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首页> 外文期刊>Journal of pharmaceutical sciences. >Application of x-ray photoelectron spectroscopic analysis to protein adsorption on materials relevant to biomanufacturing
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Application of x-ray photoelectron spectroscopic analysis to protein adsorption on materials relevant to biomanufacturing

机译:X射线光电子能谱分析在生物制造相关材料上蛋白质吸附中的应用

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摘要

X-ray photoelectron spectroscopy (XPS) has been used to analyze the adsorption of a therapeutic monoclonal antibody (mAb), rituximab, and polyclonal human IgG (hIgG) on materials relevant to biomanufacturing of protein drug products. Details of the methods used to obtain qualitative confirmation of protein adsorption, using both the nitrogen (N 1s) signal originating from mAb proteins and an iodine heteroatom label, are presented. Both rituximab and hIgG were found to adsorb to a glass vial surface, vial rubber cap liner, syringe plunger tip, cell culture flask, serological pipette, and microcentrifuge tube. There was no evidence of protein adsorption on samples of polyvinylchloride (PVC) tubing or the barrel of a syringe. Differences in XPS heteroatom peak intensities, based on whether the heteroatom label was added to the protein prior to surface adsorption or after, suggest that adsorbed rituximab on a glass vial surface is in a structural conformation that allows extensive heteroatom labeling. Using a simple uniform overlayer model, the coverage of rituximab on a glass vial surface was determined by XPS to be 3.6 mg/m 2, a value consistent with that expected for a theoretical monolayer.
机译:X射线光电子能谱(XPS)已用于分析治疗性单克隆抗体(mAb),利妥昔单抗和多克隆人IgG(hIgG)在与蛋白质药物产品的生物制造相关的材料上的吸附。本文详细介绍了使用来自mAb蛋白的氮(N 1s)信号和碘杂原子标记获得定性蛋白质吸附的方法的详细信息。发现利妥昔单抗和hIgG均吸附到玻璃小瓶表面,小瓶橡胶盖衬里,注射器柱塞头,细胞培养瓶,血清移液管和微量离心管上。没有证据表明蛋白质会吸附在聚氯乙烯(PVC)管或注射器针筒的样品上。基于在表面吸附之前还是之后将杂原子标记物添加到蛋白质上,XPS杂原子峰强度的差异表明,玻璃瓶表面吸附的利妥昔单抗处于允许广泛杂原子标记的结构构象。使用简单的均匀覆盖模型,通过XPS将利妥昔单抗在玻璃小瓶表面的覆盖率确定为3.6 mg / m 2,该值与理论单层的预期值一致。

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