Roberts Amy L, Thomas Ellen Ra, Bhosle Shriram, Game Laurence, Obraztsova Olga, Aitman Timothy J, Vyse Timothy J, Rhodes Benjamin
Arthritis Res Ther. 2014 May 21;16(3):R114. doi: 10.1186/ar4566.
The majority of the genetic variance of systemic lupus erythematosus (SLE) remains unexplained by the common disease-common variant hypothesis. Rare variants, which are not detectable by genome-wide association studies because of their low frequencies, are predicted to explain part of this "missing heritability." However, recent studies identifying rare variants within known disease-susceptibility loci have failed to show genetic associations because of their extremely low frequencies, leading to the questioning of the contribution of rare variants to disease susceptibility. A common (minor allele frequency = 17.4% in cases) nonsynonymous coding variant rs1143679 (R77H) in ITGAM (CD11b), which forms half of the heterodimeric integrin receptor, complement receptor 3 (CR3), is robustly associated with SLE and has been shown to impair CR3-mediated phagocytosis.
We resequenced ITGAM in 73 SLE cases and identified two previously unidentified, case-specific nonsynonymous variants, F941V and G1145S. Both variants were genotyped in 2,107 and 949 additional SLE cases, respectively, to estimate their frequencies in a disease population. An in vitro model was used to assess the impact of F941V and G1145S, together with two nonsynonymous ITGAM polymorphisms, A858V (rs1143683) and M441T (rs11861251), on CR3-mediated phagocytosis. A paired two-tailed t test was used to compare the phagocytic capabilities of each variant with that of wild-type CR3.
Both rare variants, F941V and G1145S, significantly impair CR3-mediated phagocytosis in an in vitro model (61% reduction, P = 0.006; 26% reduction, P = 0.0232). However, neither of the common variants, M441T and A858V, had an effect on phagocytosis. Neither rare variant was observed again in the genotyping of additional SLE cases, suggesting that their frequencies are extremely low.
Our results add further evidence to the functional importance of ITGAM in SLE pathogenesis through impaired phagocytosis. Additionally, this study provides a new example of the identification of rare variants in common-allele-associated loci, which, because of their extremely low frequencies, are not statistically associated. However, the demonstration of their functional effects adds support to their contribution to disease risk, and questions the current notion of dismissing the contribution of very rare variants on purely statistical analyses.
系统性红斑狼疮(SLE)的大部分遗传变异仍无法用常见疾病-常见变异假说解释。罕见变异因频率较低而无法通过全基因组关联研究检测到,预计可解释部分这种“缺失的遗传力”。然而,最近在已知疾病易感基因座内鉴定罕见变异的研究未能显示出遗传关联,因为其频率极低,这引发了对罕见变异对疾病易感性贡献的质疑。整合素α-M(ITGAM,CD11b)中的一个常见(病例中的次要等位基因频率 = 17.4%)非同义编码变异rs1143679(R77H),它构成异二聚体整合素受体补体受体3(CR3)的一半,与SLE密切相关,并且已被证明会损害CR3介导的吞噬作用。
我们对73例SLE患者的ITGAM进行了重测序,鉴定出两个先前未识别的、病例特异性的非同义变异,F941V和G1145S。分别在另外2107例和949例SLE患者中对这两个变异进行基因分型,以估计它们在疾病群体中的频率。使用体外模型评估F941V和G1145S以及两个非同义ITGAM多态性A858V(rs1143683)和M441T(rs11861251)对CR3介导的吞噬作用的影响。使用配对双尾t检验比较每个变异与野生型CR3的吞噬能力。
在体外模型中,两个罕见变异F941V和G1145S均显著损害CR3介导的吞噬作用(分别降低61%,P = 0.006;降低26%,P = 0.0232)。然而,常见变异M441T和A858V对吞噬作用均无影响。在另外的SLE患者基因分型中未再次观察到这两个罕见变异,表明它们的频率极低。
我们的结果进一步证明了ITGAM通过受损的吞噬作用在SLE发病机制中的功能重要性。此外,本研究提供了一个在常见等位基因相关基因座中鉴定罕见变异的新例子,这些变异由于频率极低,在统计学上无关联。然而,它们功能效应的证明支持了它们对疾病风险的贡献,并对当前仅基于统计分析而忽视非常罕见变异贡献的观念提出了质疑。
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