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抗多核点/Sp100自身抗体的临床意义

Clinical significance of anti-multiple nuclear dots/Sp100 autoantibodies.

作者信息

Wichmann I, Montes-Cano M A, Respaldiza N, Alvarez A, Walter K, Franco E, Sanchez-Roman J, Núñez-Roldán A

机构信息

Servicio de Immunología, Hospital Universitario Virgen del Rocío, Servicio Andaluz de Salud, Seville, Spain.

出版信息

Scand J Gastroenterol. 2003 Sep;38(9):996-9. doi: 10.1080/00365520310004876.

Abstract

BACKGROUND

Autoantibodies against discrete variable-sized dots observed in HEp2 cells by indirect immunofluorescence (IIF) test, called multiple nuclear dots (MND), have been closely associated with primary biliary cirrhosis (PBC). Some authors have argued that this antibody is also present in connective tissue diseases or liver diseases other than PBC as autoimmune chronic active hepatitis, particularly of the cholestatic type. We studied an unselected group of patients routinely tested for autoantibodies and positive for the MND pattern and tried to establish the correlation between the presence of this antibody and their diagnosis.

METHODS

A commercial ELISA test, using a recombinant 26 kD truncated sequence of the Sp100 protein, corresponding to an immunodominant molecular region, was used to assess the clinical correlation of these autoantibodies in 110 patients showing an anti-MND immunofluorescence pattern.

RESULTS

One-hundred-and-ten patients were MND positive by IIF. Of these, 100 were Sp100 positive by ELISA. In the Sp100 positive group, 34 had a diagnosis of PBC (30 definite and 4 suspected) while 15 patients had a non-PBC hepatopathy. Unexpectedly, 13 of the MND/Sp100 positive pattern corresponded to systemic lupus erythematosus (SLE) patients and 5 cases to collagen diseases. Another divergence with previous reports was that 34 of the positive patients showed very heterogeneous clinical pictures, different from hepatopathies or collagen diseases.

CONCLUSIONS

Anti-Sp100 antibodies can be found in many clinical conditions. Testing for MND/Sp100 positivity is useful for the diagnosis of PBC, but only when the right clinical context is present. Other diseases cannot be excluded in first line SLE.

摘要

背景

通过间接免疫荧光(IIF)试验在HEp2细胞中观察到的针对离散可变大小斑点的自身抗体,称为多核斑点(MND),与原发性胆汁性肝硬化(PBC)密切相关。一些作者认为,这种抗体也存在于结缔组织疾病或除PBC之外的肝脏疾病中,如自身免疫性慢性活动性肝炎,尤其是胆汁淤积型。我们研究了一组未经选择的常规检测自身抗体且MND模式呈阳性的患者,并试图确定这种抗体的存在与其诊断之间的相关性。

方法

使用一种商业ELISA试验,该试验使用Sp100蛋白的重组26 kD截短序列,对应于一个免疫显性分子区域,来评估110例显示抗MND免疫荧光模式的患者中这些自身抗体的临床相关性。

结果

110例患者通过IIF检测MND呈阳性。其中,100例通过ELISA检测Sp100呈阳性。在Sp100阳性组中,34例诊断为PBC(30例确诊,4例疑似),而15例患者患有非PBC肝病。出乎意料的是,13例MND/Sp100阳性模式对应于系统性红斑狼疮(SLE)患者,5例对应于胶原病。与先前报道的另一个差异是,34例阳性患者表现出非常异质的临床症状,不同于肝病或胶原病。

结论

抗Sp100抗体可在多种临床情况下发现。检测MND/Sp100阳性对PBC的诊断有用,但仅在有正确临床背景时。一线SLE不能排除其他疾病。

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