Wang J-X, Tang W, Zhou R, Wan J, Shi L-P, Zhang Y, Yang Y-F, Li Y, Zuo J-P
First Department of Pharmacology, State Key Laboratory of Drug Research, Shanghai Institute of Materia Medica, Chinese Academy of Sciences, Shanghai, PR China.
Br J Pharmacol. 2008 Mar;153(6):1303-10. doi: 10.1038/bjp.2008.11. Epub 2008 Feb 11.
Our previous study showed that SM905, a novel artemisinin derivative, exhibited potent immunosuppressive activity. In this study, we evaluate preventive and therapeutic effect of SM905 on collagen-induced arthritis (CIA) in DBA/1 mice, and investigate its mechanisms both in inflammatory and autoimmune aspects of the disease.
CIA was induced by type II bovine collagen (CII) in DBA/1 mice. SM905 was given orally either before (continuously 1 day before booster immunization) or after disease onset (continuously 14 days after booster immunization). Disease incidence and severity were monitored, mRNA expression of proinflammatory mediators was determined by real-time PCR, purified T cell proliferation was assessed using [(3)H]-thymidine incorporated assay, and T helper (Th) 17/Th1/Th2 type cytokine production was examined by ELISA.
Oral treatment with SM905 delayed disease onset, reduced arthritis incidence and severity, and suppressed the enhanced expression of pro-inflammatory cytokines, chemokines and chemokine receptors in draining lymph nodes. The CII-induced T cell proliferation and production of interleukin (IL)-17A by T cells were strikingly inhibited. Correspondingly, the mRNA expression of IL-17A and RORgamma t (a specific transcription factor for Th17) was also reduced. This effect was coupled with a striking reduction of IL-6 production, which has a critical role in Th17 development. In established arthritis, SM905 profoundly inhibited disease progression, reduced IL-17A and RORgamma t mRNA expression, and suppressed pro-inflammatory mediator expression in arthritic joints.
SM905 had beneficial effects on CIA by suppressing inflammatory and pathogenic Th17 responses.
我们之前的研究表明,新型青蒿素衍生物SM905具有强大的免疫抑制活性。在本研究中,我们评估了SM905对DBA/1小鼠胶原诱导性关节炎(CIA)的预防和治疗作用,并从该疾病的炎症和自身免疫方面研究其作用机制。
用II型牛胶原蛋白(CII)诱导DBA/1小鼠患CIA。在加强免疫前(加强免疫前连续1天)或疾病发作后(加强免疫后连续14天)口服给予SM905。监测疾病发病率和严重程度,通过实时PCR测定促炎介质的mRNA表达,使用[(3)H]-胸腺嘧啶掺入法评估纯化的T细胞增殖,并通过ELISA检测辅助性T(Th)17/Th1/Th2型细胞因子的产生。
口服SM905可延迟疾病发作,降低关节炎发病率和严重程度,并抑制引流淋巴结中促炎细胞因子、趋化因子和趋化因子受体的表达增强。CII诱导的T细胞增殖和T细胞产生白细胞介素(IL)-17A受到显著抑制。相应地,IL-17A和RORγt(Th17的特异性转录因子)的mRNA表达也降低。这种作用伴随着IL-6产生的显著减少,IL-6在Th17发育中起关键作用。在已建立的关节炎中,SM905可显著抑制疾病进展,降低IL-17A和RORγt mRNA表达,并抑制关节炎关节中促炎介质的表达。
SM905通过抑制炎症性和致病性Th17反应对CIA具有有益作用。