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非裔美国系统性红斑狼疮患者中FcγRIIIA - 158F等位基因的频率。

Frequency of the Fc gamma RIIIA-158F allele in African American patients with systemic lupus erythematosus.

作者信息

Oh M, Petri M A, Kim N A, Sullivan K E

机构信息

Department of Pediatrics, Children's Hospital of Philadelphia, University of Pennsylvania School of Medicine 19104, USA.

出版信息

J Rheumatol. 1999 Jul;26(7):1486-9.

Abstract

OBJECTIVE

Defects in genes involved in immune complex clearance constitute one of the most common gene defects identified in patients with systemic lupus erythematosus (SLE). Defects in early complement components, complement receptors, and Fc receptors have all been implicated in the susceptibility to SLE. Recently, the role of functionally relevant Fc receptor polymorphisms in the etiology of SLE has been investigated. Specifically, a polymorphism of FC gamma RIII, termed Fc gamma RIIIA-158F, has been found to be associated with SLE in 2 largely Caucasian populations and appeared to constitute a risk factor for nephritis. We investigated the association of the Fc gamma RIIIA-158F and Fc gamma RIIIA-131R polymorphisms with SLE in an African American study population.

METHODS

Nested polymerase chain reaction (PCR) and allele-specific PCR was used to genotype patients with SLE and controls.

RESULTS

There was no difference in Fc gamma RIIIA-158F or Fc gamma RIIA-131R gene frequencies in the SLE populations compared to controls. There was no significant association between Fc gamma RIIIA-158F or Fc gamma RIIA-131R and any specific clinical or laboratory variable.

CONCLUSION

In our African American study population, there did not appear to be any association of Fc gamma RIIA-158F or Fc gamma RIIA-131R with SLE.

摘要

目的

免疫复合物清除相关基因缺陷是系统性红斑狼疮(SLE)患者中最常见的基因缺陷之一。早期补体成分、补体受体及Fc受体缺陷均与SLE易感性有关。最近,功能性相关Fc受体多态性在SLE病因学中的作用已得到研究。具体而言,在两个主要为白种人的群体中发现一种名为FcγRIIIA-158F的FcγRIII多态性与SLE相关,且似乎是肾炎的一个危险因素。我们在一个非裔美国人研究群体中调查了FcγRIIIA-158F和FcγRIIIA-131R多态性与SLE的关联。

方法

采用巢式聚合酶链反应(PCR)和等位基因特异性PCR对SLE患者及对照进行基因分型。

结果

与对照组相比,SLE群体中FcγRIIIA-158F或FcγRIIIA-131R基因频率无差异。FcγRIIIA-158F或FcγRIIIA-131R与任何特定临床或实验室变量之间均无显著关联。

结论

在我们的非裔美国人研究群体中,FcγRIIIA-158F或FcγRIIIA-131R与SLE之间似乎无任何关联。

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