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

Author

Listed:
  • Sumit K. Chaturvedi

    (National Institutes of Health)

  • Jia Ma

    (National Institutes of Health
    Columbia University)

  • Patrick H. Brown

    (National Institutes of Health
    National Institute of General Medical Sciences, NIH)

  • Huaying Zhao

    (National Institutes of Health)

  • P. Schuck

    (National Institutes of Health)

Abstract

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.

Suggested Citation

  • Sumit K. Chaturvedi & Jia Ma & Patrick H. Brown & Huaying Zhao & P. Schuck, 2018. "Measuring macromolecular size distributions and interactions at high concentrations by sedimentation velocity," Nature Communications, Nature, vol. 9(1), pages 1-9, December.
  • Handle: RePEc:nat:natcom:v:9:y:2018:i:1:d:10.1038_s41467-018-06902-x
    DOI: 10.1038/s41467-018-06902-x
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