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Histology and histopathology
Jul, 2024;39 (7): 921-934.

Inflammatory suppression and immunity regulation benefits of honokiol in a rat model of acute peritonitis via the regulation of NLRP3 inflammasome and Sirt1/autophagy axis.

Ximing Pan, Zhou Hua, Guocai Fan, Qinglong Feng
Author Information
  1. Ximing Pan: Department of Emergency, Suichang People's Hospital, Lishui , PR China.
  2. Zhou Hua: Department of Nephrology, Suichang People's Hospital, Lishui, PR China.
  3. Guocai Fan: Department of Breast Surgery, Suichang People's Hospital, Lishui, PR China.
  4. Qinglong Feng: Intensive Care Unit, Quzhou Kecheng People's Hospital, Quzhou, PR China. qinglongfengicu@sina.com.
PMID: 38112214 DOI: 10.14670/HH-18-688

Abstract

BACKGROUND: NLRP3 inflammasome and Sirt1/autophagy axis are potential targets for advancing acute peritonitis (AP). Honokiol (HNK), a bioactive substance, has the potential to improve AP.
MATERIALS AND METHODS: The AP model rats were established by cecal ligation and puncture (CLP). Rats were randomized into the Sham, Sham+HNK, CLP, and CLP+HNK groups. The therapeutic effects of HNK on organ infection, inflammation and immunity were observed in AP rats. The inflammation of RAW 264.7 cells was induced by lipopolysaccharide (LPS) and divided into the Control, HNK, LPS, and LPS+HNK groups. The effects of HNK on immunity and inflammation were observed. Moreover, the inflammatory cell model was further transfected with NLRP3 overexpressing plasmid, and the regulatory effect of HNK on NLRP3 in AP cells was detected.
RESULTS: HNK treatment improved survival, biochemical indexes, and lung and kidney injury and inhibited inflammatory cytokine release and bacterial infection in CLP rats. In CLP rats and RAW 264.7 cells, HNK treatment improved the release of the CD4+ and CD8+ T cells, decreased the associated proteins' levels of the NLRP3 inflammasome, and activated the expression of proteins in the Sirt1/autophagy axis. It improved viability and reduced apoptosis and the degrees of TNF-��, IL-1��, and IL-6 mRNA in RAW 264.7 cells. In addition, HNK treatment antagonized the effect of NLRP3-overexpressed on inflammation and immunity.
CONCLUSIONS: HNK improved AP by inhibiting NLRP3 inflammasome and activating the Sirt1 autophagy axis and .

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MeSH Term

Animals
Male
Mice
Rats
Acute Disease
Allyl Compounds
Anti-Inflammatory Agents
Autophagy
Biphenyl Compounds
Disease Models, Animal
Inflammasomes
Inflammation
Lignans
NLR Family, Pyrin Domain-Containing 3 Protein
Peritonitis
Phenols
Rats, Sprague-Dawley
RAW 264.7 Cells
Signal Transduction
Sirtuin 1

Chemicals

Allyl Compounds
Anti-Inflammatory Agents
Biphenyl Compounds
honokiol
Inflammasomes
Lignans
NLR Family, Pyrin Domain-Containing 3 Protein
Nlrp3 protein, rat
Phenols
Sirt1 protein, rat
Sirtuin 1
Journal Article

Word Cloud

Created with Highcharts 10.0.0HNKNLRP3APcellsinflammasomeaxisratsCLPinflammationimmunityimprovedSirt1/autophagymodelRAW2647treatmentpotentialacuteperitonitisgroupseffectsinfectionobservedLPSinflammatoryeffectreleaseregulationBACKGROUND:targetsadvancingHonokiolbioactivesubstanceimproveMATERIALSANDMETHODS:establishedcecalligationpunctureRatsrandomizedShamSham+HNKCLP+HNKtherapeuticorganinducedlipopolysaccharidedividedControlLPS+HNKMoreovercelltransfectedoverexpressingplasmidregulatorydetectedRESULTS:survivalbiochemicalindexeslungkidneyinjuryinhibitedcytokinebacterialCD4+CD8+Tdecreasedassociatedproteins'levelsactivatedexpressionproteinsviabilityreducedapoptosisdegreesTNF-��IL-1��IL-6mRNAadditionantagonizedNLRP3-overexpressedCONCLUSIONS:inhibitingactivatingSirt1autophagyInflammatorysuppressionbenefitshonokiolratvia

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