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人类白细胞介素-1α的基因多态性

Genetic polymorphism of human interleukin-1 alpha.

作者信息

Bailly S, di Giovine F S, Blakemore A I, Duff G W

机构信息

University of Sheffield, Department of Medicine, Royal Hallamshire Hospital, GB.

出版信息

Eur J Immunol. 1993 Jun;23(6):1240-5. doi: 10.1002/eji.1830230607.

DOI:10.1002/eji.1830230607
PMID:8099012
Abstract

Interleukin-1 alpha (IL-1 alpha) has been implicated in the pathogenesis of infectious, autoimmune and inflammatory diseases. There is, however, very little information on the cis-acting sequences involved in IL-1 alpha regulation or whether there is any variation in the structure of the gene. It is known that intron 6 of IL-1 alpha shows a 5 x 46 bp tandem repeat in the genomic sequence. We have studied this region of the gene. Amplification by polymerase chain reaction showed different sized products from different individuals, most being of higher molecular weight than the expected size of 620 bp. Sequencing demonstrated that the polymorphism was due to a variable number of repeats of the 46 bp sequence. This was confirmed by restriction fragment length analysis of genomic DNA. Altogether, 72 unrelated individuals were tested and 6 alleles ranging from 5 to 18 repeats were found, the most frequent allele (62%) containing 9 repeats. This polymorphism may be of interest in gene function, since each repeat contains three potential binding sites for transcriptional factors: an SP1 site, a viral enhancer element and a glucocorticoid-responsive element. The latter, at least, demonstrates site-specific protein binding by electromobility shift assay. The functional significance of the polymorphism and its allelic frequency in inflammatory and autoimmune diseases are currently under investigation.

摘要

白细胞介素-1α(IL-1α)与感染性、自身免疫性和炎性疾病的发病机制有关。然而,关于参与IL-1α调控的顺式作用序列或该基因结构是否存在任何变异的信息非常少。已知IL-1α的内含子6在基因组序列中显示出一个5×46bp的串联重复序列。我们对该基因的这一区域进行了研究。聚合酶链反应扩增显示不同个体产生了大小不同的产物,大多数产物的分子量高于预期的620bp大小。测序表明多态性是由于46bp序列的重复次数可变所致。这通过基因组DNA的限制性片段长度分析得到了证实。总共检测了72名无关个体,发现了6个等位基因,重复次数从5次到18次不等,最常见的等位基因(62%)包含9次重复。这种多态性可能与基因功能有关,因为每个重复序列都包含转录因子的三个潜在结合位点:一个SP1位点、一个病毒增强子元件和一个糖皮质激素反应元件。至少通过电泳迁移率变动分析证明后者存在位点特异性蛋白结合。目前正在研究这种多态性及其等位基因频率在炎性和自身免疫性疾病中的功能意义。

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