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基于尺寸的病毒去除过滤器污染的分析使用分段蛋白质聚集体。

Size-based analysis of virus removal filter fouling using fractionated protein aggregates.

机构信息

Technology Development Department, Bioprocess Division, Asahi Kasei Medical Co., Ltd., Miyazaki, Japan.

Bioprocess Technology Development Department, Asahi Kasei Medical MT Corp., Miyazaki, Japan.

出版信息

Biotechnol Prog. 2024 Jan-Feb;40(1):e3391. doi: 10.1002/btpr.3391. Epub 2023 Sep 21.

Abstract

Fouling by protein aggregates reduces virus removal filter performance. In the present study, we investigated the effects of different-sized protein aggregates on fouling and aggregate retention in order to better understand the fouling mechanisms. Human immunoglobulin G was denatured by heating to produce aggregates of various sizes and then fractionated by size exclusion chromatography into different-sized aggregates with a narrow size distribution. The fractionated aggregates were filtered on Planova 20N, a virus removal filter known for its stable filtration capability. Analysis of flux behavior demonstrated different flux decrease patterns for different-sized aggregates. Observation of aggregate retention by staining revealed that larger aggregates were captured closer to the inner surface of the membrane while smaller aggregates penetrated farther into the membrane. These findings demonstrate that Planova 20N has a gradient structure with decreasing pore size from the inner to the outer surface of the membrane. This structure minimizes fouling and enables stable filtration by protecting the smaller pores located closer to the outer surface from clogging by large aggregates. Applying the predominant clogging models to the present filtrations revealed that clogging behavior transitioned from complete blocking to cake filtration as filtration progressed. In this combination model, after a certain number of pores are blocked by complete blocking, newly arrived aggregates begin to accumulate on previously captured aggregates, generating cake between capture layers within the membrane. Application of the approaches described here will facilitate elucidation of membrane fouling and virus removal mechanisms.

摘要

蛋白质聚集体的污染会降低病毒去除过滤器的性能。在本研究中,我们研究了不同大小的蛋白质聚集体对污染和聚集体截留的影响,以便更好地了解污染机制。通过加热使人免疫球蛋白 G 变性,产生不同大小的聚集体,然后通过大小排阻色谱法将其分成具有较窄分布的不同大小的聚集体。将分级的聚集体过滤在 Planova 20N 上,Planova 20N 是一种以稳定过滤能力而闻名的病毒去除过滤器。通量行为分析表明,不同大小的聚集体具有不同的通量下降模式。通过染色观察聚集体截留情况表明,较大的聚集体更靠近膜的内表面被截留,而较小的聚集体则更深入地渗透到膜中。这些发现表明 Planova 20N 具有从膜内表面到外表面孔径逐渐减小的梯度结构。这种结构通过保护更靠近外表面的较小孔免受大聚集体的堵塞,最大限度地减少污染并实现稳定的过滤。将主要的堵塞模型应用于目前的过滤,结果表明,随着过滤的进行,堵塞行为从完全堵塞转变为滤饼过滤。在这种组合模型中,在一定数量的孔被完全堵塞后,新到达的聚集体开始在先前捕获的聚集体上积累,在膜内的捕获层之间生成滤饼。应用这里描述的方法将有助于阐明膜污染和病毒去除机制。

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