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CARD15 polymorphisms in Behcet's disease.

机译:贝塞特病中的CARD15多态性。

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BACKGROUND: Behcet's disease (BD) is a chronic multi-system inflammatory disorder of unknown aetiology, which shares many features of the inflammatory bowel diseases (IBDs). CARD15 has recently been identified as the first susceptibility gene in Crohn's disease (CD). Objective: Given certain clinical and pathological similarities between CD and BD, and recent evidence of linkage of BD to the CARD15 genomic region, the aim of this study was to investigate the role of CARD15 variants in determining susceptibility to BD. Methods: We studied 374 BD patients from three ethnically homogeneous cohorts (white English, Turkish, and Middle Eastern Arabs of Palestinian and Jordanian descent). Mutation detection of CARD15 was performed by direct sequencing in a subset of patients from each group and the identified variants were genotyped in the complete cohorts. Case-control analyses were carried out with additional stratification by the BD-associated allele, HLA-B*51. Results: Mutation detection identified six previously described CARD15 polymorphisms at a frequency of > 3%. Additionally, two of the three CD-associated polymorphisms were present, but at low frequency. The frequency of haplotypes, constructed from nine genotyped polymorphisms, demonstrated significant variation between different ethnic groups. However, case-control analyses demonstrated no association between the CARD15 polymorphisms and susceptibility to BD, irrespective of HLA-B*51 status. Conclusion: CARD15 variant alleles are not associated with susceptibility to BD. Other shared loci, currently under investigation, may determine susceptibility to both CD and BD.
机译:背景:白塞病(BD)是一种病因不明的慢性多系统炎性疾病,与炎症性肠病(IBD)具有许多共同特征。 CARD15最近被确定为克罗恩病(CD)中的第一个易感基因。目的:考虑到CD和BD之间的某些临床和病理相似性,以及最近BD与CARD15基因组区域相关的证据,本研究的目的是研究CARD15变异体在确定BD易感性中的作用。方法:我们研究了来自三个种族同质队列(白人白人,土耳其裔和中东阿拉伯裔的巴勒斯坦人和约旦人)的374名BD患者。通过对每组患者的亚组进行直接测序,对CARD15进行突变检测,并在整个队列中对鉴定出的变体进行基因分型。通过与BD相关的等位基因HLA-B * 51进行分层分析,进行病例对照分析。结果:突变检测以> 3%的频率鉴定了六个先前描述的CARD15多态性。此外,存在三种CD相关的多态性中的两种,但频率较低。由9个基因型多态性构成的单倍型频率显示出不同种族之间的显着差异。然而,病例对照分析表明,无论HLA-B * 51的状态如何,CARD15多态性与对BD的易感性之间都没有关联。结论:CARD15变异等位基因与BD的易感性无关。当前正在调查的其他共享基因座可能会确定对CD和BD的敏感性。

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