补肺活血胶囊通过抑制pyrin结构域3核苷样受体炎症小体激活和巨噬细胞极化，减轻矽肺的网络药理学作用。

Journal of traditional Chinese medicine = Chung i tsa chih ying wen pan Pub Date : 2024-12-01 DOI:10.19852/j.cnki.jtcm.20240626.004

Hang Wenlu, Wang Lin, B O Yun, Zuo Shurun, Wang Songquan, L I Haiquan, B U Chunlu, Zhao Jie, Zhou Xianmei

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引用次数: 0

摘要

目的：利用网络药理学分析方法预测补肺活血胶囊（BFHX）的作用靶点，探讨其在矽肺大鼠模型中的作用和功能靶点。方法：通过网络药理学分析，将药物靶点与疾病靶点进行关联，探索BFHX影响矽肺的靶点及信号通路。培养NR8383细胞，验证核心基因和通路。建立矽肺大鼠模型，验证BFHX （0.82 g/kg）是否减轻二氧化硅所致肺纤维化的机制，以及它如何影响关键靶点和通路。结果：BFHX与硅基因靶点重叠产生159个互作靶点，通过网络拓扑分析筛选出55个互作靶点。基因本体论和京都基因百科及基因组富集分析结果表明，BFHX可能通过含pyrin结构域3 （NLRP3）的核苷酸样受体炎症体影响矽肺。在NR8383细胞中，BFHX可抑制NLRP3炎性体相关核心基因的表达。BFHX可降低大鼠肺泡炎程度和胶原沉积，减轻sio2诱导大鼠肺纤维化。透射电镜观察二氧化硅暴露后肺巨噬细胞的焦亡现象。BFHX减轻了焦亡的形态学特征。BFHX还能降低矽肺模型大鼠肺组织中NLRP3、caspase-1、白细胞介素-1β (IL-1β)、IL-18、IL-6、肿瘤坏死因子- α的表达。能量色散谱法测定BFHX对支气管肺泡灌洗液中K离子含量的影响。BFHX干预后，CD68+和CD206+的表达也有所降低。结论：nod样受体信号在BFHX对矽肺的作用中起重要作用。它通过NLRP3炎性体激活抑制肺巨噬细胞焦亡和极化，发挥抗肺纤维化作用。

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Bufei Huoxue capsule alleviates silicosis by inhibiting the activation of nucleotide-like receptor containing pyrin domain 3 inflammasome and macrophages polarization based on network pharmacology.

Objective: To predict the targets of Bufei Huoxue capsule (, BFHX) using network pharmacology analysis and to explore its effects and functional targets in a silicotic rat model.

Methods: The drug and disease targets were correlated through network pharmacology analysis to explore the targets and signaling pathways of BFHX affecting silicosis. NR8383 cells were cultured to verify the core genes and pathways. A rat model of silicosis was established to verify whether the mechanism behind SiO2-caused pulmonary fibrosis was alleviated by BFHX (0.82 g/kg) and how it affected key targets and pathways.

Results: Overlapping BFHX and silicotic gene targets produced 159 interactive targets, and 55 were screened by network topology analysis. The results of gene ontology and Kyoto encyclopedia of genes and genomes enrichment analyses suggested that BFHX could affect silicosis through the nucleotide-like receptor containing pyrin domain 3 (NLRP3) inflammasome. In NR8383 cells, the expression of core genes related to the NLRP3 inflammasome could be inhibited by BFHX treatment. BFHX reduced the degree of alveolitis and collagen deposition, attenuating pulmonary fibrosis in SiO2-induced rat model. Pulmonary macrophage pyroptosis after SiO2 exposure was observed under transmission electron microscopy. BFHX alleviated the morphological characteristics of pyroptosis. BFHX also reduced the expression of NLRP3, caspase-1, interleukin-1 beta (IL-1β), IL-18, IL-6, and tumor necrosis factor-alpha in lung tissues of silicotic rat model. BFHX affected the K ion content in bronchoalveolar lavage fluid when assessed by energy dispersive spectrometer testing. The expression of CD68+ and CD206+ were also reduced after BFHX intervention.

Conclusion: NOD-like receptor signaling is vital for BFHX's effects on silicosis. It exerts anti-pulmonary fibrosis effects by inhibiting pulmonary macrophage pyroptosis and polarization through NLRP3 inflammasome activation.

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Journal of traditional Chinese medicine = Chung i tsa chih ying wen pan

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