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Journal ArticleDOI

Both protein adsorption and aggregation contribute to shear yielding and viscosity increase in protein solutions

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TLDR
Evidence of a bulk yield stress arising from protein aggregation is presented, and correlated with results from standard characterization techniques used in the bio-pharmaceutical industry.
Abstract
A combination of sensitive rotational rheometry and surface rheometry with a double-wall ring were used to identify the origins of the viscosity increase at low shear rates in protein solutions. The rheology of two high molecular weight proteins is discussed: Bovine Serum Albumin (BSA) in a Phosphate Buffered Saline solution and an IgG1 monoclonal antibody (mAb) in a formulation buffer containing small quantities of a non-ionic surfactant. For surfactant-free BSA solutions, the interfacial viscosity dominates the low shear viscosity measured in rotational rheometers, while the surfactant-laden mAb solution has an interfacial viscosity that is small compared to that from aggregation in the bulk. A viscoelastic film forms at the air/water interface in the absence of surfactant, contributing to an apparent yield stress (thus a low shear viscosity increase) in conventional bulk rheology measurements. Addition of surfactant eliminates the interfacial yield stress. Evidence of a bulk yield stress arising from protein aggregation is presented, and correlated with results from standard characterization techniques used in the bio-pharmaceutical industry. The protein film at the air/water interface and bulk aggregates both lead to an apparent viscosity increase and their contributions are quantified using a dimensionless ratio of the interfacial and total yield stress. While steady shear viscosities at shear rates below ∼1 s(-1) contain rich information about the stability of protein solutions, embodied in the measured yield stress, such low shear rate data are regrettably often not measured and reported in the literature.

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Journal ArticleDOI

Protein aggregation, particle formation, characterization & rheology

TL;DR: This review attempts to give a concise overview of recent progress made in mechanistic understanding of protein aggregation, particulate formation and protein solution rheology and highlights some areas of controversy and debate that need further attention from the scientific community.
Journal ArticleDOI

Protein aggregation - Mechanisms, detection, and control.

TL;DR: This review is intended to summarize four major aspects of protein aggregation - (1) aggregation mechanisms, (2) aggregation-influencing factors, (3) detection of protein aggregates, and (4) control ofprotein aggregation based on recent literature in this area.
Journal ArticleDOI

Critical Examination of the Colloidal Particle Model of Globular Proteins

TL;DR: The findings point to limited validity of the colloidal protein model and to the need for further consideration and quantification of the effects of conformational changes on protein solution viscosity, protein association, and the phase behavior.
Journal ArticleDOI

Recent progresses of understanding the viscosity of concentrated protein solutions

TL;DR: A brief review of the recent experimental and theoretical progress in understanding the viscosity of concentrated protein solutions with a focus on the experimental results.
Posted ContentDOI

Measuring the density and viscosity of culture media for optimized computational fluid dynamics analysis of in vitro devices

TL;DR: The density and dynamic viscosity of DMEM and RPMI-1640 media supplemented with typical concentrations of foetal bovine serum were measured to serve as a reference for computational design analysis and demonstrated clear differences in maximum wall shear stress and pressure between fluid models.
References
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Book

The Structure and Rheology of Complex Fluids

TL;DR: In this article, the authors present a comprehensive overview of the properties and properties of complex fluids and their properties in terms of physics, chemistry, physics theory, and physics of complex fluid properties.
Journal ArticleDOI

Crystal structure of human serum albumin at 2.5 A resolution.

TL;DR: A new triclinic crystal form of human serum albumin (HSA), derived either from pool plasma or from a Pichia pastoris expression system, was obtained from polyethylene glycol 4000 solution, and three-dimensional structures of pHSA and rHSA were determined.
Journal ArticleDOI

Physical Stability of Proteins in Aqueous Solution: Mechanism and Driving Forces in Nonnative Protein Aggregation

TL;DR: The purpose of the current review is to provide a fundamental understanding of the mechanisms by which proteins aggregate and by which varying solution conditions, such as temperature, pH, salt type, salt concentration, cosolutes, preservatives, and surfactants, affect this process.
Journal ArticleDOI

Protein aggregation and its inhibition in biopharmaceutics

TL;DR: This article intends to discuss protein aggregation and its related mechanisms, methods characterizingprotein aggregation, factors affecting protein aggregation, and possible venues in aggregation prevention/inhibition in various stages of protein drug development.
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