连翘酯苷 A 通过 PPAR-γ/RXR-α 复合物抑制肺和结肠的炎症和上皮屏障损伤,从而减轻急性肺损伤。
Forsythiaside A alleviates acute lung injury by inhibiting inflammation and epithelial barrier damages in lung and colon through PPAR-γ/RXR-α complex.
机构信息
State Key Laboratory of Southwestern Chinese Medicine Resources, School of Pharmacy, Chengdu University of Traditional Chinese Medicine, Chengdu 611137, China.
State Key Laboratory of Southwestern Chinese Medicine Resources, School of Pharmacy, Chengdu University of Traditional Chinese Medicine, Chengdu 611137, China.
出版信息
J Adv Res. 2024 Jun;60:183-200. doi: 10.1016/j.jare.2023.08.006. Epub 2023 Aug 12.
INTRODUCTION
Acute lung injury (ALI) is a lung disease characterized by inflammation and still requires further drug development. Forsythiaside A as the active compound of Forsythiae Fructus has the therapeutic potential for ALI.
OBJECTIVE
To investigate the mechanism of forsythiaside A in treating ALI through PPAR-γ and its conjugate RXR-α based on gut-lung axis.
METHODS
This study constructed in vitro and in vivo injury models using LPS and TNF-α. Forsythiaside A was used for the drug treatment, and RXR-α inhibitor UVI3003 was used to interfere with PPAR-γ/RXR-α complexes in the cells. HE staining was used for histopathological examination. Serum endotoxin contents were determined using limulus lysate kit. IHC staining and Western blot were conducted to assess the protein expressions. ELISA was applied to examine the content of pro-inflammatory cytokines in the cell supernatants. The protein interactions were analyzed via CO-IP.
RESULTS
In vivo results showed that forsythiaside A regulated PPAR-γ/RXR-α and inhibited TLR4/MAPK/NF-κB and MLCK/MLC2 signal pathways, thus inhibiting inflammation and epithelial barrier damages of lung and colon in ALI mice induced by intratracheal LPS. PPAR-γ/RXR-α were promoted by forsythiaside A in lungs, whereas inhibited by forsythiaside A in colons. Additionally, in vitro results showed that forsythiaside A suppressed inflammation and epithelial barrier damages in macrophages and lung/colon epithelial cells, by manipulating PPAR-γ/RXR-α to suppress the LPS- and TNF-α-induced activation of TLR4/MAPK/NF-κB and NF-κB/MLCK/MLC2 signal pathways. Moreover, further mechanism study indicated that forsythiaside A showed a cell-specific regulatory effect on PPAR-γ/RXR-α complex. Specifically, the PPAR-γ/RXR-α protein interactions were promoted by forsythiaside A in LPS-induced macrophages RAW264.7 and TNF-α-induced lung epithelial cells A549, but inhibited by forsythiaside A in TNF-α-induced colon epithelial cells SW620.
CONCLUSION
In the treatment of ALI, Forsythiaside A inhibited inflammation and epithelial barrier damages of lung and colon through its regulation on PPAR-γ/RXR-α complex.
简介
急性肺损伤(ALI)是一种以炎症为特征的肺部疾病,仍需要进一步开发药物。连翘苷 A 作为连翘的活性化合物,具有治疗 ALI 的潜力。
目的
基于肠-肺轴,探讨连翘苷 A 通过 PPAR-γ及其结合体 RXR-α治疗 ALI 的机制。
方法
本研究采用 LPS 和 TNF-α构建了体外和体内损伤模型。用连翘苷 A 进行药物治疗,用 RXR-α抑制剂 UVI3003 干扰细胞中的 PPAR-γ/RXR-α 复合物。HE 染色进行组织病理学检查。鲎试剂试剂盒测定血清内毒素含量。免疫组化染色和 Western blot 检测蛋白表达。ELISA 法检测细胞上清液中促炎细胞因子的含量。通过 CO-IP 分析蛋白质相互作用。
结果
体内结果表明,连翘苷 A 调节 PPAR-γ/RXR-α,抑制 TLR4/MAPK/NF-κB 和 MLCK/MLC2 信号通路,从而抑制 LPS 诱导的 ALI 小鼠肺和结肠的炎症和上皮屏障损伤。PPAR-γ/RXR-α在肺部被连翘苷 A 促进,而在结肠中被连翘苷 A 抑制。此外,体外结果表明,连翘苷 A 通过调控 PPAR-γ/RXR-α抑制 TLR4/MAPK/NF-κB 和 NF-κB/MLCK/MLC2 信号通路,抑制巨噬细胞和肺/结肠上皮细胞的炎症和上皮屏障损伤。此外,进一步的机制研究表明,连翘苷 A 对 PPAR-γ/RXR-α 复合物表现出细胞特异性调节作用。具体来说,连翘苷 A 促进 LPS 诱导的巨噬细胞 RAW264.7 和 TNF-α诱导的肺上皮细胞 A549 中 PPAR-γ/RXR-α 蛋白相互作用,但抑制 TNF-α诱导的结肠上皮细胞 SW620 中 PPAR-γ/RXR-α 蛋白相互作用。
结论
在治疗 ALI 中,连翘苷 A 通过调节 PPAR-γ/RXR-α 复合物抑制肺和结肠的炎症和上皮屏障损伤。
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