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KMID : 0620920220540111927
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Experimental & Molecular Medicine
2022 Volume.54 No. 11 p.1927 ~ p.1939
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The natural product salicin alleviates osteoarthritis progression by binding to IRE1¥á and inhibiting endoplasmic reticulum stress through the IRE1¥á-I¥êB¥á-p65 signaling pathway
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Zhu Zhenglin
Gao Shengqiang
Chen Cheng
Xu Wei
Xiao Pengcheng
Chen Zhiyu
Du Chengcheng
Chen Bowen
Gao Yan
Wang Chunli
Liao Junyi
Huang Wei
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Abstract
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Despite the high prevalence of osteoarthritis (OA) in older populations, disease-modifying OA drugs (DMOADs) are still lacking. This study was performed to investigate the effects and mechanisms of the small molecular drug salicin (SA) on OA progression. Primary rat chondrocytes were stimulated with TNF-¥á and treated with or without SA. Inflammatory factors, cartilage matrix degeneration markers, and cell proliferation and apoptosis markers were detected at the mRNA and protein levels. Cell proliferation and apoptosis were evaluated by EdU assays or flow cytometric analysis. RNA sequencing, molecular docking and drug affinity-responsive target stability analyses were used to clarify the mechanisms. The rat OA model was used to evaluate the effect of intra-articular injection of SA on OA progression. We found that SA rescued TNF-¥á-induced degeneration of the cartilage matrix, inhibition of chondrocyte proliferation, and promotion of chondrocyte apoptosis. Mechanistically, SA directly binds to IRE1¥á and occupies the IRE1¥á phosphorylation site, preventing IRE1¥á phosphorylation and regulating IRE1¥á-mediated endoplasmic reticulum (ER) stress by IRE1¥á-I¥êB¥á-p65 signaling. Finally, intra-articular injection of SA-loaded lactic-co-glycolic acid (PLGA) ameliorated OA progression by inhibiting IRE1¥á-mediated ER stress in the OA model. In conclusion, SA alleviates OA by directly binding to the ER stress regulator IRE1¥á and inhibits IRE1¥á-mediated ER stress via IRE1¥á-I¥êB¥á-p65 signaling. Topical use of the small molecular drug SA shows potential to modify OA progression.
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KEYWORD
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