4.7 Article

Ameliorative effect of Berberidis radix polysaccharide selenium nanoparticles against carbon tetrachloride induced oxidative stress and inflammation

期刊

FRONTIERS IN PHARMACOLOGY
卷 13, 期 -, 页码 -

出版社

FRONTIERS MEDIA SA
DOI: 10.3389/fphar.2022.1058480

关键词

Berberidis radix polysaccharide; selenium nanoparticles; oxidative stress; hepatoprotection; anti-inflammation

资金

  1. Key R and D Program of Shandong Province (Major Scientific and Technological Innovation Project) [2021CXGC011305]
  2. Natural Science Foundation of Shandong Province of China [ZR2020QC198]
  3. Qingdao Agricultural University Doctoral Start-Up Fund [6631121044, 6631118020]
  4. National Natural Science Foundation of China [82003941, 31802229]
  5. Special Foundation for Taishan Scholar of Shandong Province

向作者/读者索取更多资源

In this study, BRP-selenium nanoparticles (BRP-SeNPs) were prepared using Berberidis radix polysaccharide (BRP) as capping agents, and their properties and pharmacological functions were investigated. The results showed that BRP-SeNPs exhibited hepatoprotective effects and attenuated oxidative stress and inflammation.
Berberidis radix polysaccharide (BRP) extracted as capping agents was applied to prepare BRP-selenium nanoparticles (BRP-SeNPs) in the redox reaction system of sodium selenite and ascorbic acid. The stability and characterization of BRP-SeNPs were investigated by physical analysis method. The results revealed that BRP were tightly wrapped on the surface of SeNPs by forming C-O...Se bonds or hydrogen bonding interaction (O-H...Se). BRP-SeNPs presented irregular, fragmented and smooth surface morphology and polycrystalline nanoring structure, and its particle size was 89.4 nm in the optimal preparation condition. The pharmacologic functions of BRP-SeNPs were explored in vitro and in vivo. The results showed that BRP-SeNPs could heighten the cell viabilities and the enzyme activity of GSH-Px and decrease the content of MDA on H2O2-induced AML-12 cells injury model. In vivo tests, the results displayed that BRP-SeNPs could increase the body weight of mice, promote the enzyme activity like SOD and GSH-Px, decrease the liver organ index and the hepatic function index such as ALT, AST, CYP2E1, reduce the content of MDA, and relieve the proinflammation factors of NO, IL-1 beta and TNF-alpha in CCl4-induced mice injury model. Liver tissue histopathological studies corroborated the improvement of BRP-SeNPs on liver of CCl4-induced mice. The results of Western blot showed that BRP-SeNPs could attenuate oxidant stress by the Nrf2/Keap1/MKP1/JNK pathways, and downregulate the proinflammatory factors by TLR4/MAPK pathway. These findings suggested that BRP-SeNPs possess the hepatoprotection and have the potential to be a green liver-protecting and auxiliary liver inflammation drugs.

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