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6 results on '"Ozolek, John"'

1. Toll-like receptor 4-mediated lymphocyte influx induces neonatal necrotizing enterocolitis

Author

Egan, Charlotte E., Sodhi, Chhinder P., Good, Misty, Lin, Joyce, Jia, Hongpeng, Yamaguchi, Yukihiro, Lu, Peng, Ma, Congrong, Branca, Maria F., Weyandt, Samantha, Fulton, William B., Nino, Diego F., Prindle, Jr., Thomas, Ozolek, John A., and Hackam, David J.

Subjects
Gene expression -- Health aspects, Enterocolitis, Neonatal necrotizing -- Comparative analysis -- Genetic aspects -- Development and progression, Enterocolitis, Pseudomembranous -- Comparative analysis -- Genetic aspects -- Development and progression, Toll-like receptors -- Health aspects, Disease susceptibility -- Genetic aspects, Health care industry
Abstract

The nature and role of the intestinal leukocytes in necrotizing enterocolitis (NEC), a severe disease affecting premature infants, remain unknown. We now show that the intestine in mouse and human NEC is rich in lymphocytes that are required for NEC development, as recombination activating gene 1-deficient ([Rag1.sup.-/-]) mice were protected from NEC and transfer of intestinal lymphocytes from NEC mice into naive mice induced intestinal inflammation. The intestinal expression of the lipopolysaccharide receptor TLR4, which is higher in the premature compared with full-term human and mouse intestine, is required for lymphocyte influx through TLR4-mediated upregulation of CCR9/CCL25 signaling. TLR4 also mediates a STAT3-dependent polarization toward increased proinflammatory [CD3.sup.+][CD4.sup.+][IL-17.sup.+] and reduced tolerogenic [Foxp3.sup.+] Treg lymphocytes (Tregs). Th17 lymphocytes were required for NEC development, as inhibition of STAT3 or IL-17 receptor signaling attenuated NEC in mice, while IL-17 release impaired enterocyte tight junctions, increased enterocyte apoptosis, and reduced enterocyte proliferation, leading to NEC. Importantly, TLR4-dependent Th17 polarization could be reversed by the enteral administration of retinoic acid, which induced Tregs and decreased NEC severity. These findings identify an important role for proinflammatory lymphocytes in NEC development via intestinal epithelial TLR4 that could be reversed through dietary modification., Introduction Necrotizing enterocolitis (NEC) is a severe inflammatory disease that affects the gastrointestinal tract of the premature infant and that causes significant morbidity and mortality in this vulnerable population (1). [...]

Published
2016
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2. Interferon-[gamma] inhibits enterocyte migration by reversibly displacing connexin43 from lipid rafts

Author

Leaphart, Cynthia L., Dai, Shipan, Gribar, Steven C., Richardson, Ward, Ozolek, John, Shi, Xia-hua, Bruns, Jennifer R., Branca, Maria, Li, Jun, Weisz, Ora A., Sodhi, Chhinder, and Hackam, David J.

Subjects
Interferon gamma -- Properties, Cell migration -- Evaluation, Cell junctions -- Properties, Enterocolitis, Neonatal necrotizing -- Development and progression, Enterocolitis, Pseudomembranous -- Development and progression, Cytokines -- Properties, Biological sciences
Abstract

Necrotizing enterocolitis (NEC) is associated with the release of interferon-[gamma] (IFN) by enterocytes and delayed intestinal restitution. Our laboratory has recently demonstrated that IFN inhibits enterocyte migration by impairing enterocyte gap junctions, intercellular channels that are composed of connexin43 (Cx43) monomers and that are required for enterocyte migration to occur. The mechanisms by which IFN inhibits gap junctions are incompletely understood. Lipid rafts are cholesterol-sphingolipid-rich microdomains of the plasma membrane that play a central role in the trafficking and signaling of various proteins. We now hypothesize that Cx43 is present on enterocyte lipid rafts and that IFN inhibits enterocyte migration by displacing Cx43 from lipid rafts in enterocytes. We now confirm our previous observations that intestinal restitution is impaired in NEC and demonstrate that Cx43 is present on lipid rafts in IEC-6 enterocytes. We show that lipid rafts are required for enterocyte migration, that IFN displaces Cx43 from lipid rafts, and that the phorbol ester phorbol 12-myristate 13-acetate (PMA) restores Cx43 to lipid rafts after treatment with IFN in a protein kinase C-dependent manner. IFN also reversibly decreased the phosphorylation of Cx43 on lipid rafts, which was restored by PMA. Strikingly, restoration of Cx43 to lipid rafts by PMA or by transfection of enterocytes with adenoviruses expressing wild-type Cx43 but not mutant Cx43 is associated with the restoration of enterocyte migration after IFN treatment. Taken together, these findings suggest an important role for lipid raft-Cx43 interactions in the regulation of enterocyte migration during exposure to IFN, such as NEC. gap junctions; connexin; necrotizing enterocolitis; cytokine; phorbol ester

Published
2008

5. Basal/myoepithelial cells in chronic sinusitis, respiratory epithelial adenomatoid hamartoma, inverted papilloma, and intestinal-type and nonintestinal-type sinonasal adenocarcinoma: an immunohistochemical study

Author

Ozolek, John A., Barnes, E. Leon, and Hunt, Jennifer L.

Subjects
Nose cancer -- Research, Adenocarcinoma -- Research, Histochemistry -- Research, Health
Abstract

* Context.--The pathogenesis of respiratory epithelial adenomatoid hamartoma (REAH) and inverted papilloma (IP) is poorly understood, especially compared with sinonasal adenocarcinoma (SNAC). One feature of malignant glandular lesions is loss [...]

Published
2007

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