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甘露糖结合蛋白基因的一个功能失调等位基因与西班牙人群中的系统性红斑狼疮相关。

A dysfunctional allele of the mannose binding protein gene associates with systemic lupus erythematosus in a Spanish population.

作者信息

Davies E J, Teh L S, Ordi-Ros J, Snowden N, Hillarby M C, Hajeer A, Donn R, Perez-Pemen P, Vilardell-Tarres M, Ollier W E

机构信息

Rheumatic Diseases Centre, University of Manchester, UK.

出版信息

J Rheumatol. 1997 Mar;24(3):485-8.

PMID:9058653
Abstract

OBJECTIVE

To determine dysfunctional mannose binding protein (MBP) status of Spanish patients with systemic lupus erythematosus (SLE) and to determine whether MBP and complement C4 null alleles contribute in an additive way to SLE susceptibility.

METHODS

The frequencies of MBP alleles (characterized by polymorphisms at codon 54 and codon 57 of exon 1) were determined by the amplification refractory mutation system-polymerase chain reaction in 50 Spanish patients with SLE and 49 matched controls. Mutant genotypes for the codon 54 mutation were confirmed using a Ban I restriction enzyme digest method. Complement C4 allotyping was achieved by agarose gel electrophoresis of neuraminidase/carboxypeptidase B digested plasma samples followed by immunofixation and staining.

RESULTS

At least one dysfunctional MBP allele, unable to activate complement, was present in 52% of patients with SLE and in 31% of controls (OR = 2.4, 95% CI 1.1-5.6). Complement C4 null alleles (either C4A or C4B) were present in 61% of patients and 43% of controls (OR = 2.1, 95% CI 0.9-4.9). A dysfunctional MBP allele and C4 null allele were present in 41% of patients and 16% of controls (OR = 3.2, 95% CI 1.2-8.1).

CONCLUSION

The presence of a dysfunctional MBP allele is a risk factor for developing SLE in this Spanish population and may affect susceptibility in an additive way with C4 null alleles.

摘要

目的

确定西班牙系统性红斑狼疮(SLE)患者中功能失调的甘露糖结合蛋白(MBP)状态,并确定MBP和补体C4无效等位基因是否以累加方式促成SLE易感性。

方法

采用扩增阻滞突变系统-聚合酶链反应,测定50例西班牙SLE患者和49例匹配对照中MBP等位基因(由外显子1第54密码子和第57密码子的多态性表征)的频率。使用Ban I限制性内切酶消化法确认第54密码子突变的突变基因型。通过对神经氨酸酶/羧肽酶B消化的血浆样本进行琼脂糖凝胶电泳,随后进行免疫固定和染色来实现补体C4别型分析。

结果

52%的SLE患者和31%的对照中存在至少一个无法激活补体的功能失调MBP等位基因(比值比=2.4,95%可信区间1.1-5.6)。61%的患者和43%的对照中存在补体C4无效等位基因(C4A或C4B)(比值比=2.1,95%可信区间0.9-4.9)。41%的患者和16%的对照中存在功能失调的MBP等位基因和C4无效等位基因(比值比=3.2,95%可信区间1.2-8.1)。

结论

在这个西班牙人群中,功能失调的MBP等位基因的存在是发生SLE的一个危险因素,并且可能与C4无效等位基因以累加方式影响易感性。

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