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白细胞介素-1基因复合体的一种罕见等位基因组合与健康个体中高水平的白细胞介素-1β血浆浓度相关。

A rare allele combination of the interleukin-1 gene complex is associated with high interleukin-1 beta plasma levels in healthy individuals.

作者信息

Hulkkonen J, Laippala P, Hurme M

机构信息

Institute of Medical Technology, University of Tampere, Tampere, Finland.

出版信息

Eur Cytokine Netw. 2000 Jun;11(2):251-5.

PMID:10903804
Abstract

Increases in the plasma levels of the inflammatory cytokines can be detected in various infectious and inflammatory diseases, but in healthy individuals these levels are in most cases low or undetectable. There is now increasing evidence that genes of the inflammatory cytokines are polymorphic and the various alleles may differ in their capability to produce the cytokine. We have measured the plasma levels IL-1 beta of 400 healthy blood donors and correlated these to the genotype (biallelelic base exchanges at the position - 889 of the IL-1 alpha gene, and at the position - 511 of the IL-1 beta gene and the pentaallelic VNTR in the second intron of the IL-1Ra gene). The median concentration of IL-1 beta was 5.8 pg/ml (upper and lower quartiles 2.2-13.6). The polymorphisms of the IL-1 beta and IL-1 Ra genes did not have any significant influence on the IL-1 beta levels, but the IL-1 alpha 2.2 homozygotes (32/400 blood donors) had significantly elevated levels (median 7.0 pg/ml, quartiles 2.2-22.4, one-way ANOVA p < 0.008 as compared to the IL-1 alpha 1.1 homozygotes and p < 0.02 as compared to the IL-1 alpha 1.2 heterozygotes). This effect of IL-1 alpha 2.2 homozygosity was more pronounced in donors, who also were carriers of the IL-1 beta allele 2. Thus these data suggest that this allele combination has a regulatory effect on basal IL-1 beta production.

摘要

在各种感染性和炎症性疾病中均可检测到炎症细胞因子血浆水平的升高,但在健康个体中,这些水平在大多数情况下较低或无法检测到。现在越来越多的证据表明,炎症细胞因子的基因具有多态性,不同的等位基因在产生细胞因子的能力上可能存在差异。我们测量了400名健康献血者的血浆白细胞介素-1β(IL-1β)水平,并将其与基因型(IL-1α基因-889位点的双等位基因突变、IL-1β基因-511位点的双等位基因突变以及IL-1受体拮抗剂(IL-1Ra)基因第二个内含子中的五等位基因可变数目串联重复序列(VNTR))进行关联分析。IL-1β的中位浓度为5.8 pg/ml(四分位数间距为2.2 - 13.6)。IL-1β和IL-1Ra基因的多态性对IL-1β水平没有显著影响,但IL-1α 2.2纯合子(32/400名献血者)的水平显著升高(中位值7.0 pg/ml,四分位数间距为2.2 - 22.4,单因素方差分析显示,与IL-1α 1.1纯合子相比p < 0.008,与IL-1α 1.2杂合子相比p < 0.02)。IL-1α 2.2纯合性的这种效应在也是IL-1β等位基因2携带者的献血者中更为明显。因此,这些数据表明这种等位基因组合对基础IL-1β的产生具有调节作用。

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