及其与单克隆抗体的相互作用

Kinetic Modeling of the Release of Ethylene Oxide from Sterilized Plastic Containers and its Interaction with Monoclonal Antibodies.

作者信息

Yu Bryan Lei, Han Jun, Hammond Matthew, Wang Xuemei, Zhang Qingchun, Clausen Andrew, Forster Ronald, Eu Mingda

机构信息

Device Technologies, Process Development, Amgen Inc., Thousand Oaks, CA

Attribute Sciences, Process Development, Amgen Inc., Thousand Oaks, CA.

出版信息

PDA J Pharm Sci Technol. 2017;71(1):11-19. doi: 10.5731/pdajpst.2016.005819.

Abstract

UNLABELLED

Ethylene oxide (ETO) is commonly used to sterilize plastic containers, but the effects of residual amounts left after sterilization on protein therapeutics are still not well understood. Here we focus primarily on the factors that influence concentrations of ETO migrating from ETO-treated plastic containers into aqueous solution. A study was designed to investigate the kinetics of this process at various temperatures, and the kinetic data could be fit with a model based on a combination of Fickean diffusion and first-order chemical reaction (to account for observed hydrolysis of ETO). The diffusion and reaction rate constants thus obtained obey Arrhenius-like temperature dependence. These results indicate that for analytical methods involving extraction into water, measurements of residual ETO in a container must account for the effects of ETO hydrolysis. Further, the effects of salt concentration and pH of the fluid in the container on accumulated ETO levels were explored. Finally, interactions of ETO with anti-streptavidin (AntiSA) Immunoglobulin G1 (IgG1) and IgG2 antibodies were studied, with ETO adducts found on all methionine residues when incubated in solutions spiked with ETO at concentrations that could be reached (based on the kinetic studies) in ETO-treated plastic vials. Overall, the likelihood of observable ETO-protein modifications upon storage in ETO-sterilized containers will depend on a complex interplay of protein properties, formulation details, storage conditions, and amount of residual ETO initially in the container.

LAY ABSTRACT

Ethylene oxide (ETO) is commonly used to sterilize plastic containers, but the effects of residual amounts left after sterilization on protein therapeutics are still not well understood. Here we describe experiments exploring the factors that influence concentrations of ETO migrating from ETO-treated plastic containers into aqueous solution over time. Additionally, interactions of ETO with model antibodies were studied, with ETO adducts found on all methionine residues when incubated in solutions spiked with ETO at concentrations that could potentially be reached in ETO-treated plastic vials. Overall, the likelihood of observable ETO-protein modifications upon storage in ETO-sterilized containers will depend on a complex interplay of protein properties, formulation details, storage conditions, and amount of residual ETO initially in the container.

摘要

未标注

环氧乙烷(ETO)常用于对塑料容器进行灭菌,但灭菌后残留量对蛋白质治疗剂的影响仍未得到充分了解。在这里,我们主要关注影响ETO从经ETO处理的塑料容器迁移到水溶液中的浓度的因素。设计了一项研究来调查该过程在不同温度下的动力学,动力学数据可以用基于菲克扩散和一级化学反应(以解释观察到的ETO水解)组合的模型来拟合。由此获得的扩散和反应速率常数服从类似阿仑尼乌斯的温度依赖性。这些结果表明,对于涉及萃取到水中的分析方法,容器中残留ETO的测量必须考虑ETO水解的影响。此外,还探讨了容器中流体的盐浓度和pH值对累积ETO水平的影响。最后,研究了ETO与抗链霉抗生物素蛋白(AntiSA)免疫球蛋白G1(IgG1)和IgG2抗体的相互作用,当在添加了ETO的溶液中孵育时,在所有甲硫氨酸残基上都发现了ETO加合物,添加的ETO浓度基于动力学研究在经ETO处理的塑料小瓶中可能达到。总体而言,在经ETO灭菌的容器中储存时可观察到的ETO-蛋白质修饰的可能性将取决于蛋白质性质、制剂细节、储存条件以及容器中初始残留ETO量的复杂相互作用。

摘要

环氧乙烷(ETO)常用于对塑料容器进行灭菌,但灭菌后残留量对蛋白质治疗剂的影响仍未得到充分了解。在这里,我们描述了一些实验,探索随着时间推移影响ETO从经ETO处理的塑料容器迁移到水溶液中的浓度的因素。此外,还研究了ETO与模型抗体的相互作用,当在添加了ETO的溶液中孵育时,在所有甲硫氨酸残基上都发现了ETO加合物,添加的ETO浓度在经ETO处理的塑料小瓶中可能达到。总体而言,在经ETO灭菌的容器中储存时可观察到的ETO-蛋白质修饰的可能性将取决于蛋白质性质、制剂细节、储存条件以及容器中初始残留ETO量的复杂相互作用。

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