ICOS gene polymorphisms in systemic lupus erythematosus: A case–control study

IF 2.3 4区 医学 Q3 GENETICS & HEREDITY
Hana Houssaini, Emna Bouallegui, Olfa Abida, Safa Tahri, Nesrine Elloumi, Hend Hachicha, Sameh Marzouk, Zouhir Bahloul, Hatem Masmoudi, Raouia Fakhfakh
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引用次数: 0

Abstract

The inducible T-cell costimulator (ICOS) may play an important role in adaptive immunity by regulating the interaction between T cells and antigen-presenting cells. Disruption of this molecule can lead to autoimmune diseases, in particular systemic lupus erythematosus (SLE). In this study, we aimed to explore the possible association between ICOS gene polymorphisms and SLE as well as their influence on disease susceptibility and clinical outcomes. A further objective was to assess the potential impact of these polymorphisms on RNA expression. A case–control study, including 151 patients with SLE, and 291 unrelated healthy controls (HC) matched in gender, and geographical origin, was performed to genotype two polymorphisms located in the ICOS gene: rs11889031 (−693 G/A) and rs10932029 (IVS1 + 173 T/C); using the polymerase chain reaction (PCR)-restriction fragment length polymorphism method. The different genotypes were validated by direct sequencing. The expression level of ICOS mRNA was assessed by quantitative PCR in peripheral blood mononuclear cells of SLE patients and HC. The results were analysed using Shesis and spss.20. Our results revealed a significant association between ICOS gene rs11889031 > CC genotype and SLE disease (codominant genetic model 1, (C/C vs. C/T), p = .001, odds ratio [OR] = 2.18 IC [1.36–3.49]); codominant genetic model 2, (C/C vs. T/T) p = .007, OR = 15.29 IC [1.97–118.5]); dominant genetic model, (C/C vs. C/T + T/T) p = .0001, OR = 2.44 IC [1.53–3.9]). Besides, there was a marginal association between rs11889031 > TT genotype and T allele with a protective role from SLE (recessive genetic model, p = .016, OR = 0.08 IC [0.01–0.63] and p = 7.6904E − 05, OR = 0.43 IC = [0.28–0.66], respectively). Moreover, statistical analysis indicated that the rs11889031 > CC genotype was linked with clinical and serological manifestations of SLE, including blood pressure, and anti-SSA antibodies production in SLE patients. However, the ICOS gene rs10932029 polymorphism was not associated with susceptibility to SLE. On the other side, we did not note any effect of the two selected polymorphisms on the level of ICOS mRNA gene expression. The study showed a significant predisposing association of the ICOS rs11889031 > CC genotype with SLE, in contrast to a protective effect of rs11889031 > TT genotype in Tunisian patients. Our results suggest that ICOS rs11889031 may act as a risk factor for SLE and could be used as a genetic susceptibility biomarker.

系统性红斑狼疮ICOS基因多态性的病例对照研究。
诱导型T细胞共刺激因子(ICOS)可能通过调节T细胞和抗原呈递细胞之间的相互作用在适应性免疫中发挥重要作用。这种分子的破坏会导致自身免疫性疾病,特别是系统性红斑狼疮(SLE)。在本研究中,我们旨在探讨ICOS基因多态性与SLE之间的可能联系,以及它们对疾病易感性和临床结果的影响。另一个目的是评估这些多态性对RNA表达的潜在影响。一项病例对照研究,包括151名SLE患者和291名在性别和地理来源上匹配的无关健康对照(HC),对ICOS基因中的两个多态性进行基因分型:rs11889031(-693 G/A)和rs10932029(IVS1+173 T/C);采用聚合酶链式反应(PCR)-限制性片段长度多态性方法。通过直接测序验证了不同的基因型。定量PCR检测SLE患者和HC外周血单个核细胞ICOS mRNA的表达水平。使用Shesis和sps.20对结果进行分析。我们的研究结果显示,ICOS基因rs11889031>CC基因型与SLE疾病之间存在显著相关性(共显性遗传模型1,(C/C vs.C/T),p=0.001,比值比[OR]=2.18IC[1.36-3.49]);共显性遗传模型2,(C/C与T/T)p=.007,OR=15.29 IC[1.97-118.5]);此外,rs11889031>TT基因型和T等位基因对SLE的保护作用之间存在边际关联(隐性遗传模型,分别为p=0.016,OR=0.08IC[0.01-0.63]和p=7.6904E-05,OR=0.43IC=[0.28-0.66])。此外,统计分析表明,rs11889031>CC基因型与SLE患者的临床和血清学表现有关,包括血压和抗SSA抗体的产生。ICOS基因rs10932029多态性与SLE易感性无关。另一方面,我们没有注意到两种选择的多态性对ICOS mRNA基因表达水平的任何影响。研究显示ICOS rs11889031>CC基因型与SLE有显著的易感性关联,而突尼斯患者的rs11889031/TT基因型具有保护作用。我们的研究结果表明,ICOS rs11889031可能是SLE的危险因素,并可作为遗传易感性的生物标志物。
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来源期刊
CiteScore
4.70
自引率
0.00%
发文量
48
审稿时长
6-12 weeks
期刊介绍: The International Journal of Immunogenetics (formerly European Journal of Immunogenetics) publishes original contributions on the genetic control of components of the immune system and their interactions in both humans and experimental animals. The term ''genetic'' is taken in its broadest sense to include studies at the evolutionary, molecular, chromosomal functional and population levels in both health and disease. Examples are: -studies of blood groups and other surface antigens- cell interactions and immune response- receptors, antibodies, complement components and cytokines- polymorphism- evolution of the organisation, control and function of immune system components- anthropology and disease associations- the genetics of immune-related disease: allergy, autoimmunity, immunodeficiency and other immune pathologies- All papers are seen by at least two independent referees and only papers of the highest quality are accepted.
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