首页> 外文期刊>Human Immunology: Official Journal of the American Society for Histocompatibility and Immunogenetics >HLA-G gene expression influenced at allelic level in association with end stage renal disease and acute allograft rejection
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HLA-G gene expression influenced at allelic level in association with end stage renal disease and acute allograft rejection

机译:HLA-G基因表达在等位基因水平与晚期肾脏疾病和急性同种异体移植排斥相关

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Background: Human leukocyte antigen (HLA)-G is a non-classical major-histocompatibility complex class-I molecule associated with immunosuppressive function. We have evaluated the impact of HLA-G allele associated with untranslated-region (UTR)-haplotype in end stage renal disease (ESRD) and acute allograft rejection (AR) cases. The mRNA levels of different HLA-G isoforms were evaluated in ESRD and AR cases. Subsequently, the total HLA-G mRNA levels and protein concentration were evaluated against its UTR-haplotype among ESRD and AR cases. Methodology: Sequence based typing of the promoter region was carried-out to evaluate the impact of HLA-G haplotype in 350 ESRD cases and 300 controls. HLA-G gene expression was evaluated at the transcriptional level using semi-quantitative and quantitative PCR, whereas protein concentration was determined by ELISA among both cases and control. Results: Increased risk was observed for G*. 01:01:01:03, G*. 01:01:02, G*. 01:06 and G*. 01:05:N haplotypes while G*. 01:01:01:01 and G*.01:04:01 haplotypes showed a protective effect in ESRD and AR cases. Higher level of soluble HLA-G isoforms (G5 and G6) was observed among ESRD cases. Reduced levels of soluble isoform (G5) and increased levels of membrane bound (G1 and G3) isoforms were found among AR cases, revealing risk association. Decreased HLA-G expression was observed at both mRNA and protein level for G*. 01:01:01:03 and G*. 01:05:N haplotypes in ESRD and AR cases. Conclusions: These results suggest that the variation in the expression profile of membrane bound and soluble isoforms may modulate the risk for ESRD and AR. UTR-haplotypes appear to be involved in different HLA-G expression patterns at transcriptional and translational levels.
机译:背景:人类白细胞抗原(HLA)-G是与免疫抑制功能相关的非经典主要组织相容性复合物I类分子。我们评估了与非翻译区(UTR)-单倍型相关的HLA-G等位基因在终末期肾脏疾病(ESRD)和急性同种异体移植排斥(AR)病例中的影响。在ESRD和AR患者中评估了不同HLA-G亚型的mRNA水平。随后,在ESRD和AR病例中针对其UTR-单倍型评估了总的HLA-G mRNA水平和蛋白质浓度。方法:进行基于序列的启动子区域分型,以评估HLA-G单倍型在350例ESRD病例和300例对照中的影响。使用半定量和定量PCR在转录水平评估HLA-G基因表达,而在病例和对照中均通过ELISA测定蛋白质浓度。结果:观察到G *的风险增加。 01:01:01:03,G *。 01:01:02,G *。 01:06和G *。 01:05:N单倍型,而G *。 01:01:01:01和G * .01:04:01单倍型在ESRD和AR患者中显示出保护作用。在ESRD病例中观察到较高水平的可溶性HLA-G同工型(G5和G6)。在AR病例中发现可溶性同工型(G5)水平降低和膜结合同工型(G1和G3)水平升高,表明存在风险关联。在G *的mRNA和蛋白水平均观察到HLA-G表达降低。 01:01:01:03和G *。 01:05:ESRD和AR病例中有N个单倍型。结论:这些结果表明膜结合和可溶性同工型的表达谱的变化可能调节ESRD和AR的风险。 UTR单倍型似乎在转录和翻译水平上参与了不同的HLA-G表达模式。

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