Participation of Integrin a5B1 in the Fibronectin-Mediated Adherence of Enteroaggregative Escherichia coli to Intestinal Cells
Author
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Izquierdo, Mariana
Author
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Alvestegui, Alejandra
es_CL
Author
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Nataro, James P.
es_CL
Author
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Ruiz Pérez, Fernando
es_CL
Author
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Farfán Urzúa, Mauricio Javier
es_CL
Admission date
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2014-12-17T01:42:46Z
Available date
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2014-12-17T01:42:46Z
Publication date
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2014
Cita de ítem
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Biomed Res Int. 2014; 2014: 781246. 8 pages
en_US
Identifier
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dx.doi.org/10.1155/2014/781246
Identifier
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https://repositorio.uchile.cl/handle/2250/129404
General note
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Artículo de publicación ISI
en_US
Abstract
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Adherence to the intestinal epithelia is a key feature in enteroaggregative Escherichia coli (EAEC) infection. The aggregative adherence fimbriae (AAFs) are involved in EAEC interaction with receptors at the surface of intestinal cells. We and others have demonstrated that fibronectin is a receptor for AAF/II fimbriae. Considering that the major cellular receptor of fibronectin is integrin a5B1, in this study we evaluated the participation of this receptor in the fibronectin-mediated adherence of EAEC strain 042 to intestinal cells. We found that EAEC strain 042 has the ability to bind directly and indirectly to integrin a5B1; direct binding was not mediated by AAF/II fimbriae and indirect binding was mediated by AAF/II and fibronectin. Coimmunoprecipitation assays confirmed the formation of the complex AafA/fibronectin/integrin a5B1. To evaluate EAEC adherence to intestinal cells, T84 cells were incubated with fibronectin and an antibody that blocks the interaction region of integrin a5B1 to fibronectin, the RGD site. Under these conditions, we found the number of adherent bacteria to epithelial cells significantly reduced. Additionally, fibronectin-mediated adherence of EAEC strain 042 was abolished in HEp-2 cells transfected with integrin a5 shRNA. Altogether, our data support the involvement of integrin a5B1 in the fibronectin-mediated EAEC binding to intestinal cells.
en_US
Patrocinador
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Thisworkwas supported byGrant no. 1120809 from FONDECYT
to Mauricio J. Farfan. Work in the Nataro lab was supported
by Grant no. AI-033096 from the National Institutes
of Health to James P. Nataro.