白细胞介素-6家族细胞因子受体gp130的酪氨酸759位点发生点突变,会加剧DBA/1J小鼠的胶原诱导性关节炎。
Point mutation of tyrosine 759 of the IL-6 family cytokine receptor, gp130, augments collagen-induced arthritis in DBA/1J mice.
作者信息
Tsuji Fumio, Yoshimi Miwa, Katsuta Osamu, Takai Miwa, Ishihara Katsuhiko, Aono Hiroyuki
机构信息
Research and Development Center, Santen Pharmaceutical Co, Ltd, Ikoma-shi, Nara, Japan.
出版信息
BMC Musculoskelet Disord. 2009 Feb 19;10:23. doi: 10.1186/1471-2474-10-23.
BACKGROUND
Knock-in mice (gp130F759) with a Y759F point mutation in gp130, a signal transducing receptor subunit shared by members of the IL-6 cytokine family, show sustained activation of STAT3, enhanced acute-phase or immune responses, and autoimmune arthritis. We conducted a detailed analysis of collagen-induced arthritis (CIA) in gp130F759 with a DBA/1J background (D/J.gp130F759).
METHODS
We backcrossed gp130F759 to C57BL/6 and DBA/1J, and compared the pathologic changes, including occurrence of arthritis, in the two distinct genetic backgrounds. We analyzed CIA in D/J.gp130F759 and investigated the effects of methotrexate (MTX) on CIA.
RESULTS
C57BL/6 background gp130F759 mice, but not D/J.gp130F759, spontaneously developed polyarthritis and glomerulonephritis. On the other hand, keratitis of the eyes only developed in D/J.gp130F759, indicating the influence of genetic background on disease development in gp130F759 mice. Resistance of the DBA/1J background against spontaneous arthritis urged us to examine CIA in D/J.gp130F759. CIA in D/J.gp130F759 was more severe, with greater bone destruction, than the control mice. After collagen immunization, splenomegaly and serum levels of rheumatoid factor and anti-DNA antibody were augmented in D/J.gp130F759. Bio-Plex analysis of serum cytokines revealed increased IL-12p40 and PDGF-BB before immunization, and increased levels of IFN-gamma, IL-17, TNF-alpha, IL-9, and MIP-1beta 8 days after the booster dose. IL-6 and PDGF-BB in D/J.gp130F759 showed distinct kinetics from the other cytokines; higher levels were observed after arthritis development. MTX partially attenuated the development of arthritis and inhibited bone destruction in D/J.gp130F759, with reduction of anti-type II collagen antibody levels, suggesting that MTX mainly affects antigen-specific immune responses in CIA.
CONCLUSION
The Tyr-759 point mutation of the IL-6 family cytokine receptor subunit, gp130, caused autoimmune disease, and this was also influenced by the genetic background. CIA in D/J.gp130F759 is useful for evaluating drugs in a relatively short period because sustained activation of STAT3 may enhance the disease symptoms.
背景
携带IL-6细胞因子家族成员共有的信号转导受体亚基gp130中Y759F点突变的敲入小鼠(gp130F759)表现出STAT3的持续激活、增强的急性期或免疫反应以及自身免疫性关节炎。我们对具有DBA/1J背景(D/J.gp130F759)的gp130F759小鼠的胶原诱导性关节炎(CIA)进行了详细分析。
方法
我们将gp130F759回交到C57BL/6和DBA/1J,并比较了这两种不同遗传背景下的病理变化,包括关节炎的发生情况。我们分析了D/J.gp130F759中的CIA,并研究了甲氨蝶呤(MTX)对CIA的影响。
结果
C57BL/6背景的gp130F759小鼠会自发发展为多关节炎和肾小球肾炎,而D/J.gp130F759小鼠则不会。另一方面,仅D/J.gp130F759小鼠发生了眼部角膜炎,这表明遗传背景对gp130F759小鼠疾病发展有影响。DBA/1J背景对自发关节炎的抗性促使我们研究D/J.gp130F759中的CIA。D/J.gp130F759中的CIA比对照小鼠更严重,骨破坏更大。胶原免疫后,D/J.gp130F759小鼠的脾脏肿大以及类风湿因子和抗DNA抗体的血清水平升高。血清细胞因子的生物芯片分析显示,免疫前IL-12p40和血小板衍生生长因子BB(PDGF-BB)升高,加强免疫剂量8天后,干扰素-γ、白细胞介素-17、肿瘤坏死因子-α、白细胞介素-9和巨噬细胞炎性蛋白-1β水平升高。D/J.gp130F759中的白细胞介素-6和PDGF-BB与其他细胞因子表现出不同的动力学;关节炎发生后观察到更高水平。MTX部分减轻了D/J.gp130F759小鼠关节炎的发展并抑制了骨破坏,同时抗II型胶原抗体水平降低,这表明MTX主要影响CIA中的抗原特异性免疫反应。
结论
IL-6家族细胞因子受体亚基gp130的Tyr-759点突变导致了自身免疫性疾病,并且这也受到遗传背景的影响。D/J.gp130F759中的CIA对于在相对较短的时间内评估药物很有用,因为STAT3持续激活可能会加重疾病症状。
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