AAV production in stable packaging cells requires expression of adenovirus 22/33K protein to allow episomal amplification of integrated rep/cap genes

Su, Weiheng; Seymour, Leonard W.; Cawood, Ryan

doi:10.1038/s41598-023-48901-z

Cited by 6 publications

(1 citation statement)

References 36 publications

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“…In 2023, the same authors [ 66 ] published an adaptation of the TESSA system to use in the context of packaging cell lines containing the rep and cap genes (HeLa RC32). The original TESSA system enables rAAV production only when the rep and cap genes are provided in trans , but not from stable packaging cells.…”

Section: Stable Packaging and Producer Cell Linesmentioning

confidence: 99%

Development of Stable Packaging and Producer Cell Lines for the Production of AAV Vectors

Merten

2024

Microorganisms

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Today, recombinant adeno-associated virus (rAAV) vectors represent the vector systems which are mostly used for in vivo gene therapy for the treatment of rare and less-rare diseases. Although most of the past developments have been performed by using a transfection-based method and more than half of the authorized rAAV-based treatments are based on transfection process, the tendency is towards the use of stable inducible packaging and producer cell lines because their use is much more straightforward and leads in parallel to reduction in the overall manufacturing costs. This article presents the development of HeLa cell-based packaging/producer cell lines up to their use for large-scale rAAV vector production, the more recent development of HEK293-based packaging and producer cell lines, as well as of packaging cell lines based on the use of Sf9 cells. The production features are presented in brief (where available), including vector titer, specific productivity, and full-to-empty particle ratio.

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Section: Stable Packaging and Producer Cell Linesmentioning

confidence: 99%

Development of Stable Packaging and Producer Cell Lines for the Production of AAV Vectors

Merten

2024

Microorganisms

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Molecular design of controllable recombinant adeno‐associated virus (AAV) expression systems for enhanced vector production

Johari,

Pohle,

Whitehead

et al. 2024

Biotechnology Journal

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Recombinant adeno‐associated virus (rAAV) is the leading vector for the delivery of gene therapies. However, low viral genome (VG) titers are common and the proportion of “full” capsids containing the therapeutic gene payload can be highly variable. The coordinated molecular design of plasmids encoding viral components and Helper functions remains a major challenge for rAAV manufacturing. Here we present the design of improved Rep/Cap and Helper plasmids for rAAV2/8 production, (i) a Rep/Cap expression vector harboring independently controllable rep and cap genes and (ii) an improved Helper plasmid harboring E4 gene deletion variants. First, an optimized Rep/Cap vector utilized a truncated p5 promoter, a p5 cis‐regulatory element at the 3′ end in combination with a heterologous promoter to drive Cap expression and an additional copy of the rep52/40 gene to overexpress short Rep proteins. We demonstrate that Rep78 is essential for efficient rAAV2/8 production in HEK293 cells, and a higher ratio of short Rep to long Rep proteins enhances genome packaging. Second, we identified regulators and open reading frames within the Helper plasmid that contribute to increased rAAV2/8 production. While L4‐33k/22k is integral to optimal production, the use of E4orf6–6/7 subset significantly enhanced VG titer. Together, an optimal combination of engineered Rep/Cap and Helper plasmid variants increased VG titer by 3.1‐fold. This study demonstrates that configuring and controlling the expression of the different AAV genetic elements contributes toward high rAAV production and product quality (full/empty capsid ratio).

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Characterization of the function of Adenovirus L4 gene products and their impact on AAV vector production

Nie,

Pan,

et al. 2024

Molecular Therapy - Methods & Clinical Development

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AAV production in stable packaging cells requires expression of adenovirus 22/33K protein to allow episomal amplification of integrated rep/cap genes

Cited by 6 publications

References 36 publications

Development of Stable Packaging and Producer Cell Lines for the Production of AAV Vectors

Development of Stable Packaging and Producer Cell Lines for the Production of AAV Vectors

Molecular design of controllable recombinant adeno‐associated virus (AAV) expression systems for enhanced vector production

Characterization of the function of Adenovirus L4 gene products and their impact on AAV vector production

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