Protein arginine deiminase 4 inhibition is sufficient for the amelioration of collagen‐induced arthritis

V. Willis, N. Banda, K. N. Cordova, P. Chandra, W. Robinson, D. C. Cooper, D. Lugo, G. Mehta, S. Taylor, P. Tak, R. Prinjha, H. Lewis, V. Holers
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引用次数: 83

Abstract

Citrullination of joint proteins by the protein arginine deiminase (PAD) family of enzymes is recognized increasingly as a key process in the pathogenesis of rheumatoid arthritis. This present study was undertaken to explore the efficacy of a novel PAD4‐selective inhibitor, GSK199, in the murine collagen‐induced arthritis model of rheumatoid arthritis. Mice were dosed daily from the time of collagen immunization with GSK199. Efficacy was assessed against a wide range of end‐points, including clinical disease scores, joint histology and immunohistochemistry, serum and joint citrulline levels and quantification of synovial autoantibodies using a proteomic array containing joint peptides. Administration of GSK199 at 30 mg/kg led to significant effects on arthritis, assessed both by global clinical disease activity and by histological analyses of synovial inflammation, pannus formation and damage to cartilage and bone. In addition, significant decreases in complement C3 deposition in both synovium and cartilage were observed robustly with GSK199 at 10 mg/kg. Neither the total levels of citrulline measurable in joint and serum, nor levels of circulating collagen antibodies, were affected significantly by treatment with GSK199 at any dose level. In contrast, a subset of serum antibodies reactive against citrullinated and non‐citrullinated joint peptides were reduced with GSK199 treatment. These data extend our previous demonstration of efficacy with the pan‐PAD inhibitor Cl‐amidine and demonstrate robustly that PAD4 inhibition alone is sufficient to block murine arthritis clinical and histopathological end‐points.
抑制蛋白精氨酸脱亚胺酶4足以改善胶原诱导的关节炎
蛋白精氨酸脱亚胺酶(PAD)家族对关节蛋白的瓜氨酸化作用越来越被认为是类风湿关节炎发病的关键过程。本研究旨在探讨一种新型PAD4选择性抑制剂GSK199在类风湿性关节炎小鼠胶原诱导的关节炎模型中的作用。小鼠从胶原蛋白免疫开始每天给药。疗效通过广泛的终点进行评估,包括临床疾病评分、关节组织学和免疫组织化学、血清和关节瓜氨酸水平,以及使用含有关节肽的蛋白质组学阵列对滑膜自身抗体进行量化。GSK199以30 mg/kg的剂量给药对关节炎有显著影响,通过全球临床疾病活动性和滑膜炎症、滑膜形成和软骨和骨损伤的组织学分析来评估。此外,10 mg/kg的GSK199显著降低了滑膜和软骨中的补体C3沉积。GSK199治疗对关节和血清中可测量的瓜氨酸总水平和循环胶原抗体水平均无显著影响。相比之下,GSK199治疗降低了针对瓜氨酸化和非瓜氨酸化关节肽的血清抗体亚群。这些数据扩展了我们之前对pan - PAD抑制剂Cl -脒的有效性论证,并有力地证明了单独抑制PAD4足以阻断小鼠关节炎的临床和组织病理学终点。
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