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合成 AAV 基因治疗载体的生产、加工和特性。

Production, Processing, and Characterization of Synthetic AAV Gene Therapy Vectors.

机构信息

Dept. of Infectious Diseases/Virology, Medical Faculty, University of Heidelberg, 69120, Heidelberg, Germany.

BioQuant, Cluster of Excellence CellNetworks, University of Heidelberg, 69120, Heidelberg, Germany.

出版信息

Biotechnol J. 2021 Jan;16(1):e2000025. doi: 10.1002/biot.202000025. Epub 2020 Oct 7.

Abstract

Over the last two decades, gene therapy vectors based on wild-type Adeno-associated viruses (AAV) are safe and efficacious in numerous clinical trials and are translated into three approved gene therapy products. Concomitantly, a large body of preclinical work has illustrated the power and potential of engineered synthetic AAV capsids that often excel in terms of an organ or cell specificity, the efficiency of in vitro or in vivo gene transfer, and/or reactivity with anti-AAV immune responses. In turn, this has created a demand for new, scalable, easy-to-implement, and plug-and-play platform processes that are compatible with the rapidly increasing range of AAV capsid variants. Here, the focus is on recent advances in methodologies for downstream processing and characterization of natural or synthetic AAV vectors, comprising different chromatography techniques and thermostability measurements. To illustrate the breadth of this portfolio, two chimeric capsids are used as representative examples that are derived through forward- or backwards-directed molecular evolution, namely, AAV-DJ and Anc80. Collectively, this ever-expanding arsenal of technologies promises to facilitate the development of the next AAV vector generation derived from synthetic capsids and to accelerate their manufacturing, and to thus boost the field of human gene therapy.

摘要

在过去的二十年中,基于野生型腺相关病毒(AAV)的基因治疗载体在众多临床试验中是安全且有效的,并已转化为三种获得批准的基因治疗产品。与此同时,大量的临床前工作说明了工程合成 AAV 衣壳的强大功能和潜力,这些衣壳在器官或细胞特异性、体外或体内基因转移的效率以及/或与抗 AAV 免疫反应的反应性方面通常表现出色。反过来,这就需要新的、可扩展的、易于实施的、即插即用的平台工艺,这些工艺与不断增加的 AAV 衣壳变体兼容。在这里,重点是介绍天然或合成 AAV 载体的下游处理和特性分析的最新方法学进展,包括不同的色谱技术和热稳定性测量。为了说明这一组合的广泛性,我们选择了两种嵌合衣壳作为代表性示例,它们分别通过前向或后向分子进化得到,即 AAV-DJ 和 Anc80。总之,这一不断扩展的技术组合有望促进下一代源自合成衣壳的 AAV 载体的开发,并加速其制造,从而推动人类基因治疗领域的发展。

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