Using extensional flow to reveal diverse aggregation landscapes for three IgG1 molecules

Willis, Leon F.; Kumar, Amit; Dobson, John; Bond, Nicholas J.; Lowe, David C.; Turner, Richard E.; Radford, Sheena E.; Kapur, Nikil; Brockwell, David J.

doi:10.1002/bit.26543

Cited by 15 publications

(26 citation statements)

References 64 publications

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“…Different types of stresses and flow fields have been suggested to be critical in promoting the aggregation of proteins (Bee, Stevenson et al, ; Bekard, Asimakis, Bertolini, & Dunstan, ; Elias & Joshi, ). In addition to shaking and wall shear rate, elongational strain and cavitation shocks have also been recently proposed to potentially trigger protein aggregation (Dobson et al, ; Duerkop, Berger, Dürauer, & Jungbauer, ; Willis et al, ). Despite the considerable research efforts of the past decades, there still is no clear consensus regarding the type and magnitude of hydrodynamic stress required to induce protein aggregation, and mechanistic explanations of the processes involved remain elusive (Bee, Stevenson et al, ; Bekard, Barnham, White, & Dunstan, ; Biddlecombe et al, ; Dobson et al, ; Thomas & Geer, ).…”

Section: Introductionmentioning

confidence: 99%

Synergistic effects of flow and interfaces on antibody aggregation

Grigolato

Arosio

2019

Biotech & Bioengineering

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During the manufacturing process, solutions of protein‐based drugs are exposed to hydrodynamic forces, which can potentially affect protein stability and aggregation. Despite being an area of extensive investigation, the effect of hydrodynamic flow on protein aggregation is still controversial. In this study, we designed an experimental setup that allowed us to investigate flow‐ and interface‐induced protein aggregation of two model immunoglobulins in the presence of well‐defined flow stresses and solid–liquid interfaces. Within the range of shear rates typically encountered in bioprocessing ( γ ̇ = 10 – 10 3 normals − 1), we observed that increasing the shear rate by three orders of magnitude had a negligible effect on protein aggregation. By contrast, changes in the materials of the syringe barrels had a dramatic effect on the monomer loss, demonstrating the key role of solid–liquid interfaces in flow‐induced aggregation. This finding was confirmed by the observed inverse dependence of the aggregation rate on the initial protein concentration, which is inconsistent with mechanisms of protein aggregation in bulk solution. Overall, our results reveal the presence of a synergistic effect of interfaces and hydrodynamic flow in flow‐induced protein aggregation, which arises from the formation of protein particles or films on interfaces followed by displacement by flow or mechanical scraping.

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Section: Introductionmentioning

confidence: 99%

Synergistic effects of flow and interfaces on antibody aggregation

Grigolato

Arosio

2019

Biotech & Bioengineering

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“…This group of antibodies, dubbed the (Clinical) 33 herein, showed varied responses in the assays employed previously (Supplementary Table I and Figure S1) . The magnitude of aggregation triggered by the EFD is strongly dependent on protein concentration, strain rate (which is controlled by changing the velocity of the syringe driver) pass number (the number of times the fluid is shuttled through the capillary) and solution conditions (eg, arginine succinate buffer suppressing flow‐induced aggregation), yielding a complex response surface to flow . Here, the large number of antibodies to be studied, together with sample limitations, precluded such a detailed study.…”

Section: Resultsmentioning

confidence: 98%

“…In addition, we showed that a candidate mAb with poor biophysical and pharmacokinetic properties (MEDI1912_WFL) was more sensitive to hydrodynamic flow (in terms of quantity of aggregate produced) than its derivative (MEDI1912_STT), rationally engineered to improve its biophysical characteristics . Finally, we used the EFD to identify which factors (protein concentration, sequence, buffer components, and flow conditions) are key to modulating the flow‐induced aggregation of three model IgG1 mAbs . These data show the utility of hydrodynamic force as a potential developability assay.…”

Section: Introductionmentioning

confidence: 90%

“…It is becoming clear, however, that many aggregation pathways initiate from activated, partially unfolded metastable states that may not be detected by these techniques, especially in accelerated stability assays . To address this issue, we previously developed a device that exerts hydrodynamic forces, similar to those applied during bioprocessing, onto proteins . In this method, fluid is passed between two syringes coupled via a narrow glass capillary (one fifteenth of the syringes' diameter) (Figure A).…”

Section: Introductionmentioning

confidence: 99%

“…These data show the utility of hydrodynamic force as a potential developability assay. As these studies used only three IgG1 mAbs, our understanding of the behavior of a broader range of therapeutic mAbs, or how the EFD relates to other methods of assessing aggregation, remained unknown.…”

Section: Introductionmentioning

confidence: 99%

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The uniqueness of flow in probing the aggregation behavior of clinically relevant antibodies

Willis

Kumar

Jain

et al. 2020

Engineering Reports

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The development of therapeutic monoclonal antibodies (mAbs) can be hindered by their tendency to aggregate throughout their lifetime, which can illicit immunogenic responses and render mAb manufacturing unfeasible. Consequently, there is a need to identify mAbs with desirable thermodynamic stability, solubility, and lack of self-association. These behaviors are assessed using an array of in silico and in vitro assays, as no single assay can predict aggregation and developability. We have developed an extensional and shear flow device (EFD), which subjects proteins to defined hydrodynamic forces which mimic those experienced in bioprocessing. Here, we utilize the EFD to explore the aggregation propensity of 33 IgG1 mAbs, whose variable domains are derived from clinical antibodies. Using submilligram quantities of material per replicate, wide-ranging EFD-induced aggregation (9-81% protein in pellet) was observed for these mAbs, highlighting the EFD as a sensitive method to assess aggregation propensity. By comparing the EFD-induced aggregation data to those obtained previously from 12 other biophysical assays, we show that the EFD provides distinct information compared with current measures of adverse biophysical behavior. Assessing a candidate's liability to hydrodynamic force thus adds novel insight into the rational selection of developable mAbs that complements other assays. K E Y W O R D S aggregation, developability, extensional flow, monoclonal antibody, shear flowThis is an open access article under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.

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Polysorbate identity and quantity dictate the extensional flow properties of protein‐excipient solutions

2022

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While protein medications are promising for treatment of cancer and autoimmune diseases, challenges persist in terms of development and injection stability of highconcentration formulations. Here, the extensional flow properties of proteinexcipient solutions are examined via dripping-onto-substrate extensional rheology, using a model ovalbumin (OVA) protein and biocompatible excipients polysorbate 20 (PS20) and 80 (PS80). Despite similar PS structures, differences in extensional flow are observed based on PS identity in two regimes: at moderate total concentrations where surface tension differences drive changes in extensional flow behavior, and at small PS:OVA ratios, which impact the onset of weakly elastic flow behavior.Undesirable elasticity is observed in ultra-concentrated formulations, independent of PS identity; higher PS contents are required to observe these effects than in analogous polymeric excipient solutions. These studies reveal novel extensional flow behaviors in protein-excipient solutions, and provide a straightforward methodology for assessing the extensional flow stability of new protein-excipient formulations.

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Using extensional flow to reveal diverse aggregation landscapes for three IgG1 molecules

Cited by 15 publications

References 64 publications

Synergistic effects of flow and interfaces on antibody aggregation

Synergistic effects of flow and interfaces on antibody aggregation

The uniqueness of flow in probing the aggregation behavior of clinically relevant antibodies

Polysorbate identity and quantity dictate the extensional flow properties of protein‐excipient solutions

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