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分析型阴离子交换色谱和基于 LC-MS 的肽图分析揭示热应激条件下 AAV1 和 AAV8 的不同化学降解途径。

Distinct chemical degradation pathways of AAV1 and AAV8 under thermal stress conditions revealed by analytical anion exchange chromatography and LC-MS-based peptide mapping.

机构信息

Analytical Chemistry Group, Regeneron Pharmaceuticals Inc., Tarrytown, New York 10591-6707, United States.

Formulation Development Group, Regeneron Pharmaceuticals Inc., Tarrytown, New York 10591-6707, United States.

出版信息

J Pharm Biomed Anal. 2024 Dec 15;251:116452. doi: 10.1016/j.jpba.2024.116452. Epub 2024 Aug 26.

DOI:10.1016/j.jpba.2024.116452
PMID:39217700
Abstract

Adeno-associated virus (AAV)-based gene therapy is experiencing a rapid growth in the field of medicine and holds great promise in combating a wide range of human diseases. For successful development of AAV-based products, comprehensive thermal stability studies are often required to establish storage conditions and shelf life. However, as a relatively new modality, limited studies have been reported to elucidate the chemical degradation pathways of AAV products under thermal stress conditions. In this study, we first presented an intriguing difference in charge profile shift between thermally stressed AAV8 and AAV1 capsids when analyzed by anion exchange chromatography. Subsequently, a novel and robust peptide mapping protocol was developed and applied to elucidate the underlying chemical degradation pathways of thermally stressed AAV8 and AAV1. Compared to the conventional therapeutic proteins, the unique structure of AAV capsids also led to some key differences in how modifications at specific sites may impact the overall charge properties. Finally, despite the high sequency identity, the analysis revealed that the opposite charge profile shifts between thermally stressed AAV8 and AAV1 could be mainly attributed to a single modification unique to each serotype.

摘要

腺相关病毒(AAV)为基础的基因治疗在医学领域正在迅速发展,并在治疗各种人类疾病方面具有广阔的前景。为了成功开发基于 AAV 的产品,通常需要进行全面的热稳定性研究,以确定储存条件和保质期。然而,作为一种相对较新的治疗方式,针对热应激条件下 AAV 产品的化学降解途径,已有报道的研究非常有限。在本研究中,我们首先通过阴离子交换色谱分析,发现受热应激的 AAV8 和 AAV1 衣壳之间的电荷量分布变化存在显著差异。随后,我们开发了一种新颖而强大的肽图分析方法,并将其应用于阐明受热应激的 AAV8 和 AAV1 的化学降解途径。与传统治疗性蛋白相比,AAV 衣壳的独特结构也导致了一些关键的差异,即在特定部位的修饰如何影响整体电荷量特性。最后,尽管具有很高的序列同一性,但分析表明,受热应激的 AAV8 和 AAV1 之间的电荷量分布变化的相反趋势主要归因于每个血清型特有的单一修饰。

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