AI Article Synopsis

  • Fab is a promising type of antibody drug, and researchers are working to enhance its thermal stability for better therapeutic use.
  • The study introduced disulfide bonds into the Fab fragment, resulting in variants that showed improved thermal stability without losing their biological function.
  • The variants with these disulfide bonds had a 6.5°C increase in denaturation temperatures, maintained their ability to bind antigens, and were less prone to aggregation compared to the original Fab.

Article Abstract

Fab is a promising format for antibody drug. Therefore, efforts have been made to improve its thermal stability for therapeutic and commercial use. So far, we have attempted to introduce a disulfide bond into the Fab fragment to improve its thermal stability and demonstrated that it is possible to do this without sacrificing its biochemical function. In this study, to develop a novel stabilization strategy for Fab, we attempted to introduce a disulfide bond between the variable and constant domains and prepared three variants of Fab; H:G10C + H:P210C, L:P40C + L:E165C, and H:G10C + H:P210C + L:P40C + L:E165C. Differential scanning calorimetry measurements showed that each of these variants had improved thermal stability. In addition, the variants with two disulfide bonds demonstrated a 6.5 °C increase in their denaturation temperatures compared to wild-type Fab. The introduction of disulfide bonds was confirmed by X-ray crystallography, and the variants retained their antigen-binding activity. The variants were also found to be less aggregative than the wild type. Our results demonstrate that the introduction of a disulfide bond between the variable and constant domains significantly improves the thermal stability of Fab.

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Source
http://dx.doi.org/10.1016/j.bbrc.2024.149592DOI Listing

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