Antibody response to fibronectin-binding adhesin FnbpA in patients with Staphylococcal aureus infections
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Abstract
We have analyzed antibody reactivity to a fibronectin-binding microbial surface component that recognizes
adhesive matrix molecules (MSCRAMM) in blood plasma collected from patients with staphylococcal infections.
All patients had elevated levels of anti-MSCRAMM antibodies compared to those of young children who,
presumably, had not been exposed to staphylococcal infections. The anti-MSCRAMM antibodies preferentially
reacted with the ligand-binding repeat domain of the adhesin. However, these antibodies did not inhibit fibronectin
binding. Essentially, all patients had antibodies which specifically recognized the fibronectin-MSCRAMM
complex but not the isolated components. Epitopes recognized by these anti-ligand-induced binding sites antibodies
were found in each repeat unit of the MSCRAMM. These results demonstrate that staphylococci have
bound fibronectin some time during infection and that each repeat unit in the MSCRAMM can engage in
ligand binding. Furthermore, our previously proposed model, suggesting that an unordered structure in the
MSCRAMM undergoes a conformational change upon ligand binding (K. House-Pompeo, Y. Xu, D. Joh, P. Speziale,
and M. Ho¨o¨k, J. Biol. Chem. 271:1379–1384, 1996), is presumably operational in patients during infections