Laboratory of Anti-inflammation and Immunopharmacology, Shanghai Institute of Materia Medica, Chinese Academy of Sciences, Shanghai 201203, China.
School of Pharmacy, University of Chinese Academy of Sciences, Beijing 100049, China.
J Adv Res. 2021 Mar 4;33:241-251. doi: 10.1016/j.jare.2021.02.006. eCollection 2021 Nov.
Arctigenin, derived from Arctium lappa L., has multiple pharmacological activities, including immunoregulatory, anti-diabetic, anti-tumor, and neuroprotective effects. Nevertheless, the potential therapeutic target of arctigenin in modulating inflammation remains undefined.
In the present study, we identified that arctigenin was a phosphodiesterase-4 (PDE4) selective inhibitor for the first time. Further investigations were performed to fully uncover the effects and mechanism of arctigenin on experimental murine psoriasis model.
Crystal structure determination, PDEs enzyme assay, and isothermal titration calorimetry were included to illustrate the binding specialty, inhibitory effects, and selectivity of arctigenin on PDE4D. The anti-inflammatory effects were conducted in LPS-activated human peripheral blood mononuclear cells (PBMCs) and RAW264.7 cells. Imiquimod-induced murine psoriasis was performed to uncover the therapeutic effects and mechanism of arctigenin .
Arctigenin could bind to the catalytic domain of PDE4D via formation of hydrogen bonds as well as π-π stacking interactions between the dibenzyl butyrolactone of arctigenin and several residues of PDE4D. Accordingly, arctigenin showed prominent anti-inflammation in human PBMCs and murine RAW264.7 cells. PDE4 inhibition by arctigenin resulted in elevation of intracellular cyclic adenosine monophosphate (cAMP) and phosphorylation of cAMP-response element binding protein (CREB), which were largely blocked through intervention of protein kinase A (PKA) activity by H89 treatment or reduction of protein expression by siRNA transfection. Moreover, we first identified that a topical application of arctigenin ameliorated experimental psoriatic manifestations in imiquimod-induced murine psoriasis model by decreasing adhesion and chemotaxis of several inflammatory cells. Further proteomics analysis revealed that arctigenin could rectify the immune dysfunction and hyperactivation of keratinocytes in the inflamed skin microenvironments, which might be largely related to the expression of Keratins.
The research provided credible clew that inhibition of PDE4 by arctigenin might function as the potential therapeutic approach for the treatment of psoriasis.
牛蒡子苷元来源于牛蒡(Arctium lappa L.),具有多种药理活性,包括免疫调节、抗糖尿病、抗肿瘤和神经保护作用。然而,牛蒡子苷元在调节炎症方面的潜在治疗靶点尚不清楚。
本研究首次发现牛蒡子苷元是一种磷酸二酯酶 4(PDE4)选择性抑制剂。进一步的研究旨在充分揭示牛蒡子苷元对实验性银屑病模型的作用机制。
通过晶体结构测定、PDEs 酶测定和等温滴定量热法阐明了牛蒡子苷元与 PDE4D 的结合特异性、抑制作用和选择性。在脂多糖激活的人外周血单核细胞(PBMCs)和 RAW264.7 细胞中进行了抗炎作用研究。采用咪喹莫特诱导的小鼠银屑病模型揭示了牛蒡子苷元的治疗作用和机制。
牛蒡子苷元可通过氢键和π-π堆积相互作用与 PDE4D 的二苄基丁内酯形成复合物,从而与 PDE4D 的催化结构域结合。因此,牛蒡子苷元在人 PBMCs 和鼠 RAW264.7 细胞中表现出显著的抗炎作用。牛蒡子苷元抑制 PDE4 导致细胞内环腺苷酸(cAMP)水平升高和 cAMP 反应元件结合蛋白(CREB)磷酸化,这一过程可通过 H89 处理抑制蛋白激酶 A(PKA)活性或 siRNA 转染降低蛋白表达而被阻断。此外,我们首次发现,牛蒡子苷元通过减少几种炎症细胞的黏附和趋化作用,改善了咪喹莫特诱导的小鼠银屑病模型中的实验性银屑病表现。进一步的蛋白质组学分析表明,牛蒡子苷元可以纠正炎症皮肤微环境中的免疫功能障碍和角质形成细胞的过度激活,这可能与角蛋白的表达有很大关系。
该研究为牛蒡子苷元抑制 PDE4 可能作为治疗银屑病的潜在治疗方法提供了可靠的线索。
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