Hyperforin modulates MAPK/CCL11 signaling to reduce the inflammatory response of nasal mucosal epithelial cells caused by allergic rhinitis by targeting BCL6

IF 2.4 4区 医学 Q3 MEDICINE, RESEARCH & EXPERIMENTAL Experimental and therapeutic medicine Pub Date : 2023-10-27 DOI:10.3892/etm.2023.12278
Chen Xu, Wen Su
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Abstract

Hyperforin is a type of bicyclic tetraketone with four isoprenoid chains extracted from Hypericum perforatum L. that has multiple biological activities such as anti‑diabetes, antitumor and anti‑inflammation. However, the role and potential mechanism of hyperforin in allergic rhinitis (AR) remains to be clarified. In the present study, cell viability was analyzed using Cell Counting Kit‑8 assay, while inflammation was detected using ELISA and reverse transcription‑quantitative PCR. Epithelial cell barrier damage was measured using western blotting and immunofluorescence staining. The expression levels of B‑cell lymphoma 6 (BCL6) and the p38 MAPK/C‑C motif chemokine 11 (CCL11) pathway were detected using western blotting. In addition, the association between hyperforin and BCL6 was analyzed by SWISS TargetPrediction, DisGeNET, Gene Ontology and Pathway databases. Molecular docking was performed using AutoDockTools 1.5.6 and Discovery Studio 4.5 software. The data demonstrated that there were 16 interlinking target genes of hyperforin with AR, in which BCL6 was the most relevant one with hyperforin in AR. The binding between hyperforin and BCL6 was verified, and molecular docking was modeled. The results revealed that hyperforin inhibited IL‑13‑induced nasal epithelial inflammatory cytokine release and repressed the damage to the cellular barrier from IL‑13 stimulation. In addition, hyperforin activated BCL6 expression and significantly suppressed the expression of p38 MAPK/CCL11. Silencing of BCL6 reversed the effects of hyperforin on IL‑13‑induced inflammation and barrier damage. In summary, the present results revealed that hyperforin suppressed IL‑13‑induced nasal epithelial cell inflammation and barrier damage by targeting BCL6/p38 MAPK/CCL11, which may provide promising therapeutic targets for AR.
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hyperperforin通过靶向BCL6调控MAPK/CCL11信号通路,降低变应性鼻炎引起的鼻黏膜上皮细胞炎症反应
贯叶连翘素是一种从贯叶连翘中提取的具有4条类异戊二烯链的双环四酮类化合物,具有抗糖尿病、抗肿瘤、抗炎症等多种生物活性。然而,hyperperin在变应性鼻炎(AR)中的作用和潜在机制尚不清楚。在本研究中,使用cell Counting Kit - 8测定法分析细胞活力,使用ELISA和反转录定量PCR检测炎症。采用western blotting和免疫荧光染色检测上皮细胞屏障损伤。采用western blotting检测B细胞淋巴瘤6 (BCL6)和p38 MAPK/C‑C基序趋化因子11 (CCL11)通路的表达水平。此外,通过SWISS TargetPrediction、DisGeNET、Gene Ontology和Pathway数据库分析hyperperforin与BCL6的相关性。使用AutoDockTools 1.5.6和Discovery Studio 4.5软件进行分子对接。数据显示,hyperperforin与AR有16个互联靶基因,其中BCL6是AR中与hyperperforin关联最密切的基因。验证了hyperperforin与BCL6的结合,并建立了分子对接模型。结果显示,hyperperin抑制IL - 13诱导的鼻上皮炎性细胞因子释放,抑制IL - 13刺激对细胞屏障的损伤。此外,hyperperforin激活BCL6的表达,显著抑制p38 MAPK/CCL11的表达。BCL6的沉默逆转了hyperperin对IL - 13诱导的炎症和屏障损伤的作用。综上所述,本研究结果表明,hyperperin通过靶向BCL6/p38 MAPK/CCL11抑制IL - 13诱导的鼻上皮细胞炎症和屏障损伤,可能为AR的治疗提供有希望的靶点。
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来源期刊
Experimental and therapeutic medicine
Experimental and therapeutic medicine MEDICINE, RESEARCH & EXPERIMENTAL-
CiteScore
1.50
自引率
0.00%
发文量
570
审稿时长
1 months
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