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CTLA-4 +49A/G and CT60 gene polymorphisms in primary Sjögren syndrome

机译:原发性干燥综合征的CTLA-4 + 49A / G和CT60基因多态性

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CTLA-4 encodes cytotoxic T lymphocyte-associated antigen-4, a cell-surface molecule providing a negative signal for T-cell activation. CTLA-4 gene polymorphisms have been widely studied in connection with genetic susceptibility to various autoimmune diseases, but studies have led to contradictory results in different populations. This case-control study sought to investigate whether CTLA-4 CT60 and/or +49A/G polymorphisms were involved in the genetic predisposition to primary Sjögren syndrome (pSS). We analysed CTLA-4 CT60 and +49A/G polymorphisms in a first cohort of 142 patients with pSS (cohort 1) and 241 controls, all of Caucasian origin. A replication study was performed on a second cohort of 139 patients with pSS (cohort 2). In cohort 1, the CTLA-4 +49A/G*A allele was found on 73% of chromosomes in patients with pSS, compared with 66% in controls (p = 0.036; odds ratio (OR) 1.41, 95% confidence interval (CI) 1.02 to 1.95). No difference in CTLA-4 CT60 allelic or genotypic distribution was observed between patients (n = 142) and controls (n = 241). In the replication cohort, the CTLA-4 +49A/G*A allele was found on 62% of chromosomes in patients with pSS, compared with 66% in controls (p = 0.30; OR 0.85, 95% CI 0.63 to 1.16). Thus, the CTLA-4 +49A/G*A allele excess among patients from cohort 1 was counterbalanced by its under-representation in cohort 2. When the results from the patients in both cohorts were pooled (n = 281), there was no difference in CTLA-4 +49A/G allelic or genotypic distribution in comparison with controls. Our results demonstrate a lack of association between CTLA-4 CT60 or +49A/G polymorphisms and pSS. Premature conclusions might have been made if a replication study had not been performed. These results illustrate the importance of case-control studies performed on a large number of patients. In fact, sampling bias may account for some contradictory results previously reported for CTLA-4 association studies in autoimmune diseases.
机译:CTLA-4编码细胞毒性T淋巴细胞相关抗原4,这是一种细胞表面分子,可为T细胞活化提供负信号。关于各种自身免疫性疾病的遗传易感性,已经广泛研究了CTLA-4基因多态性,但是研究导致了不同人群中的矛盾结果。这项病例对照研究旨在调查CTLA-4 CT60和/或+ 49A / G多态性是否与原发性Sjögren综合征(pSS)的遗传易感性有关。我们分析了142名pSS患者(队列1)和241名对照(均为白种人)的第一批患者的CTLA-4 CT60和+ 49A / G多态性。在139名pSS患者的第二个队列中进行了复制研究(队列2)。在队列1中,在患有pSS的患者中73%的染色体上发现了CTLA-4 + 49A / G * A等位基因,而在对照组中则为66%(p = 0.036;优势比(OR)1.41,95%置信区间( CI)1.02至1.95)。在患者(n = 142)和对照组(n = 241)之间未观察到CTLA-4 CT60等位基因或基因型分布的差异。在复制队列中,pSS患者中62%的染色体上发现了CTLA-4 + 49A / G * A等位基因,而对照组中这一比例为66%(p = 0.30; OR 0.85,95%CI 0.63至1.16)。因此,队列1的代表性不足抵消了队列1中患者的CTLA-4 + 49A / G * A等位基因过量。当汇总两个队列中患者的结果(n = 281)时,没有发现与对照组相比,CTLA-4 + 49A / G等位基因或基因型分布的差异。我们的结果表明,CTLA-4 CT60或+ 49A / G多态性与pSS之间缺乏关联。如果没有进行复制研究,可能会得出过早的结论。这些结果说明了对大量患者进行病例对照研究的重要性。实际上,抽样偏倚可能解释了先前针对自身免疫性疾病的CTLA-4关联研究报告的一些矛盾结果。

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