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Measuring macromolecular size distributions and interactions at high concentrations by sedimentation velocity

机译:通过沉降速度测量高浓度下的大分子尺寸分布和相互作用

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摘要

In concentrated macromolecular solutions, weak physical interactions control the solution behavior including particle size distribution, aggregation, liquid-liquid phase separation, or crystallization. This is central to many fields ranging from colloid chemistry to cell biology and pharmaceutical protein engineering. Unfortunately, it is very difficult to determine macromolecular assembly states and polydispersity at high concentrations in solution, since all motion is coupled through long-range hydrodynamic, electrostatic, steric, and other interactions, and scattering techniques report on the solution structure when average interparticle distances are comparable to macromolecular dimensions. Here we present a sedimentation velocity technique that, for the first time, can resolve macromolecular size distributions at high concentrations, by simultaneously accounting for average mutual hydrodynamic and thermodynamic interactions. It offers high resolution and sensitivity of protein solutions up to 50 mg/ml, extending studies of macromolecular solution state closer to the concentration range of therapeutic formulations, serum, or intracellular conditions.
机译:在浓缩的大分子溶液中,弱的物理相互作用控制溶液的行为,包括粒径分布,聚集,液-液相分离或结晶。这对于从胶体化学到细胞生物学和药物蛋白质工程的许多领域至关重要。不幸的是,很难确定溶液中高浓度下的大分子组装状态和多分散性,因为所有运动都是通过远程流体动力学,静电,空间和其他相互作用耦合的,并且当平均粒子间距离时,散射技术会报告溶液结构与大分子尺寸相比在这里,我们提出了一种沉降速度技术,该技术首次可以通过同时考虑平均相互的水动力和热动力相互作用来解析高浓度下的大分子尺寸分布。它提供高达50μmg/ ml的蛋白质溶液的高分辨率和灵敏度,将大分子溶液状态的研究扩展到更接近治疗剂,血清或细胞内条件的浓度范围。

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