Literature DB >> 23364425

Rattus model utilizing selective pulmonary ischemia induces bronchiolitis obliterans organizing pneumonia.

John C Densmore1, Paul M Jeziorczak, Anne V Clough, Kirkwood A Pritchard, Breana Cummens, Meetha Medhora, Arjun Rao, Elizabeth R Jacobs.   

Abstract

Bronchiolitis obliterans organizing pneumonia (BOOP), a morbid condition when associated with lung transplant and chronic lung disease, is believed to be a complication of ischemia. Our goal was to develop a simple and reliable model of lung ischemia in the Sprague-Dawley rat that would produce BOOP. Unilateral ischemia without airway occlusion was produced by an occlusive slipknot placed around the left main pulmonary artery. Studies were performed 7 days later. Relative pulmonary and systemic flow to each lung was measured by injection of technetium Tc 99m macroaggregated albumin. Histological sections were examined for structure and necrosis and scored for BOOP. Apoptosis was detected by immunohistochemistry with an antibody against cleaved caspase 3. Pulmonary artery blood flow to left lungs was less than 0.1% of the cardiac output, and bronchial artery circulation was ∼2% of aortic artery flow. Histological sections from ischemic left lungs consistently showed Masson bodies, inflammation, and young fibroblasts filling the distal airways and alveoli, consistent with BOOP. In quantitative evaluation of BOOP using epithelial changes, inflammation and fibrosis were higher in ischemic left lungs than right or sham-operated left lungs. Apoptosis was increased in areas exhibiting histological BOOP, but there was no histological evidence of necrosis. Toll-like receptor 4 expression was increased in ischemic left lungs over right. An occlusive slipknot around the main left pulmonary artery in rats produces BOOP, providing direct evidence that ischemia without immunomodulation or coinfection is sufficient to initiate this injury. It also affords an excellent model to study signaling and genetic mechanisms underlying BOOP.

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Year:  2013        PMID: 23364425      PMCID: PMC3578046          DOI: 10.1097/SHK.0b013e318281a58c

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


  62 in total

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  7 in total

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Authors:  John C Densmore; Terry R Schaid; Paul M Jeziorczak; Meetha Medhora; Said Audi; Shraddha Nayak; John Auchampach; Melinda R Dwinell; Aron M Geurts; Elizabeth R Jacobs
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2.  Assessment of Protection Offered By the NRF2 Pathway Against Hyperoxia-Induced Acute Lung Injury in NRF2 Knockout Rats.

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3.  Autophagy, TERT, and mitochondrial dysfunction in hyperoxia.

Authors:  Andreas M Beyer; Laura E Norwood Toro; William E Hughes; Micaela Young; Anne V Clough; Feng Gao; Meetha Medhora; Said H Audi; Elizabeth R Jacobs
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4.  In vivo molecular imaging stratifies rats with different susceptibilities to hyperoxic acute lung injury.

Authors:  Said H Audi; Pardis Taheri; Ming Zhao; Kurt Hu; Elizabeth R Jacobs; Anne V Clough
Journal:  Am J Physiol Lung Cell Mol Physiol       Date:  2022-08-09       Impact factor: 6.011

5.  99MTc-Hexamethylpropyleneamine Oxime Imaging for Early Detection of Acute Lung Injury in Rats Exposed to Hyperoxia or Lipopolysaccharide Treatment.

Authors:  Said H Audi; Anne V Clough; Steven T Haworth; Meetha Medhora; Mahsa Ranji; John C Densmore; Elizabeth R Jacobs
Journal:  Shock       Date:  2016-10       Impact factor: 3.454

6.  Two Genetically Similar H9N2 Influenza A Viruses Show Different Pathogenicity in Mice.

Authors:  Qingtao Liu; Yuzhuo Liu; Jing Yang; Xinmei Huang; Kaikai Han; Dongmin Zhao; Keran Bi; Yin Li
Journal:  Front Microbiol       Date:  2016-11-04       Impact factor: 5.640

7.  Protection by Inhaled Hydrogen Therapy in a Rat Model of Acute Lung Injury can be Tracked in vivo Using Molecular Imaging.

Authors:  Said H Audi; Elizabeth R Jacobs; Xiao Zhang; Amadou K S Camara; Ming Zhao; Meetha M Medhora; Benjamin Rizzo; Anne V Clough
Journal:  Shock       Date:  2017-10       Impact factor: 3.454

  7 in total

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