Assessing production variability in empty and filled adeno-associated viruses by single molecule mass analyses

基因组 免疫原性 生物 衣壳 计算生物学 基因传递 碎片(计算) 基因 遗传增强 病毒学 遗传学 免疫系统 生态学
作者
Eduard H.T.M. Ebberink,Alisa Ruisinger,Markus Nuebel,Marco Thomann,Albert J. R. Heck
出处
期刊:Molecular therapy. Methods & clinical development [Elsevier]
卷期号:27: 491-501 被引量:1
标识
DOI:10.1016/j.omtm.2022.11.003
摘要

Adeno-associated viruses (AAVs) are useful vehicles for gene therapy because of their stability, low immunogenicity. and non-pathogenicity. However, disparity in AAV sample preparations (e.g., in capsid composition, DNA packaging, and impurities) gives rise to product heterogeneity, with possibly undesired effects on gene delivery. Ideally, AAV production should be with full control of AAV structure and genetic payload. Therefore, robust, efficient, and low material consuming methods are essential to characterize AAVs. Here, we use two emerging single-molecule techniques, mass photometry and Orbitrap-based charge-detection mass spectrometry, and show how they may efficiently and accurately characterize AAVs. We were able to resolve heterogeneous pools of particles, evaluating AAVs from two different serotypes (AAV8 and AAV2), produced by three independent production platforms, either lacking a genome or packed with a transgene. Together our data confirm that the different AAV production methods result in rather different and diverse AAV particle distributions. Especially for the packed AAVs, frequently additional subspecies were observed, next to the expected packed genome, mostly resulting from under- or overpackaging of genome material and/or residual empty particles. This work further establishes that both these single-particle techniques may become valuable tools in characterizing AAVs before they are used in gene therapy.
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