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Soybean Extract Ameliorates Lung Injury induced by Uranium Inhalation: An integrated strategy of network pharmacology, metabolomics, and transcriptomics - 08/11/24

Doi : 10.1016/j.biopha.2024.117451 
Xin Yang a, 1, Hongying Liang a, 1, Yufu Tang a, Ruifeng Dong a, Qimiao Liu b, Wanqing Pang b, Lixia Su a, Xiaona Gu a, Mengya Liu a, Qingdong Wu a, Xiangming Xue a, , Jingming Zhan a,
a Division of Radiology and Environmental Medicine, China Institute for Radiation Protection, Taiyuan 030006, China 
b Institutes of Biomedical Sciences, Shanxi University, Taiyuan 030006, China 

Corresponding authors.

Abstract

Aim

This study aimed to evaluate the protective effect of soybean extract (SE) against uranium-induced lung injury in rats.

Materials and methods

A rat lung injury model was established through nebulized inhalation of uranyl nitrate. Pretreatment with SE or sterile water (control group) by gavage for seven days before uranium exposure and until the experiment endpoints. The levels of uranium in lung tissues were detected by ICP-MS. Paraffin embedding-based hematoxylin & eosin staining and Masson’s staining for the lung tissue were performed to observe the histopathological imaging features. A public database was utilized to analyze the network pharmacological association between SE and lung injury. The expression levels of proteins indicating fibrosis were measured by enzyme-linked immunosorbent assay. RNA-seq transcriptomic and LC-MS/MS targeted metabolomics were conducted in lung tissues.

Results

Uranium levels in the lung tissues were lower in SE-pretreated rats than in the uranium-treated group. Inflammatory cell infiltration and the deposition of extracellular matrix were attenuated, and the levels of alpha-smooth muscle actin, transforming growth factor beta1, and hydroxyproline decreased in SE-pretreated rats compared to the uranium-treated group. Active ingredients of SE were related to inflammation, oxidative stress, and drug metabolism. A total of 67 differentially expressed genes and 39 differential metabolites were identified in the SE-pretreated group compared to the uranium-treated group, focusing on the drug metabolism-cytochrome P450, glutathione metabolism, IL-17 signaling pathway, complement, and coagulation cascades.

Conclusions

These findings suggest that SE may ameliorate uranium-induced pulmonary inflammation and fibrosis by regulating glutathione metabolism, chronic inflammation, and immune regulation.

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Graphical Abstract




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Highlights

The protective effect of SE was verified in UILI.
An integrated strategy explored the pharmacological mechanism.
SE attenuates UILI by suppressing inflammation and immunomodulation-related gene expression.
SE may attenuate uranium-induced oxidative stress in the lungs.

El texto completo de este artículo está disponible en PDF.

Keywords : Soybean extract, Uranium-induced lung injury, Network pharmacology, Transcriptomics, Metabolomics


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© 2024  The Authors. Publicado por Elsevier Masson SAS. Todos los derechos reservados.
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