Publications by authors named "Arnik Shah"

Biotherapeutic's higher order structure (HOS) is a critical determinant of its functional properties and conformational relevance. Here, we evaluated two covalent labeling methods: diethylpyrocarbonate (DEPC)-labeling and fast photooxidation of proteins (FPOP), in conjunction with mass spectrometry (MS), to investigate structural modifications for the new class of immuno-oncological therapy known as bispecific antigen-binding biotherapeutics (BABB). The evaluated techniques unveiled subtle structural changes occurring at the amino acid residue level within the antigen-binding domain under both native and thermal stress conditions, which cannot be detected by conventional biophysical techniques, e.

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Article Synopsis
  • Charge variant characterization is essential for ensuring the quality, safety, and efficacy of biologic therapeutics, as these charge variants can significantly affect their performance and immunogenicity.
  • Traditional methods for characterizing these variants are labor-intensive and challenging, especially for low concentration products.
  • Recent advancements in pH-based ion-exchange chromatography and mass spectrometry have led to a more efficient workflow for identifying post-translational modifications in bispecific antigen-binding proteins, allowing for rapid and precise characterization of therapeutic proteins.
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Fragmentation of therapeutic proteins is a potential critical quality attribute (CQA) that can occur or during manufacturing or storage due to enzymatic and non-enzymatic degradation pathways, such as hydrolysis, peroxide mediation, and acid/metal catalysis. Characterization of the fragmentation pattern of a therapeutic protein is traditionally accomplished using capillary gel electrophoresis with UV detection under both non-reducing and reducing conditions (nrCGE and rCGE). However, such methods are incompatible with direct coupling to mass spectrometry (MS) due to the use of anionic surfactants, , sodium dodecyl sulfate (SDS).

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