Eynott Paul R, Xu Li, Bennett Brydon L, Noble Alistair, Leung Sum-Yee, Nath Puneeta, Groneberg David A, Adcock Ian M, Chung K Fan
Thoracic Medicine, National Heart and Lung Institute, Imperial College School of Medicine, London, UK.
Immunology. 2004 Jul;112(3):446-53. doi: 10.1111/j.1365-2567.2004.01887.x.
Jun N-terminal kinase (JNK) has been implicated in the pathogenesis of inflammatory diseases including asthma. We examined the effect of SP600125 (anthra [1,9-cd] pyrazol-6 (2H)-one), a novel inhibitor of JNK in a model of asthma. Brown-Norway rats were sensitized to ovalbumin and treated with SP600125 intraperitoneally (90 mg/kg in total). SP600125 inhibited allergen-induced, increased activity of phosphorylated c-jun but not of phosphorylated-MAPKAPK2, indicative of activation of p38 MAPK, in the lung. SP600125 inhibited macrophage (P < 0.04), lymphocyte (P < 0.05), eosinophil (P < 0.04) and neutrophil (P < 0.005) numbers in bronchoalveolar lavage. Eosinophil and T-cell accumulation in the airways, mRNA expression for interleukin-1beta, tumour necrosis factor-beta, interleukin-3, interleukin-4 and interleukin-5, serum levels of allergen-specific immunoglobulin E and bronchial hyperresponsiveness were not affected by SP600125. Selective inhibition of JNK reduced inflammatory cell egress into the airway lumen after single allergen exposure. The role of JNK mitogen-activated protein kinase activation may be limited in the pathogenesis of bronchial hyperresponsiveness after single allergen exposure.
Jun氨基末端激酶(JNK)与包括哮喘在内的炎症性疾病的发病机制有关。我们在哮喘模型中研究了新型JNK抑制剂SP600125(蒽[1,9-cd]吡唑-6(2H)-酮)的作用。将棕色挪威大鼠用卵清蛋白致敏,然后腹腔注射SP600125(总量90mg/kg)。SP600125抑制了变应原诱导的肺中磷酸化c-jun活性的增加,但未抑制磷酸化MAPKAPK2的活性,这表明p38 MAPK被激活。SP600125抑制了支气管肺泡灌洗中的巨噬细胞数量(P<0.04)、淋巴细胞数量(P<0.05)、嗜酸性粒细胞数量(P<0.04)和中性粒细胞数量(P<0.005)。气道中的嗜酸性粒细胞和T细胞积聚、白细胞介素-1β、肿瘤坏死因子-β、白细胞介素-3、白细胞介素-4和白细胞介素-5的mRNA表达、变应原特异性免疫球蛋白E的血清水平以及支气管高反应性均不受SP600125的影响。单次变应原暴露后,JNK丝裂原活化蛋白激酶激活的作用在支气管高反应性的发病机制中可能有限。