4.7 Article

Antibody orientation at bacterial surfaces is related to invasive infection

Journal

JOURNAL OF EXPERIMENTAL MEDICINE
Volume 209, Issue 13, Pages 2367-2381

Publisher

ROCKEFELLER UNIV PRESS
DOI: 10.1084/jem.20120325

Keywords

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Funding

  1. Swedish Research Council [7480, 2008:3356]
  2. Swedish Foundation for Strategic Research [FFL4]
  3. Crafoordska Stiftelsen [20090802, 20100892]
  4. Swedish Government Funds for Clinical Research (ALF)
  5. Hansa Medical AB
  6. Medical Faculty at Lund University
  7. Foundation of Knut
  8. Foundation of Alice Wallenberg
  9. Foundation of Torsten
  10. Foundation of Ragnar Soderberg
  11. Foundation of Alfred Osterlund
  12. Foundation of Greta
  13. Foundation of Johan Kock
  14. Foundation of Lars Hiertas Minne
  15. Foundation of Royal Physiographic Society

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Several of the most significant bacterial pathogens in humans, including Streptococcus pyogenes, express surface proteins that bind IgG antibodies via their fragment crystallizable (Fc) region, and the dogma is that this protects the bacteria against phagocytic killing in blood. However, analysis of samples from a patient with invasive S. pyogenes infection revealed dramatic differences in the presence and orientation of IgG antibodies at the surface of bacteria from different sites. In the throat, IgG was mostly bound to the bacterial surface via Fc, whereas in the blood IgG was mostly bound via fragment antigen-binding (Fab). In infected and necrotic tissue, the Fc-binding proteins were removed from the bacterial surface. Further investigation showed that efficient bacterial IgGFc-binding occurs only in IgG-poor environments, such as saliva. As a consequence, the bacteria are protected against phagocytic killing, whereas in blood plasma where the concentration of IgG is high, the antibodies preferentially bind via Fab, facilitating opsonization and bacterial killing. IgG-poor environments represent the natural habitat for IgGFc-binding bacteria, and IgGFc-binding proteins may have evolved to execute their function in such environments. The lack of protection in plasma also helps to explain why cases of severe invasive infections with IgGFc-binding bacteria are so rare compared with superficial and uncomplicated infections.

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