Affinity chromatography for virus-like particle manufacturing: Challenges, solutions, and perspectives

IF 3.8 2区 化学 Q1 BIOCHEMICAL RESEARCH METHODS Journal of Chromatography A Pub Date : 2024-03-27 DOI:10.1016/j.chroma.2024.464851
Jing Ma, Zengquan Tian, Qinghong Shi, Xiaoyan Dong, Yan Sun
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Abstract

The increasing medical application of virus-like particles (VLPs), notably vaccines and viral vectors, has increased the demand for commercial VLP production. However, VLP manufacturing has not yet reached the efficiency level achieved for recombinant protein therapeutics, especially in downstream processing. This review provides a comprehensive analysis of the challenges associated with affinity chromatography for VLP purification with respect to the diversity and complexity of VLPs and the associated upstream and downstream processes. The use of engineered affinity ligands and matrices for affinity chromatography is first discussed. Although several representative affinity ligands are currently available for VLP purification, most of them have difficulty in balancing ligand universality, ligand selectivity and mild operation conditions. Then, phage display technology and computer-assisted design are discussed as efficient methods for the rapid discovery of high-affinity peptide ligands. Finally, the VLP purification by affinity chromatography is analyzed. The process is significantly influenced by virus size and variation, ligand type and chromatographic mode. To address the updated regulatory requirements and epidemic outbreaks, technical innovations in affinity chromatography and process intensification and standardization in VLP purification should be promoted to achieve rapid process development and highly efficient VLP manufacturing, and emphasis is given to the discovery of universal ligands, applications of gigaporous matrices and platform technology. It is expected that the information in this review can provide a better understanding of the affinity chromatography methods available for VLP purification and offer useful guidance for the development of affinity chromatography for VLP manufacturing in the decades to come.

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用于制造类病毒粒子的亲和层析技术:挑战、解决方案和展望
病毒样颗粒(VLP),尤其是疫苗和病毒载体在医学上的应用日益广泛,增加了对商业化 VLP 生产的需求。然而,VLP 的生产效率尚未达到重组蛋白疗法的水平,尤其是在下游加工方面。本综述针对 VLP 的多样性和复杂性以及相关的上游和下游工艺,全面分析了用于 VLP 纯化的亲和色谱法所面临的挑战。首先讨论了亲和层析中使用工程亲和配体和基质的问题。虽然目前有几种具有代表性的亲和配体可用于 VLP 纯化,但它们大多难以兼顾配体的通用性、配体的选择性和温和的操作条件。然后,讨论了噬菌体展示技术和计算机辅助设计作为快速发现高亲和性多肽配体的有效方法。最后,分析了亲和层析法纯化 VLP 的过程。这一过程受病毒大小和变异、配体类型和色谱模式的影响很大。针对最新的监管要求和疫情爆发,应推动亲和层析技术创新和 VLP 纯化过程的集约化和标准化,以实现快速工艺开发和高效 VLP 生产,并重点关注通用配体的发现、千孔基质的应用和平台技术。希望本综述中的信息能让人们更好地了解用于 VLP 纯化的亲和层析方法,并为未来几十年亲和层析在 VLP 生产中的发展提供有益的指导。
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来源期刊
Journal of Chromatography A
Journal of Chromatography A 化学-分析化学
CiteScore
7.90
自引率
14.60%
发文量
742
审稿时长
45 days
期刊介绍: The Journal of Chromatography A provides a forum for the publication of original research and critical reviews on all aspects of fundamental and applied separation science. The scope of the journal includes chromatography and related techniques, electromigration techniques (e.g. electrophoresis, electrochromatography), hyphenated and other multi-dimensional techniques, sample preparation, and detection methods such as mass spectrometry. Contributions consist mainly of research papers dealing with the theory of separation methods, instrumental developments and analytical and preparative applications of general interest.
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