Autoantibodies against human calpastatin in rheumatoid arthritis: epitope mapping and analysis of patient sera.

K J Lackner, U Schlosser, B Lang, G Schmitz
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引用次数: 30

Abstract

Autoantibodies against calpastatin have recently been described to be highly prevalent in sera of patients with rheumatoid arthritis (RA). When the sera of 45 patients with RA were analysed for autoantibodies against calpastatin by a newly developed enzyme-linked immunosorbent assay (ELISA), only four sera (8.9%) tested positive, which is not significantly different from the frequency observed in healthy controls. Since the ELISA is based on a synthetic peptide containing the C-terminal 27 amino acids of calpastatin bound to the solid phase, this negative result might be the consequence of the small antigen used. Therefore, a systematic analysis of the epitopes for autoantibodies in calpastatin was performed using sera from RA patients and healthy individuals. Recombinant fusion proteins containing fragments of calpastatin or the complete protein were produced and sera analysed by Western blots. In the N-terminal portion (amino acids 1-369), at least two major epitopes exist, against which 65% of normal sera as well as 76% of RA sera show reactivity in Western blot assays. These epitopes are not useful for clinical diagnostics. Only five out of 45 (11.1%) RA sera reacted against the C-terminal portion (amino acids 363-708) of calpastatin, while four out of 52 (7.7%) control sera showed reactivity. Three of the five RA sera and two out of four control sera had autoantibodies against the C-terminal 27 amino acids of calpastatin. These three patient sera had already been tested positive in the ELISA. The fourth patient positive in the ELISA was Western blot negative. The differences between the group of RA patients and controls are not statistically significant. When the clinical characteristics of the four patients with autoantibodies against the carboxyl end of calpastatin were analysed, it became apparent that all four had significantly elevated C-reactive protein (>50 mg/l). This observation might indicate that calpastatin autoantibodies are found in RA patients with more active disease. Thus, while the majority of RA patients do not have an increased prevalence of calpastatin autoantibodies, it cannot be ruled out definitively that a small subgroup may be characterized by autoantibodies to the C-terminus of calpastatin.

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类风湿关节炎中抗人钙pastatin的自身抗体:表位定位和患者血清分析。
抗calpastatin的自身抗体最近在类风湿关节炎(RA)患者的血清中高度流行。用新开发的酶联免疫吸附试验(ELISA)对45例RA患者的血清进行calpastatin自身抗体分析,只有4例(8.9%)血清呈阳性,与健康对照组的阳性率无显著差异。由于ELISA是基于含有钙pastatin的c端27个氨基酸结合到固相的合成肽,因此该阴性结果可能是使用小抗原的结果。因此,使用RA患者和健康个体的血清对calpastatin中自身抗体的表位进行了系统的分析。制备含有钙pastatin片段或完整蛋白的重组融合蛋白,并用Western blots分析血清。在n端部分(氨基酸1-369),至少存在两个主要的表位,65%的正常血清和76%的RA血清在Western blot检测中显示出反应性。这些表位对临床诊断没有用处。45份RA血清中只有5份(11.1%)对calpastatin的c末端(363-708氨基酸)有反应,而52份对照血清中有4份(7.7%)有反应。5个RA血清中的3个和4个对照血清中的2个具有针对calpastatin c -末端27个氨基酸的自身抗体。这三名患者的血清在酶联免疫吸附试验中均呈阳性。第4例ELISA阳性患者为Western blot阴性。RA患者组与对照组比较差异无统计学意义。当分析4例calpastatin羧基端自身抗体患者的临床特征时,很明显,4例患者的c反应蛋白明显升高(>50 mg/l)。这一观察结果可能表明calpastatin自身抗体在RA患者的活动性更强。因此,虽然大多数RA患者没有calpastatin自身抗体的增加,但不能明确排除一小部分患者可能以calpastatin c端自身抗体为特征。
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