Enteropathogenic
 Escherichia coli
 ,
 Shigella flexneri
 , and
 Listeria monocytogenes
 Recruit a Junctional Protein, Zonula Occludens-1, to Actin Tails and Pedestals

Hanajima-Ozawa, Miyuki; Matsuzawa, Takeshi; Fukui, Atsushi; Kamitani, Shigeki; Ohnishi, Hiroe; Abe, Akio; Horiguchi, Yasuhiko; Miyake, Masami

doi:10.1128/iai.01479-06

Cited by 34 publications

(24 citation statements)

References 59 publications

(71 reference statements)

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“…5G and H; yellow pedestals). This was recently reported by Hanajima-Ozawa et al (15), who showed recruitment of ZO-1 into pedestals caused by a human EPEC strain. Moreover, cells infected with the wild type transformed with pespF showed pedestals bigger than those seen in cells infected with the untransformed wild type (Fig.…”

Section: Resultsmentioning

confidence: 51%

EspF Interacts with Nucleation-Promoting Factors To Recruit Junctional Proteins into Pedestals for Pedestal Maturation and Disruption of Paracellular Permeability

Peralta-Ramirez¹,

Hernández²,

Manning‐Cela

et al. 2008

Infect Immun

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Many pathogenic bacteria subvert normal host cell processes by delivering effector proteins which mimic eukaryotic functions directly into target cells. EspF is a multifunctional protein injected into host cells by attaching and effacing pathogens, but its mechanism of action is not understood completely. In silico analyses of EspF revealed two key motifs: proline-rich domains and PDZ domain binding motifs. Such functional domains may allow EspF to act as an actin nucleation-promoting factor by mimicking host proteins. In agreement with these predictions, we found that EspF from rabbit enteropathogenic Escherichia coli (E22) participates in the regulation of actin polymerization by binding to a complex of proteins at the tight junctions (TJ). EspF bound to actin and profilin throughout the course of infection. However, after 2 h of infection, EspF also bound to the neural Wiskott-Aldrich syndrome protein and to the Arp2/3, zonula occludens-1 (ZO-1), and ZO-2 proteins. Moreover, EspF caused occludin, claudin, ZO-1, and ZO-2 redistribution and loss of transepithelial electrical resistance, suggesting that actin sequestration by EspF may cause local actin depolymerization leading to EspF-induced TJ disruption. Furthermore, EspF caused recruitment of these TJ proteins into the pedestals. An E22 strain lacking EspF did not cause TJ disruption and pedestals were smaller than those induced by the wild-type strain. Additionally, the pedestals were located mainly in the TJ. The overexpression of EspF caused bigger pedestals located along the length of the cells. Thus, actin sequestration by EspF allows the recruitment of junctional proteins into the pedestals, leading to the maturation of actin pedestals and the disruption of paracellular permeability.

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Section: Resultsmentioning

confidence: 51%

EspF Interacts with Nucleation-Promoting Factors To Recruit Junctional Proteins into Pedestals for Pedestal Maturation and Disruption of Paracellular Permeability

Peralta-Ramirez¹,

Hernández²,

Manning‐Cela

et al. 2008

Infect Immun

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“…L. monocytogenes infection is known to reduce the TEER of epithelial monolayers (33), as also observed in this study (Table 2), which can contribute to paracellular bacterial translocation (15,27). Although the exact mechanism for a Listeriainduced reduction in TEER is unknown, it has been linked to virulence traits such as actin cytoskeleton disruption following invasion (26,52,60), as well as extracellular secretion of LLO (50). Although the presence or absence of LAP expression did not induce changes in TEER (Table 2), it is possible that a weakened epithelial barrier facilitates LAP-Hsp60-mediated bacterial translocation.…”

mentioning

confidence: 54%

Listeria monocytogenes Uses Listeria Adhesion Protein (LAP) To Promote Bacterial Transepithelial Translocation and Induces Expression of LAP Receptor Hsp60

Burkholder¹,

Bhunia

2010

Infect Immun

110

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“…In contrast, our findings indicate an opposite sequence of events, where bacteria enter into infected eukaryotic cells to induce changes in intercellular junctions by altering signal transduction pathways. A similar sequence of events has also been described for other invasive pathogens (38), but contrasts with Helicobacter pylori infection, which is reported to alter the physiology of apical junctional complexes without entering into the cytoplasm (39).…”

Section: Discussionmentioning

confidence: 94%

Campylobacter jejuni Mediated Disruption of Polarized Epithelial Monolayers is Cell-Type Specific, Time Dependent, and Correlates With Bacterial Invasion

2008

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The precise mechanism by which the most common cause of bacterial enterocolitis in humans, Campylobacter jejuni, perturbs the intestinal mucosa remains elusive. To define effects of C. jejuni infection on mucosal permeability, Madin-Darby canine kidney (MDCK)-I and T84 cell monolayers were infected with C. jejuni for up to 48 h. All three tested C. jejuni strains caused a 73-78% reduction in transepithelial electrical resistance (TER) in intestinal (T84) cell monolayers, whereas only one strain slightly reduced TER of MDCK-I cells by 25% after 48 h infection. Infection with C. jejuni strains also caused a 2.3-4.5-fold increase in dextran permeability, but only in T84 cells. C. jejuni infection of monolayers also caused morphologic changes in desmosomes, observed by transmission electron microscopy. The cell-type specificity, demonstrated by increased T84 monolayer permeability, correlated with higher bacterial invasion into these cells, relative to MDCK-I cells. In T84 cells, invasion and bacterial translocation preceded barrier disruption and inhibition of C. jejuni invasion using a pharmacological inhibitor of phosphoinositide 3-kinase, reduced the drop in TER. These findings suggest that C. jejuni disruption of monolayers is mediated by invasion, provide new insights into C. jejuni-host epithelial barrier interactions, and offer potential mechanisms of intestinal injury and chronic immune stimulation. (Pediatr Res 64: 599-604, 2008)

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Enteropathogenic Escherichia coli , Shigella flexneri , and Listeria monocytogenes Recruit a Junctional Protein, Zonula Occludens-1, to Actin Tails and Pedestals

Cited by 34 publications

References 59 publications

EspF Interacts with Nucleation-Promoting Factors To Recruit Junctional Proteins into Pedestals for Pedestal Maturation and Disruption of Paracellular Permeability

EspF Interacts with Nucleation-Promoting Factors To Recruit Junctional Proteins into Pedestals for Pedestal Maturation and Disruption of Paracellular Permeability

Listeria monocytogenes Uses Listeria Adhesion Protein (LAP) To Promote Bacterial Transepithelial Translocation and Induces Expression of LAP Receptor Hsp60

Campylobacter jejuni Mediated Disruption of Polarized Epithelial Monolayers is Cell-Type Specific, Time Dependent, and Correlates With Bacterial Invasion

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