Proteomic analysis of the effects of accumulated heat in the gastrointestinal tract on lipopolysaccharide-induced pneumonia in mice

Proteomic analysis of the effects of accumulated heat in the gastrointestinal tract on lipopolysaccharide-induced pneumonia in mice

Objective: To examine the effects of accumulated heat in GI tract (AHGIT) on lung tissue protein expression in pneumonic mice. Methods: Nebulized lipopolysaccharides (LPS) were administered to induce a pneumonic mouse model (M1), and a high-calorie/protein diet combined with nebulized LPS was used t...

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Main Authors: Zi'an Zheng, Chen Bai, Tiegang Liu, Yunhui Wang, Yuxiang Wan, Jingnan Xu, Xueyan Ma, Liyi Yan, He Yu, Jianhua Zhen, Xiaohong Gu
Format: Article
Language:English
Published: Elsevier 2017-04-01
Series:Journal of Traditional Chinese Medical Sciences
Subjects:
AHGIT
Proteomics
Pneumonia
Immunoinflammation
Metabolism
Online Access:http://www.sciencedirect.com/science/article/pii/S2095754817301606
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spelling doaj-d0cdc66dd08941b0a71313d535780c792021-04-02T10:17:49ZengElsevierJournal of Traditional Chinese Medical Sciences2095-75482017-04-014212714010.1016/j.jtcms.2017.09.002Proteomic analysis of the effects of accumulated heat in the gastrointestinal tract on lipopolysaccharide-induced pneumonia in miceZi'an Zheng0Chen Bai1Tiegang Liu2Yunhui Wang3Yuxiang Wan4Jingnan Xu5Xueyan Ma6Liyi Yan7He Yu8Jianhua Zhen9Xiaohong Gu10Beijing University of Chinese Medicine, ChinaBeijing University of Chinese Medicine, ChinaBeijing University of Chinese Medicine, ChinaBeijing University of Chinese Medicine, ChinaBeijing University of Chinese Medicine, ChinaBeijing University of Chinese Medicine, ChinaBeijing University of Chinese Medicine, ChinaBeijing University of Chinese Medicine, ChinaBeijing University of Chinese Medicine, ChinaThe Second Respiratory Department of TCM, China-Japan Friendship Hospital, ChinaBeijing University of Chinese Medicine, ChinaObjective: To examine the effects of accumulated heat in GI tract (AHGIT) on lung tissue protein expression in pneumonic mice. Methods: Nebulized lipopolysaccharides (LPS) were administered to induce a pneumonic mouse model (M1), and a high-calorie/protein diet combined with nebulized LPS was used to induce AHGIT pneumonia (M2). Isobaric tag for relative and absolute quantitation (iTRAQ) proteomics was applied to study lung protein expression, followed by bioinformatics analysis. Results: M1 mice developed alveolar damage with prominent septum thickening, vascular dilation, hyperaemia and infiltration of large amounts of inflammatory cells. M2 mice developed more severe pathological responses. A total of 2626 proteins were reliably identified in the lung tissue. Compared with normal mice, the M1 mice had 344 differentially expressed proteins in their lungs, which are involved in the following biological processes: response to organic substance, response to cytokine, response to external stimulus, defense response and immune system process. They are also involved in the following Kyoto Encyclopedia of Genes and Genomes (KEGG) pathways: ECM-receptor interaction, leukocyte transendothelial migration, Fc gamma R-mediated phagocytosis, complement and coagulation cascades, and antigen processing and presentation. Compared with the M1 group, the M2 mice had 164 differentially expressed proteins in their lungs, including 14 upregulated and 150 downregulated proteins. These proteins are involved in the following biological processes: small molecule metabolism, ribose phosphate metabolic process, cell adhesion and biological adhesion. The relevant KEGG pathways included oxidative phosphorylation, Citrate cycle (TCA cycle), complement and coagulation cascades, and vascular smooth muscle contraction. Conclusions: AHGIT aggravated the lung inflammatory damage in the mice with LPS-induced pneumonia. It may affect the mouse substance/energy metabolism, and therefore the immune function, to aggravate the LPS-induced inflammatory damage.http://www.sciencedirect.com/science/article/pii/S2095754817301606AHGITProteomicsPneumoniaImmunoinflammationMetabolism
