Adhesins of Leptospira interrogans Mediate the Interaction to Fibrinogen and Inhibit Fibrin Clot Formation In Vitro

Oliveira, Rômulo Silva de; Domingos, Renan F.; Siqueira, Gabriela H.; Fernandes, Luis G. V.; Souza, Natalie M.; Vieira, Mônica L.; Morais, Zenáide Maria de; Vasconcellos, Sílvio Arruda; Nascimento, Ana L. T. O.

doi:10.1371/journal.pntd.0002396

Cited by 43 publications

(53 citation statements)

References 59 publications

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“…In vitro, Leptospira-bound plasmin degrades ECM components such as fibronectin (Vieira et al 2009) and human fibrinogen , and may activate host matrix metalloproteases which in turn could contribute to tissue degradation. Plasmin-coated leptospires also crossed human umbilical vein epithelial cell monolayers more efficiently than normal leptospires, although the precise mechanism was not investigated (Vieira et al 2013). Taken together these data suggest that surface-bound plasmin may facilitate crossing of ECM and tissue barriers and degradation of fibrin clots by leptospires, resulting in dissemination throughout the host.…”

Section: Leptospiral Binding Of Plasminogenmentioning

confidence: 94%

“…Plasmin-coated leptospires also crossed human umbilical vein epithelial cell monolayers more efficiently than normal leptospires, although the precise mechanism was not investigated (Vieira et al 2013). As found in other pathogens (Lähteenmäki et al 2001), leptospires may up regulate activators of plasminogen in host cells (Vieira et al 2013). As found in other pathogens (Lähteenmäki et al 2001), leptospires may up regulate activators of plasminogen in host cells (Vieira et al 2013).…”

Section: Leptospiral Binding Of Plasminogenmentioning

confidence: 99%

“…Transcytosis across human umbilical vein endothelial cell (HUVEC) monolayers was enhanced when leptospires were coated with plasminogen or plasmin, suggesting a proteolytic mechanism (Vieira et al 2013). Transcytosis across human umbilical vein endothelial cell (HUVEC) monolayers was enhanced when leptospires were coated with plasminogen or plasmin, suggesting a proteolytic mechanism (Vieira et al 2013).…”

Section: Crossing Host Tissue Barriersmentioning

confidence: 99%

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Leptospira and Leptospirosis

Faine¹

2015

Current Topics in Microbiology and Immunology

119

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Section: Leptospiral Binding Of Plasminogenmentioning

confidence: 94%

Section: Leptospiral Binding Of Plasminogenmentioning

confidence: 99%

Section: Crossing Host Tissue Barriersmentioning

confidence: 99%

See 1 more Smart Citation

Leptospira and Leptospirosis

Faine¹

2015

Current Topics in Microbiology and Immunology

119

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“…We have recently demonstrated that leptospires bind human fibrinogen (Oliveira et al, 2013) and human thrombin (Fernandes et al, 2015), reducing fibrin clot formation and possibly interfering with the rheological properties of the clot, a characteristic that might add to the haemorrhagic symptoms in severe leptospirosis. Vieira et al (2009) have reported that pathogenic leptospires are able to bind plasminogen (PLG) and subvert the host machinery to convert it into its active form, plasmin (PLA), the main fibrinolytic enzyme.…”

Section: Introductionmentioning

confidence: 99%

“…Vieira et al (2009) have reported that pathogenic leptospires are able to bind plasminogen (PLG) and subvert the host machinery to convert it into its active form, plasmin (PLA), the main fibrinolytic enzyme. PLA-bound leptospires are able to degrade fibrinogen (Oliveira et al, 2013).…”

Section: Introductionmentioning

confidence: 99%

Decrease in antithrombin III and prothrombin serum levels contribute to coagulation disorders during leptospirosis

et al. 2016

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The Molecular Basis of Leptospiral Pathogenesis

Murray

2014

Current Topics in Microbiology and Immunology

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The mechanisms of disease pathogenesis in leptospirosis are poorly defined. Recent developments in the application of genetic tools in the study of Leptospira have advanced our understanding by allowing the assessment of mutants in animal models. As a result, a small number of essential virulence factors have been identified, though most do not have a clearly defined function. Significant advances have also been made in the in vitro characterization of leptospiral interaction with host structures, including extracellular matrix proteins (such as laminin, elastin, fibronectin, collagens), proteins related to hemostasis (fibrinogen, plasmin), and soluble mediators of complement resistance (factor H, C4b-binding protein), although none of these in vitro findings has been translated to the host animal. Binding to host structures may permit colonization of the host, prevention of blood clotting may contribute to hemorrhage, while interaction with complement resistance mediators may contribute to survival in serum. While not a classical intracellular pathogen, the interaction of leptospires and phagocytic cells appears complex, with bacteria surviving uptake and promoting apoptosis; mutants relating to these processes (such as cell invasion and oxidative stress resistance) are attenuated in vivo. Another feature of leptospiral biology is the high degree of functional redundancy and the surprising lack of attenuation of mutants in what appear to be certain virulence factors, such as LipL32 and LigB. While many advances have been made, there remains a lack of understanding of how Leptospira causes tissue pathology. It is likely that leptospires have many novel pathogenesis mechanisms that are yet to be identified.

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Adhesins of Leptospira interrogans Mediate the Interaction to Fibrinogen and Inhibit Fibrin Clot Formation In Vitro

Cited by 43 publications

References 59 publications

Leptospira and Leptospirosis

Leptospira and Leptospirosis

Decrease in antithrombin III and prothrombin serum levels contribute to coagulation disorders during leptospirosis

The Molecular Basis of Leptospiral Pathogenesis

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