首页> 美国卫生研究院文献>other >Distinct Transcript Isoforms of the Atypical Chemokine Receptor 1 (ACKR1) / Duffy Antigen Receptor for Chemokines (DARC) Gene Are Expressed in Lymphoblasts and Altered Isoform Levels Are Associated with Genetic Ancestry and the Duffy-Null Allele
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Distinct Transcript Isoforms of the Atypical Chemokine Receptor 1 (ACKR1) / Duffy Antigen Receptor for Chemokines (DARC) Gene Are Expressed in Lymphoblasts and Altered Isoform Levels Are Associated with Genetic Ancestry and the Duffy-Null Allele

机译:非典型趋化因子受体1(ACKR1)/达菲趋化因子抗原受体(DARC)基因的不同转录同工型在淋巴细胞中表达并且同工型水平的改变与遗传祖先和达菲空等位基因有关

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摘要

The Atypical ChemoKine Receptor 1 (ACKR1) gene, better known as Duffy Antigen Receptor for Chemokines (DARC or Duffy), is responsible for the Duffy Blood Group and plays a major role in regulating the circulating homeostatic levels of pro-inflammatory chemokines. Previous studies have shown that one common variant, the Duffy Null (Fy-) allele that is specific to African Ancestry groups, completely removes expression of the gene on erythrocytes; however, these individuals retain endothelial expression. Additional alleles are associated with a myriad of clinical outcomes related to immune responses and inflammation. In addition to allele variants, there are two distinct transcript isoforms of DARC which are expressed from separate promoters, and very little is known about the distinct transcriptional regulation or the distinct functionality of these protein isoforms. Our objective was to determine if the African specific Fy- allele alters the expression pattern of DARC isoforms and therefore could potentially result in a unique signature of the gene products, commonly referred to as antigens. Our work is the first to establish that there is expression of DARC on lymphoblasts. Our data indicates that people of African ancestry have distinct relative levels of DARC isoforms expressed in these cells. We conclude that the expression of both isoforms in combination with alternate alleles yields multiple Duffy antigens in ancestry groups, depending upon the haplotypes across the gene. Importantly, we hypothesize that DARC isoform expression patterns will translate into ancestry-specific inflammatory responses that are correlated with the axis of pro-inflammatory chemokine levels and distinct isoform-specific interactions with these chemokines. Ultimately, this work will increase knowledge of biological mechanisms underlying disparate clinical outcomes of inflammatory-related diseases among ethnic and geographic ancestry groups.
机译:非典型化学趋化因子受体1(ACKR1)基因,众所周知的趋化因子达菲抗原受体(DARC或达菲),负责达菲血型,并在调节促炎性趋化因子的循环体内稳态中起主要作用。先前的研究表明,一种常见的变体,对非洲祖先群体具有特异性的达菲空(Fy-)等位基因,完全消除了该基因在红血球上的表达。然而,这些个体保留了内皮表达。其他等位基因与无数与免疫反应和炎症相关的临床结果相关。除等位基因变体外,DARC还存在两种不同的转录亚型,分别从不同的启动子表达,而对这些蛋白亚型的独特转录调控或独特功能知之甚少。我们的目标是确定非洲特定的Fy等位基因是否会改变DARC同工型的表达模式,并因此有可能导致通常被称为抗原的基因产物的独特标记。我们的工作是第一个确定DARC在淋巴母细胞中表达的研究。我们的数据表明,非洲血统的人在这些细胞中表达的DARC亚型具有相对不同的相对水平。我们得出结论,根据同基因的单倍型,两种同种型与替代等位基因的结合在祖先组中产生多个达菲抗原。重要的是,我们假设DARC同工型表达模式将转化为祖先特异性的炎症反应,与促炎性趋化因子水平的轴相关,并且与这些趋化因子有明显的同工型特异性相互作用。最终,这项工作将增加有关种族和地理血统的炎症相关疾病不同临床结果的生物学机制的知识。

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