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Characterization of Protein-Excipient Microheterogeneity in Biopharmaceutical Solid-State Formulations by Confocal Fluorescence Microscopy.

Stijn H S KoshariJean L RossPurnendu K NayakIsidro E ZarragaKarthikan RajagopalNorman J WagnerAbraham M Lenhoff
Published in: Molecular pharmaceutics (2017)
Protein-stabilizer microheterogeneity is believed to influence long-term protein stability in solid-state biopharmaceutical formulations and its characterization is therefore essential for the rational design of stable formulations. However, the spatial distribution of the protein and the stabilizer in a solid-state formulation is, in general, difficult to characterize because of the lack of a functional, simple, and reliable characterization technique. We demonstrate the use of confocal fluorescence microscopy with fluorescently labeled monoclonal antibodies (mAbs) and antibody fragments (Fabs) to directly visualize three-dimensional particle morphologies and protein distributions in dried biopharmaceutical formulations, without restrictions on processing conditions or the need for extensive data analysis. While industrially relevant lyophilization procedures of a model IgG1 mAb generally lead to uniform protein-excipient distribution, the method shows that specific spray-drying conditions lead to distinct protein-excipient segregation. Therefore, this method can enable more definitive optimization of formulation conditions than has previously been possible.
Keyphrases
  • solid state
  • protein protein
  • amino acid
  • single molecule
  • data analysis
  • binding protein
  • optical coherence tomography
  • computed tomography
  • radiation therapy
  • squamous cell carcinoma
  • raman spectroscopy
  • high speed