A human monoclonal antibody bivalently binding two different epitopes in streptococcal M protein mediates immune function

  • Bahnan W
  • Happonen L
  • Khakzad H
  • et al.
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Abstract

Group A streptococci have evolved multiple strategies to evade human antibodies, making it challenging to create effective vaccines or antibody treatments. Here, we have generated antibodies derived from the memory B cells of an individual who had successfully cleared a group A streptococcal infection. The antibodies bind with high affinity in the central region of the surface-bound M protein. Such antibodies are typically non-opsonic. However, one antibody could effectively promote vital immune functions, including phagocytosis and in vivo protection. Remarkably, this antibody primarily interacts through a bivalent dual-Fab cis mode, where the Fabs bind to two distinct epitopes in the M protein. The dual-Fab cis-binding phenomenon is conserved across different groups of M types. In contrast, other antibodies binding with normal single-Fab mode to the same region cannot bypass the M protein's virulent effects. A broadly binding, protective monoclonal antibody could be a candidate for anti-streptococcal therapy. Our findings highlight the concept of dual-Fab cis binding as a means to access conserved, and normally non-opsonic regions, regions for protective antibody targeting.

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APA

Bahnan, W., Happonen, L., Khakzad, H., Kumra Ahnlide, V., de Neergaard, T., Wrighton, S., … Nordenfelt, P. (2023). A human monoclonal antibody bivalently binding two different epitopes in streptococcal M protein mediates immune function. EMBO Molecular Medicine, 15(2). https://doi.org/10.15252/emmm.202216208

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