MICA基因三联体重复多态性和MEFV突变的基因型对家族性地中海热患者淀粉样变性及疾病进程的影响。

The contribution of genotypes at the MICA gene triplet repeat polymorphisms and MEFV mutations to amyloidosis and course of the disease in the patients with familial Mediterranean fever.

作者信息

Turkcapar Nuran, Tuncali Timur, Kutlay Sim, Burhan Basak Yalcin, Kinikli Gulay, Erturk Sehsuvar, Duman Murat

机构信息

Department of Clinical Immunology and Rheumatology, School of Medicine, Ankara University, Ankara, Turkey.

出版信息

Rheumatol Int. 2007 Apr;27(6):545-51. doi: 10.1007/s00296-006-0255-8. Epub 2006 Nov 11.

DOI:10.1007/s00296-006-0255-8

PMID:17102945

Abstract

OBJECTIVE

To evaluate the effects of MEFV genotypes and the major histocompatibility complex class I chain-related gene A (MICA) triplet repeat polymorphism on the severity and clinical features of familial Mediterranean fever (FMF) and amyloidosis in a group of Turkish FMF patients.

METHODS

We evaluated 105 adult FMF patients (with or without amyloidosis, 33 and 72, respectively) along with 107 healthy controls who were neither related to the patients nor had a family history of FMF or Behcet's disease. After recording the demographic and clinical data, the predominant mutations in the MEFV gene locus (M694V, M680I, V726A, M694I, and E148Q) were investigated by direct sequencing. MICA transmembrane polymorphisms in exon 5 were studied by vertical gel electrophoresis and fragment analysis of the amplicons obtained from MICA locus with appropriate primers.

RESULTS

Earlier age at onset, increased frequency of attacks, arthritis attacks, erysipelas-like erythema, increased severity scores and amyloidosis were significantly more common in M694V homozygous patients compared to the patients not M694V homozygous (P = 0.005, OR 4.55; P = 0.001, OR 7.60; P = 0.003, OR 4.57; P = 0.002, OR 7.58; P = 0.004, OR 5.15 and P = 0.018, OR 3.33, respectively). We did not detect any modifying effects of MICA alleles as an independently risk factor on the amyloidosis development. However, when we examined the effects of MICA alleles on the course of the disease and development of amyloidosis in the M694V homozygous patients, A5 allele had a protective effect against the development of amyloidosis (P = 0.038, OR(adj) 0.26 with A5 and P = 0.009, OR(adj) 4.42 without A5).

CONCLUSION

Though the effects of the MEFV genotypes seem clear, there are definitely other modifying factors or genes on the development of amyloidosis and on the course of the disease. For example, some MICA alleles have a protective effect on the prognostic factors in FMF.

摘要

目的

评估一组土耳其家族性地中海热（FMF）患者中MEFV基因分型和主要组织相容性复合体I类链相关基因A（MICA）三联体重复多态性对FMF严重程度及临床特征以及淀粉样变性的影响。

方法

我们评估了105例成年FMF患者（分别有33例和72例伴有或不伴有淀粉样变性）以及107名健康对照者，这些对照者与患者无亲缘关系，也无FMF或白塞病家族史。记录人口统计学和临床数据后，通过直接测序研究MEFV基因座中的主要突变（M694V、M680I、V726A、M694I和E148Q）。通过垂直凝胶电泳和用适当引物从MICA基因座获得的扩增子的片段分析，研究外显子5中的MICA跨膜多态性。

结果

与非M694V纯合子患者相比，M694V纯合子患者发病年龄更早、发作频率增加、关节炎发作、丹毒样红斑、严重程度评分增加以及淀粉样变性更为常见（P分别为0.005，OR为4.55；P为0.001，OR为7.60；P为0.003，OR为4.57；P为0.002，OR为7.58；P为0.004，OR为5.15；P为0.018，OR为3.33）。我们未检测到MICA等位基因作为淀粉样变性发展的独立危险因素的任何修饰作用。然而，当我们研究MICA等位基因对M694V纯合子患者疾病进程和淀粉样变性发展的影响时，A5等位基因对淀粉样变性的发展具有保护作用（有A5时P = 0.038，OR(adj)为0.26；无A5时P = 0.009，OR(adj)为4.42）。