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Literature DB >> 11837790

Nitric oxide directly impairs intestinal barrier function.

Abstract

Excess production of nitric oxide (NO) has been implicated in endotoxin-induced loss of gut barrier function in vivo. Thus, we tested the direct effect of NO on the barrier function of intestinal mucosal membranes suspended ex vivo in Ussing chambers and on IEC-6 enterocyte monolayers. In these experiments, ex vivo-mounted ileal membranes or IEC-6 cell enterocyte monolayers were exposed to the NO donor, S-nitroso-N-acetyl-penicillamine (SNAP) over a dose range (10 microm to 2 mM) or medium. SNAP at concentrations of 1 or 2 mM, but not 10 or 100 microM, increased the rates of bacterial translocation (BT) across both the ileal membranes and the IEC-6 monolayers by >1 log (P < 0.05), as well as the permeability of the IEC-6 monolayers to phenol red (P < 0.05). The ileal membranes exposed to 1 or 2 mM SNAP for 3 h manifested histologic evidence of mucosal injury and decreases in electrical resistance and potential difference values (P < 0.05), while the IEC-6 cells exposed to SNAP for 18 h had increased levels of cell death (P < 0.05). Since NO produced locally by stimulated enterocytes could contribute to barrier dysfunction, NO production, iNOS mRNA levels, and monolayer permeability were measured in enterocytes (IEC-6 and Caco-2) exposed to medium, endotoxin (lipopolysaccharide [25 microg/mL]) or a cytokine mixture (IL-1beta 10 ng/mL, TNF-alpha 10 ng/mL, and INF-gamma 250 U/mL) for 6 or 24 h. Endotoxin increased NO production, iNOS mRNA expression, and monolayer permeability in the IEC-6, but not the Caco-2 cells, while exposure to the cytokine mixture increased both NO production, iNOS mRNA expression, and monolayer permeability in both the IEC-6 and Caco-2 cell lines. Based on the results of these studies it appears that NO can directly increase ileal mucosal membrane and enterocyte monolayer permeability and BT and that increased NO production and iNOS mRNA expression is associated with endotoxin- and/or cytokine-induced loss of enterocyte monolayer barrier function.

Entities: Chemical Disease Gene Species

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Year: 2002 PMID： 11837790 DOI： 10.1097/00024382-200202000-00010

Source DB: PubMed Journal: Shock ISSN： 1073-2322 Impact factor: 3.454

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Cited

21 in total

1. Hypoxia-inducible factor plays a gut-injurious role in intestinal ischemia reperfusion injury.

Authors: Kolenkode B Kannan; Iriana Colorado; Diego Reino; David Palange; Qi Lu; Xiaofa Qin; Billy Abungu; Anthony Watkins; Francis J Caputo; Da-Zhong Xu; Gregg L Semenza; Edwin A Deitch; Rena Feinman
Journal: Am J Physiol Gastrointest Liver Physiol Date: 2010-12-23 Impact factor: 4.052

2. Insulin-like growth factor I improves intestinal barrier function in cirrhotic rats.

Authors: V Lorenzo-Zúñiga; C M Rodríguez-Ortigosa; R Bartolí; M-L Martínez-Chantar; L Martínez-Peralta; A Pardo; I Ojanguren; J Quiroga; R Planas; J Prieto
Journal: Gut Date: 2006-01-24 Impact factor: 23.059

3. Characterization of turkey inducible nitric oxide synthase and identification of its expression in the intestinal epithelium following astrovirus infection.

Authors: R Ryan Meyerhoff; Prashant K Nighot; Rizwana A Ali; Anthony T Blikslager; Matthew D Koci
Journal: Comp Immunol Microbiol Infect Dis Date: 2011-11-25 Impact factor: 2.268

Review 4. Alcohol abuse and the injured host: dysregulation of counterregulatory mechanisms review.

Authors: Patricia E Molina; Jesse K Sulzer; Annie M Whitaker
Journal: Shock Date: 2013-03 Impact factor: 3.454

5. Inducible nitric oxide synthase knockout mice are resistant to diet-induced loss of gut barrier function and intestinal injury.

Authors: Edwin A Deitch; Alexander Shorshtein; Jesse Houghton; Qi Lu; Dazhong Xu
Journal: J Gastrointest Surg Date: 2002 Jul-Aug Impact factor: 3.452

Nitric oxide directly impairs intestinal barrier function.

1. Hypoxia-inducible factor plays a gut-injurious role in intestinal ischemia reperfusion injury.

2. Insulin-like growth factor I improves intestinal barrier function in cirrhotic rats.

3. Characterization of turkey inducible nitric oxide synthase and identification of its expression in the intestinal epithelium following astrovirus infection.

Review 4. Alcohol abuse and the injured host: dysregulation of counterregulatory mechanisms review.

5. Inducible nitric oxide synthase knockout mice are resistant to diet-induced loss of gut barrier function and intestinal injury.

Review 6. iNOS expression in oral and gastrointestinal tract mucosa.

7. Long-term ketamine abuse induces cystitis in rats by impairing the bladder epithelial barrier.

8. Estrogen receptor hormone agonists limit trauma hemorrhage shock-induced gut and lung injury in rats.

9. Tumor necrosis factor alpha increases intestinal permeability in mice with fulminant hepatic failure.

10. Orexigenic hormone ghrelin ameliorates gut barrier dysfunction in sepsis in rats.