Antje Pegel scite author profile

Antje Pegel

4Publications

70Citation Statements Received

64Citation Statements Given

How they've been cited

109

How they cite others

Affiliations

Rentschler Biopharma (Germany), Boehringer Ingelheim (Germany), Technical University of Munich

Publications

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Rational plasmid design and bioprocess optimization to enhance recombinant adeno‐associated virus (AAV) productivity in mammalian cells

Emmerling

Pegel

Milián

et al. 2015

Biotechnology Journal

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Viral vectors used for gene and oncolytic therapy belong to the most promising biological products for future therapeutics. Clinical success of recombinant adeno-associated virus (rAAV) based therapies raises considerable demand for viral vectors, which cannot be met by current manufacturing strategies. Addressing existing bottlenecks, we improved a plasmid system termed rep/cap split packaging and designed a minimal plasmid encoding adenoviral helper function. Plasmid modifications led to a 12-fold increase in rAAV vector titers compared to the widely used pDG standard system. Evaluation of different production approaches revealed superiority of processes based on anchorage- and serum-dependent HEK293T cells, exhibiting about 15-fold higher specific and volumetric productivity compared to well-established suspension cells cultivated in serum-free medium. As for most other viral vectors, classical stirred-tank bioreactor production is thus still not capable of providing drug product of sufficient amount. We show that manufacturing strategies employing classical surface-providing culture systems can be successfully transferred to the new fully-controlled, single-use bioreactor system Integrity(TM) iCELLis(TM) . In summary, we demonstrate substantial bioprocess optimizations leading to more efficient and scalable production processes suggesting a promising way for flexible large-scale rAAV manufacturing.

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Heterologous expression of the lipid transfer protein CERT increases therapeutic protein productivity of mammalian cells

Florin

Pegel

Becker

et al. 2009

Journal of Biotechnology

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Evaluation of disposable filtration systems for harvesting high cell density fed batch processes

et al. 2011

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A System for Repertoire Cloning and Phage Display of Murine and Leporid Antibody Fragments

Schüller

Wiebe

Pegel

et al. 2010

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Even though rabbit antibodies (Abs) are known to exceed murine Abs with respect to specificity, affinity, and stability, cloned leporid immune repertoires have been rarely considered in recombinant Ab preparation for environmental analysis. We have developed a set of four tetp/o-based phasmid vectors that allow the efficient cloning of both murine and leporid Ab repertoires. These vectors differ in the design of the cloning sites, choice of signal peptides, and antibiotic selection markers. A set of 39 primer oligodeoxynucleotides has been developed for the PCR amplification of rabbit Ab genes, representing the most exhaustive coverage of the leporid immune repertoire described so far. The atrazine-specific murine Fab fragment K411B and a cloned V-gene repertoire from sulfonamide-immunized rabbits were used to compare these phasmids with respect to expression of Fab fragments, phagemid titers, and number of Fab displaying phagemid particles. Our results show that the ratio of recombinant phagemids could be increased up to 65% of total phage titer by utilizing the appropriate phasmid. Based on this system, the selection of two sulfonamide-specific rabbit Abs, SA2 23 and SA2 90, was accomplished after a single phagemid panning round.

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Antje Pegel

Rational plasmid design and bioprocess optimization to enhance recombinant adeno‐associated virus (AAV) productivity in mammalian cells

Heterologous expression of the lipid transfer protein CERT increases therapeutic protein productivity of mammalian cells

Evaluation of disposable filtration systems for harvesting high cell density fed batch processes

A System for Repertoire Cloning and Phage Display of Murine and Leporid Antibody Fragments

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