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Levels of human platelet-derived soluble CD40 ligand depend on haplotypes of CD40LG-CD40-ITGA2

机译:人血小板衍生的可溶性CD40配体的水平取决于CD40LG-CD40-ITGA2的单倍型

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摘要

Increased circulating soluble CD40 ligand (sCD40L) is commonly associated with inflammatory disorders. We aimed to investigate whether gene polymorphisms in CD40LG, CD40 and ITGA2 are associated with a propensity to secrete sCD40L; thus, we examined this issue at the level of human platelets, the principal source of sCD40L. We performed single polymorphism and haplotype analyses to test for the effect of twelve polymorphisms across the CD40LG, CD40 and ITGA2 genes in blood donors. ITGA2 presented a positive association with rs1126643, with a significant modification in sCD40L secretion (carriers of C allele, P = 0.02), unlike the investigated CD40LG and CD40 polymorphisms. One CD40LG haplotype (TGGC) showing rs975379 (C/T), rs3092952 (A/G), rs3092933 (A/G) and rs3092929 (A/C) was associated with increased sCD40L levels (1.906 μg/L (95% CI: 1.060 to 2.751); P = 0.000009). The sCD40L level was associated with the inter-chromosomal CD40LG/CD40/ITGA2 haplotype (ATC), displaying rs3092952 (A/G), rs1883832 (C/T) and rs1126643 (C/T), with increased sCD40L levels (P = 0.0135). Our results help to decipher the genetic role of CD40LG, CD40 and ITGA2 with regard to sCD40L levels found in platelet components. Given the crucial role of sCD40L, this haplotype study in a transfusion model may be helpful to further determine the role of haplotypes in inflammatory clinical settings.
机译:循环可溶性CD40配体(sCD40L)增加通常与炎症性疾病有关。我们旨在研究CD40LG,CD40和ITGA2中的基因多态性是否与分泌sCD40L的倾向有关。因此,我们在人血小板(sCD40L的主要来源)的水平上研究了这个问题。我们进行了单多态性和单倍型分析,以测试献血者中CD40LG,CD40和ITGA2基因中十二种多态性的影响。 ITGA2与rs1126643呈正相关,与sCD40L和CD40多态性不同,它的sCD40L分泌(C等位基因的携带者,P = modification0.02)有显着改变。一种显示rs975379(C / T),rs3092952(A / G),rs3092933(A / G)和rs3092929(A / C)的CD40LG单倍型(TGGC)与sCD40L水平升高(1.906μg/ L(95%CI: 1.060至2.751); P = 0.000009)。 sCD40L水平与染色体间CD40LG / CD40 / ITGA2单倍型(ATC)相关,显示rs3092952(A / G),rs1883832(C / T)和rs1126643(C / T),而sCD40L水平升高(P = 0.0135 )。我们的研究结果有助于破译CD40LG,CD40和ITGA2关于血小板成分中sCD40L水平的遗传作用。考虑到sCD40L的关键作用,该单倍型研究在输血模型中可能有助于进一步确定单倍型在炎症性临床环境中的作用。

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