Jörg M. Windisch scite author profile

PurposeFollowing two cases of neutralizing antibodies to epoetin alfa in an investigational clinical study, a small number of individual syringes of two drug product batches were found to contain unusually high levels of aggregation at the end of the clinical trial.MethodsWe undertook an extensive analytical approach to determine the root-cause of the increased aggregation in the affected batches.ResultsSoluble tungsten was found in the syringes, most likely derived from the pins used to manufacture the syringes. Spiking of epoetin alfa with sodium polytungstate or an extract of tungsten pins used to manufacture the syringes induced the formation of aggregates, both dimers that appeared to be covalently linked by disulphide bonds as well as higher-order aggregates. Sodium polytungstate had also a strong denaturing effect on the protein.ConclusionsWe propose tungsten-mediated unfolding and aggregation of epoetin alfa in pre-filled syringes as a potential root cause for increased immunogenicity. This finding may be more broadly applicable to this and other classes of therapeutic proteins.

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Taking immunogenicity assessment of therapeutic proteins to the next level

Büttel

Chamberlain²,

Chowers

et al. 2011

Biologicals

126

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Totality of the evidence at work: The first U.S. biosimilar

Holzmann¹,

Balser²,

Windisch³

2015

Expert Opinion on Biological Therapy

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RNase of classical swine fever virus: biochemical characterization and inhibition by virus-neutralizing monoclonal antibodies

Windisch

Schneider

Stark

et al. 1996

J Virol

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The structural glycoprotein E0 of classical swine fever virus (CSFV) possesses an intrinsic RNase activity. Here we present the first comprehensive biochemical characterization of E0, using a recombinant glycoprotein expressed in insect cells. We were able to show that the presence of neither carbohydrate moieties nor disulfide bonds is a prerequisite for RNase activity. In addition, virus-neutralizing and nonneutralizing anti-E0 monoclonal antibodies were tested for their ability to influence RNase activity. In these experiments, the antibodies which effectively blocked the infection of STE cells also exerted a high degree of E0 RNase inhibition. This correlation suggests that the RNase activity of CSFV E0 plays a role in the viral life cycle.

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Specific neurotrophin binding to leucine‐rich motif peptides of TrkA and TrkB

et al. 1995

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Jörg M. Windisch

Tungsten-Induced Denaturation and Aggregation of Epoetin Alfa During Primary Packaging as a Cause of Immunogenicity

Taking immunogenicity assessment of therapeutic proteins to the next level

Totality of the evidence at work: The first U.S. biosimilar

RNase of classical swine fever virus: biochemical characterization and inhibition by virus-neutralizing monoclonal antibodies

Specific neurotrophin binding to leucine‐rich motif peptides of TrkA and TrkB

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