Modulation of tumor necrosis factor-induced increase in renal (LLC-PK1) transepithelial permeability

Mullin, James M.; Laughlin, Kathleen V.; Marano, Colleen; Russo, Linda; Soler, Aléjandro Peralta

doi:10.1152/ajprenal.1992.263.5.f915

Cited by 47 publications

(46 citation statements)

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“…Tumor necrosis factor-α (TNF-α) appears to play an important role in regulating intestinal epithelial barrier function since TNFα-neutralizing antibodies restored barrier function in Crohn's disease patients (Suenaert et al, 2002). Exposure of cultured epithelial monolayers to TNF-α in vitro caused epithelial barrier loss (Mullin et al, 1992;Marano et al, 1998). In another study, exposure of cultured epithelial monolayers to TNF-α increased MLC phosphorylation which was associated with impaired barrier function (Zolotarevsky et al, 2002).…”

Section: The Leaky Epithelial Barrier In Intestinal Diseasesmentioning

confidence: 99%

Alcohol, intestinal bacterial growth, intestinal permeability to endotoxin, and medical consequences: Summary of a symposium

Purohit

Bode

et al. 2008

Alcohol

274

220

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Section: The Leaky Epithelial Barrier In Intestinal Diseasesmentioning

confidence: 99%

Alcohol, intestinal bacterial growth, intestinal permeability to endotoxin, and medical consequences: Summary of a symposium

Purohit

Bode

et al. 2008

Alcohol

274

220

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“…50,51 There have been many hypotheses as to the mechanism of TNF-induced barrier dysfunction, including single cell epithelial apoptosis, 52 nonapoptotic mechanisms, 53 and reduced transcription of tight junction proteins. 54 Although a role for each of these processes cannot be excluded, a series of recent reports suggests that TNF regulates tight junction permeability via cytoskeletal contraction.…”

Section: Tnf Regulates Barrier Function In Vitromentioning

confidence: 99%

Molecular Basis of Epithelial Barrier Regulation

Turner

2006

The American Journal of Pathology

488

166

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The intestinal epithelium is faced with the complex task of providing a barrier while also allowing nutrient and water absorption. The frequency with which these processes are disrupted in disease can be taken as evidence of their importance. It is therefore of interest to define the mechanisms of altered intestinal barrier and transport function and develop means to correct diseaseassociated defects. Over the past 10 years, some of the molecular events underlying physiological epithelial barrier regulation have been described. Remarkably, recent advances have shown that activation of the same mechanisms is central to barrier dysfunction in both in vitro and in vivo models of disease. Although the contribution of barrier dysfunction to pathogenesis of chronic disease remains incompletely understood, it is now clear that cytoskeletal regulation of barrier function is both an important pathogenic process and that targeted inhibition of myosin light chain kinase, which affects this cytoskeleton-dependent tight junction dysfunction, is an attractive candidate for therapeutic intervention.

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“…Since macrophages, even metabolically stressed macrophages (Table 1), release a variety of mediators following activation, we opted to focus subsequent studies on TNF-␣, a factor which has been implicated in IBD and has been shown to affect endothelial (11,12), gut (38), and kidney (25,26) epithelial permeability.…”

Section: Dnp Causes Metabolic Stress In Differentiated Macrophagesmentioning

confidence: 99%

“…This loss of epithelial integrity was inhibited by neutralizing antibodies to TNF-␣. Although TNF-␣ can directly increase paracellular permeability across selected renal and enteric epithelial cell lines (25,38), by itself TNF-␣ has minimal direct effects on the barrier properties of T84 cell monolayers (4,23), indicating that TNF-␣ was either activating LPMC and/or working in concert with other mediators released from the LPMC to increase the permeability to T84 cell monolayers (50).…”

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Decreased epithelial barrier function evoked by exposure to metabolic stress and nonpathogenicE. coliis enhanced by TNF-α

Lewis¹,

Caldwell²,

Phan³

et al. 2008

American Journal of Physiology-Gastrointestinal and Liver Physi

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DM. Decreased epithelial barrier function evoked by exposure to metabolic stress and nonpathogenic E. coli is enhanced by TNF-␣. Am J Physiol Gastrointest Liver Physiol 294: G669-G678, 2008. First published January 10, 2008 doi:10.1152/ajpgi.00382.2007.-A defect in mitochondrial activity contributes to many diseases. We have shown that monolayers of the human colonic T84 epithelial cell line exposed to dinitrophenol (DNP, uncouples oxidative phosphorylation) and nonpathogenic Escherichia coli (E. coli) (strain HB101) display decreased barrier function. Here the impact of DNP on macrophage activity and the effect of TNF-␣, DNP, and E. coli on epithelial permeability were assessed. DNP treatment of the human THP-1 macrophage cell line resulted in reduced ATP synthesis, and, although hyporesponsive to LPS, the metabolically stressed macrophages produced IL-1␤, IL-6, and TNF-␣. Given the role of TNF-␣ in inflammatory bowel disease (IBD) and the association between increased permeability and IBD, recombinant TNF-␣ (10 ng/ml) was added to the DNP (0.1 mM) ϩ E. coli (10 6 colony-forming units), and this resulted in a significantly greater loss of T84 epithelial barrier function than that elicited by DNP ϩ E. coli. This increased epithelial permeability was not due to epithelial death, and the enhanced E. coli translocation was reduced by pharmacological inhibitors of NF-␤ signaling (pyrrolidine dithiocarbamate, NF-␤ essential modifier-binding peptide, BAY 11-7082, and the proteosome inhibitor, MG132). In contrast, the drop in transepithelial electrical resistance was unaffected by the inhibitors of NF-␤. Thus, as an integrative model system, our findings support the induction of a positive feedback loop that can severely impair epithelial barrier function and, as such, could contribute to existing inflammation or trigger relapses in IBD. Thus metabolically stressed epithelia display increased permeability in the presence of viable nonpathogenic E. coli that is exaggerated by TNF-␣ released by activated immune cells, such as macrophages, that retain this ability even if they themselves are experiencing a degree of metabolic stress. permeability; bacterial translocation; NFB; T84 cells; macrophages A NUMBER OF PUTATIVE CAUSATIVE agents/mechanisms have been proposed for the inflammatory bowel diseases (IBDs): genetic predisposition, infection, dysregulated immune reactions, triggers from the commensal flora, and a defect in epithelial permeability (44). Abnormal mitochondria have been observed in epithelial cells in tissues resected from patients with Crohn's disease (28), indicating metabolic stress (i.e., ATP depletion) in these individuals. Similarly, reductions in mitochondria acetoacetyl CoA thiolase have been shown in the epithelium of patients with ulcerative colitis, which would result in reduced ATP synthesis from butyrate, and hence these cells would experience a degree of metabolic stress (36). Metabolic stress can arise as a consequence of infection, ischemia, and inflammation itself (8, 14). Thus we hypothes...

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Modulation of tumor necrosis factor-induced increase in renal (LLC-PK1) transepithelial permeability

Cited by 47 publications

References 0 publications

Alcohol, intestinal bacterial growth, intestinal permeability to endotoxin, and medical consequences: Summary of a symposium

Alcohol, intestinal bacterial growth, intestinal permeability to endotoxin, and medical consequences: Summary of a symposium

Molecular Basis of Epithelial Barrier Regulation

Decreased epithelial barrier function evoked by exposure to metabolic stress and nonpathogenicE. coliis enhanced by TNF-α

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