多发性肌炎患者中针对运动神经元存活复合体的自身抗体:D、E、F和G蛋白的免疫沉淀,无小核核糖核蛋白的其他成分。
Autoantibodies to survival of motor neuron complex in patients with polymyositis: immunoprecipitation of D, E, F, and G proteins without other components of small nuclear ribonucleoproteins.
作者信息
Satoh Minoru, Chan Jason Y F, Ross Steven J, Ceribelli Angela, Cavazzana Ilaria, Franceschini Franco, Li Yi, Reeves Westley H, Sobel Eric S, Chan Edward K L
机构信息
University of Florida, Gainesville, FL, USA.
出版信息
Arthritis Rheum. 2011 Jul;63(7):1972-8. doi: 10.1002/art.30349.
OBJECTIVE
Autoantibodies in the systemic rheumatic diseases are clinically useful biomarkers of the diagnosis or of certain clinical characteristics. An unusual pattern of immunoprecipitation, in which the D, E, F, and G proteins of small nuclear RNPs (snRNP) but without other components of the snRNP, was noticed at the autoantibody screening. The purpose of this study was to examine the target antigens and clinical manifestations associated with this specificity.
METHODS
Autoantibodies in sera from 1,966 American patients (including 434 with systemic lupus erythematosus, 121 with scleroderma, 86 with polymyositis/dermatomyositis [PM/DM]) and 248 Italian patients with autoimmune diseases were screened by immunoprecipitation of (35) S-methionine-labeled cell extracts. Sera with which D, E, F, and G proteins of snRNP was immunoprecipitated, but without the other snRNP proteins, were further examined by analysis of RNA components by immunoprecipitation (silver staining), Western blotting using survival of motor neuron (SMN) complex, and immunofluorescence.
RESULTS
Three sera that immunoprecipitated D, E, F, and G proteins without other components (U1-70K, A, B'/B, C) of the snRNP were found. Four additional proteins (130 kd, 120 kd, 38 kd, and 33 kd) were also commonly immunoprecipitated. The target antigen was identified as SMN complex (Gemin 3, Gemin 4, SMN, and Gemin 2, respectively), which plays a critical role in the assembly of snRNP. In immunofluorescence analyses, all 3 sera showed nuclear dots (Cajal bodies) and cytoplasmic staining. Only 1 serum was weakly positive on Western blotting of SMN, suggesting that these sera mainly recognize native molecule or quaternary structure. All 3 patients were white women with PM, an interesting finding, since deletion or mutation of SMN is known to cause spinal muscular atrophy.
CONCLUSION
SMN complex was identified as a new Cajal body autoantigen recognized by sera from white patients with PM. The biologic and clinical significance of anti-SMN autoantibodies will need to be clarified.
目的
系统性风湿性疾病中的自身抗体是诊断或某些临床特征的临床有用生物标志物。在自身抗体筛查中发现了一种不寻常的免疫沉淀模式,即小核核糖核蛋白(snRNP)的D、E、F和G蛋白出现免疫沉淀,但snRNP的其他成分未出现。本研究的目的是检测与这种特异性相关的靶抗原和临床表现。
方法
通过对(35)S-甲硫氨酸标记的细胞提取物进行免疫沉淀,对1966例美国患者(包括434例系统性红斑狼疮患者、121例硬皮病患者、86例多发性肌炎/皮肌炎[PM/DM]患者)和248例意大利自身免疫性疾病患者血清中的自身抗体进行筛查。对snRNP的D、E、F和G蛋白出现免疫沉淀但其他snRNP蛋白未出现的血清,通过免疫沉淀(银染)分析RNA成分、使用运动神经元存活(SMN)复合体进行蛋白质印迹以及免疫荧光进一步检测。
结果
发现3份血清能免疫沉淀snRNP的D、E、F和G蛋白,而snRNP的其他成分(U1-70K、A、B'/B、C)未出现。另外4种蛋白(130 kd、120 kd、38 kd和33 kd)也常出现免疫沉淀。靶抗原被鉴定为SMN复合体(分别为Gemin 3、Gemin 4、SMN和Gemin 2),其在snRNP组装中起关键作用。在免疫荧光分析中,所有3份血清均显示核点(卡哈尔体)和细胞质染色。只有1份血清在SMN的蛋白质印迹上呈弱阳性,提示这些血清主要识别天然分子或四级结构。所有3例患者均为患有PM的白人女性,这一发现很有趣,因为已知SMN的缺失或突变会导致脊髓性肌萎缩。
结论
SMN复合体被鉴定为患有PM的白人患者血清识别的一种新的卡哈尔体自身抗原。抗SMN自身抗体的生物学和临床意义有待阐明。
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