Guo Qingqing, Zheng Kang, Fan Danping, Zhao Yukun, Li Li, Bian Yanqin, Qiu Xuemei, Liu Xue, Zhang Ge, Ma Chaoying, He Xiaojuan, Lu Aiping
Institute of Basic Research in Clinical Medicine, China Academy of Chinese Medical SciencesBeijing, China.
Institute for Advancing Translational Medicine in Bone and Joint Diseases, School of Chinese Medicine, Hong Kong Baptist UniversityKowloon Tong, Hong Kong.
Front Pharmacol. 2017 May 3;8:230. doi: 10.3389/fphar.2017.00230. eCollection 2017.
This study aimed to explore underlying action mechanism of Wu-Tou decoction (WTD) in rheumatoid arthritis (RA) through network pharmacology prediction and experimental verification. Chemical compounds and human target proteins of WTD as well as RA-related human genes were obtained from TCM Database @ Taiwan, PubChem and GenBank, respectively. Subsequently, molecular networks and canonical pathways presumably involved in the treatment of WTD on RA were generated by ingenuity pathway analysis (IPA) software. Furthermore, experimental validation was carried out with MIP-1β-induced U937 cell model and collagen induced arthritis (CIA) rat model. CCR5 signaling pathway in macrophages was shown to be the top one shared signaling pathway associated with both cell immune response and cytokine signaling. In addition, protein kinase C (PKC) δ and p38 in this pathway were treated as target proteins of WTD in RA. experiments indicated that WTD inhibited MIP-1β-induced production of TNF-α, MIP-1α, and RANTES as well as phosphorylation of CCR5, PKC δ, and p38 in U937 cells. WTD treatment maintained the inhibitory effects on production of TNF-α and RANTES in MIP-1β-induced U937 cells after CCR5 knockdown. experiments demonstrated that WTD ameliorated symptoms in CIA rats, decreased the levels of IL-1β, IL-2, IL-6, TNF-α, MIP-1α, MIP-2, RANTES, and IP-10 in serum of CIA rats, as well as mRNA levels of MIP-1α, MIP-2, RANTES, and IP-10 in ankle joints of CIA rats. Furthermore, WTD also lowered the phosphorylation levels of CCR5, PKC δ and p38 in both ankle joints and macrophages in ankle joints from CIA rats. It was demonstrated in this research that WTD played a role in inhibiting inflammatory response in RA which was closely connected with the modulation effect of WTD on CCR5 signaling pathway in macrophages.
本研究旨在通过网络药理学预测和实验验证,探索乌头汤(WTD)治疗类风湿关节炎(RA)的潜在作用机制。分别从台湾中医药数据库、PubChem和GenBank获取乌头汤的化学成分和人类靶蛋白以及RA相关的人类基因。随后,通过Ingenuity Pathway Analysis(IPA)软件生成了可能参与乌头汤治疗RA的分子网络和经典通路。此外,利用MIP-1β诱导的U937细胞模型和胶原诱导性关节炎(CIA)大鼠模型进行了实验验证。巨噬细胞中的CCR5信号通路被证明是与细胞免疫反应和细胞因子信号传导相关的首要共享信号通路。此外,该通路中的蛋白激酶C(PKC)δ和p38被视为乌头汤在RA中的靶蛋白。实验表明,乌头汤可抑制MIP-1β诱导的U937细胞中TNF-α、MIP-1α和RANTES的产生以及CCR5、PKC δ和p38的磷酸化。在CCR5基因敲低后,乌头汤处理对MIP-1β诱导的U937细胞中TNF-α和RANTES的产生仍具有抑制作用。实验证明,乌头汤可改善CIA大鼠的症状,降低CIA大鼠血清中IL-1β、IL-2、IL-6、TNF-α、MIP-1α、MIP-2、RANTES和IP-10的水平,以及CIA大鼠踝关节中MIP-1α、MIP-2、RANTES和IP-10的mRNA水平。此外,乌头汤还降低了CIA大鼠踝关节和踝关节巨噬细胞中CCR5、PKC δ和p38的磷酸化水平。本研究表明,乌头汤在抑制RA炎症反应中发挥作用,这与乌头汤对巨噬细胞中CCR5信号通路的调节作用密切相关。
