Affiliation:
1. Department of Microbiology and Immunology, University of Michigan School of Medicine
2. Department of Biologic and Materials Sciences, University of Michigan School of Dentistry, Ann Arbor, Michigan 48109
Abstract
ABSTRACT
Yersinia pestis
, the causative agent of plague, evades host immune responses and rapidly causes disease. The
Y. pestis
adhesin Ail mediates host cell binding and is critical for Yop delivery. To identify the Ail receptor(s), Ail was purified following overexpression in
Escherichia coli
. Ail bound specifically to fibronectin, an extracellular matrix protein with the potential to act as a bridge between Ail and host cells. Ail expressed by
E. coli
also mediated binding to purified fibronectin, and Ail-mediated
E. coli
adhesion to host cells was dependent on fibronectin. Ail expressed by
Y. pestis
bound purified fibronectin, as did the
Y. pestis
adhesin plasminogen activator (Pla). However, a KIM5 Δ
ail
mutant had decreased binding to host cells, while a KIM5 Δ
pla
mutant had no significant defect in adhesion. Furthermore, treatment with antifibronectin antibodies decreased Ail-mediated adhesion by KIM5 and the KIM5 Δ
pla
mutant, indicating that the Ail-fibronectin interaction was important for cell binding. Finally, antifibronectin antibodies inhibited the KIM5-mediated cytotoxicity of host cells in an Ail-dependent fashion. These data indicate that Ail is a key adhesin that mediates binding to host cells through interaction with fibronectin on the surface of host cells, and this interaction is important for Yop delivery by
Y. pestis
.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Immunology,Microbiology,Parasitology
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