collection DOAJ
language English
format Article
sources DOAJ
author Zi'an Zheng
Chen Bai
Tiegang Liu
Yunhui Wang
Yuxiang Wan
Jingnan Xu
Xueyan Ma
Liyi Yan
He Yu
Jianhua Zhen
Xiaohong Gu
spellingShingle Zi'an Zheng
Chen Bai
Tiegang Liu
Yunhui Wang
Yuxiang Wan
Jingnan Xu
Xueyan Ma
Liyi Yan
He Yu
Jianhua Zhen
Xiaohong Gu
Proteomic analysis of the effects of accumulated heat in the gastrointestinal tract on lipopolysaccharide-induced pneumonia in mice
Journal of Traditional Chinese Medical Sciences
AHGIT
Proteomics
Pneumonia
Immunoinflammation
Metabolism
author_facet Zi'an Zheng
Chen Bai
Tiegang Liu
Yunhui Wang
Yuxiang Wan
Jingnan Xu
Xueyan Ma
Liyi Yan
He Yu
Jianhua Zhen
Xiaohong Gu
author_sort Zi'an Zheng
title Proteomic analysis of the effects of accumulated heat in the gastrointestinal tract on lipopolysaccharide-induced pneumonia in mice
title_short Proteomic analysis of the effects of accumulated heat in the gastrointestinal tract on lipopolysaccharide-induced pneumonia in mice
title_full Proteomic analysis of the effects of accumulated heat in the gastrointestinal tract on lipopolysaccharide-induced pneumonia in mice
title_fullStr Proteomic analysis of the effects of accumulated heat in the gastrointestinal tract on lipopolysaccharide-induced pneumonia in mice
title_full_unstemmed Proteomic analysis of the effects of accumulated heat in the gastrointestinal tract on lipopolysaccharide-induced pneumonia in mice
title_sort proteomic analysis of the effects of accumulated heat in the gastrointestinal tract on lipopolysaccharide-induced pneumonia in mice
publisher Elsevier
series Journal of Traditional Chinese Medical Sciences
issn 2095-7548
publishDate 2017-04-01
description Objective: To examine the effects of accumulated heat in GI tract (AHGIT) on lung tissue protein expression in pneumonic mice. Methods: Nebulized lipopolysaccharides (LPS) were administered to induce a pneumonic mouse model (M1), and a high-calorie/protein diet combined with nebulized LPS was used to induce AHGIT pneumonia (M2). Isobaric tag for relative and absolute quantitation (iTRAQ) proteomics was applied to study lung protein expression, followed by bioinformatics analysis. Results: M1 mice developed alveolar damage with prominent septum thickening, vascular dilation, hyperaemia and infiltration of large amounts of inflammatory cells. M2 mice developed more severe pathological responses. A total of 2626 proteins were reliably identified in the lung tissue. Compared with normal mice, the M1 mice had 344 differentially expressed proteins in their lungs, which are involved in the following biological processes: response to organic substance, response to cytokine, response to external stimulus, defense response and immune system process. They are also involved in the following Kyoto Encyclopedia of Genes and Genomes (KEGG) pathways: ECM-receptor interaction, leukocyte transendothelial migration, Fc gamma R-mediated phagocytosis, complement and coagulation cascades, and antigen processing and presentation. Compared with the M1 group, the M2 mice had 164 differentially expressed proteins in their lungs, including 14 upregulated and 150 downregulated proteins. These proteins are involved in the following biological processes: small molecule metabolism, ribose phosphate metabolic process, cell adhesion and biological adhesion. The relevant KEGG pathways included oxidative phosphorylation, Citrate cycle (TCA cycle), complement and coagulation cascades, and vascular smooth muscle contraction. Conclusions: AHGIT aggravated the lung inflammatory damage in the mice with LPS-induced pneumonia. It may affect the mouse substance/energy metabolism, and therefore the immune function, to aggravate the LPS-induced inflammatory damage.
topic AHGIT
Proteomics
Pneumonia
Immunoinflammation
Metabolism
url http://www.sciencedirect.com/science/article/pii/S2095754817301606
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