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天疱疮患者临床表型和自身抗体谱是否始终一致?一项队列研究。

Are clinical phenotype and autoantibody profile always concordant in pemphigus? A study in a cohort of pemphigus patients.

机构信息

DISSAL, Section of Dermatology, IRCCS, Azienda Ospedaliera San Martino-IST, Via Pastore 1, Genoa 16132, Italy.

出版信息

Eur J Dermatol. 2013 Jan-Feb;23(1):40-8. doi: 10.1684/ejd.2012.1903.

DOI:10.1684/ejd.2012.1903
PMID:23400331
Abstract

BACKGROUND

The clinical phenotype of different forms of pemphigus is reportedly defined by the anti-desmoglein (Dsg) autoantibody profile. In routine practice, however, this is not always the case.

OBJECTIVES

To verify the relationship between the anti-Dsg1 and -3 autoantibody profiles and titers on the one hand and the clinical phenotype and disease activity on the other.

MATERIALS AND METHODS

we followed-up clinically and serologically 20 pemphigus patients, including 3 mucosal pemphigus (mPV), 9 mucocutaneous pemphigus (mcPV), and 8 cutaneous pemphigus (PF).

RESULTS

We found that the cutaneous and/or mucosal involvement and the autoantibody profile were only concordant in mPV patients. On the contrary, in other clinical forms this correlation was often absent.

CONCLUSIONS

  1. The discrepancy between autoantibody profile and the clinical phenotype, at least in PF patients, appears to be due to non-pathogenic anti-Dsg3 antibodies; 2) in a proportion of patients the relationship between the Dsg1 and Dsg3 ELISA titers and the disease severity was absent; 3) in some patients, the anti-Dsg1 and -3 autoantibodies were lacking at diagnosis, suggesting a role of other antigens in the pathogenesis of the disease and, lastly, 4) the pure cutaneous and mucosal forms tend to respond more efficiently to the therapy than the mucocutaneous forms and have a persistent response.
摘要

背景

不同类型天疱疮的临床表型据报道由抗桥粒芯糖蛋白(Dsg)自身抗体谱定义。然而,在常规实践中,情况并非总是如此。

目的

验证抗 Dsg1 和 -3 自身抗体谱和滴度与临床表型和疾病活动之间的关系。

材料和方法

我们对 20 例天疱疮患者进行了临床和血清学随访,包括 3 例黏膜天疱疮(mPV)、9 例黏膜皮肤天疱疮(mcPV)和 8 例皮肤天疱疮(PF)。

结果

我们发现,皮肤和/或黏膜受累与自身抗体谱仅在 mPV 患者中一致。相反,在其他临床形式中,这种相关性常常不存在。

结论

1)自身抗体谱与临床表型之间的差异,至少在 PF 患者中,似乎是由于非致病性抗 Dsg3 抗体引起的;2)在一部分患者中,Dsg1 和 Dsg3 ELISA 滴度与疾病严重程度之间没有关系;3)在一些患者中,在诊断时缺乏抗 Dsg1 和 -3 自身抗体,提示其他抗原在疾病发病机制中的作用,最后,4)单纯的皮肤和黏膜形式比黏膜皮肤形式更有效地响应治疗,并且具有持续的反应。

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