Finnegan Sorcha, Robson Joanne, Scaife Caitriona, McAllister Catherine, Pennington Stephen R, Gibson David S, Rooney Madeleine E
Arthritis Res Ther. 2014 Jan 13;16(1):R8. doi: 10.1186/ar4434.
Juvenile idiopathic arthritis (JIA) is the most common rheumatological disease of childhood with a prevalence of around 1 in 1,000. Without appropriate treatment it can have devastating consequences including permanent disability from joint destruction and growth deformities. Disease aetiology remains unknown. Investigation of disease pathology at the level of the synovial membrane is required if we want to begin to understand the disease at the molecular and biochemical level. The synovial membrane proteome from early disease-stage, treatment naive JIA patients was compared between polyarticular and oligoarticular subgroups.
Protein was extracted from 15 newly diagnosed, treatment naive JIA synovial membrane biopsies and separated by two dimensional fluorescent difference in-gel electrophoresis. Proteins displaying a two-fold or greater change in expression levels between the two subgroups were identified by matrix assisted laser desorption ionization-time of flight mass spectrometry with expression further verified by Western blotting and immunohistochemistry.
Analysis of variance analysis (P ≤ 0.05) revealed 25 protein spots with a two-fold or greater difference in expression levels between polyarticular and oligoarticular patients. Hierarchical cluster analysis with Pearson ranked correlation revealed two distinctive clusters of proteins. Some of the proteins that were differentially expressed included: integrin alpha 2b (P = 0.04); fibrinogen D fragment (P = 0.005); collagen type VI (P = 0.03); fibrinogen gamma chain (P = 0.05) and peroxiredoxin 2 (P = 0.02). The identified proteins are involved in a number of different processes including platelet activation and the coagulation system.
The data indicate distinct synovial membrane proteome profiles between JIA subgroups at an early stage in the disease process. The identified proteins also provide insight into differentially perturbed pathways which could influence pathological events at the joint level.
青少年特发性关节炎(JIA)是儿童期最常见的风湿性疾病,患病率约为千分之一。若未经适当治疗,可能会产生毁灭性后果,包括因关节破坏和生长畸形导致的永久性残疾。疾病病因仍不明。如果我们想在分子和生化水平上开始了解该疾病,就需要对滑膜水平的疾病病理学进行研究。比较了多关节型和少关节型亚组中疾病早期、未接受过治疗的JIA患者的滑膜蛋白质组。
从15例新诊断的、未接受过治疗的JIA滑膜活检样本中提取蛋白质,通过二维荧光差异凝胶电泳进行分离。通过基质辅助激光解吸电离飞行时间质谱法鉴定在两个亚组之间表达水平有两倍或更大变化的蛋白质,并通过蛋白质印迹法和免疫组织化学进一步验证其表达。
方差分析(P≤0.05)显示,多关节型和少关节型患者之间有25个蛋白质斑点的表达水平有两倍或更大差异。采用Pearson等级相关性的层次聚类分析显示出两个不同的蛋白质簇。一些差异表达的蛋白质包括:整合素α2b(P = 0.04);纤维蛋白原D片段(P = 0.005);Ⅵ型胶原(P = 0.03);纤维蛋白原γ链(P = 0.05)和过氧化物酶2(P = 0.02)。所鉴定的蛋白质参与了许多不同的过程,包括血小板活化和凝血系统。
数据表明在疾病过程的早期,JIA亚组之间的滑膜蛋白质组谱不同。所鉴定的蛋白质也为可能影响关节水平病理事件的差异扰动途径提供了见解。
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