Torres Anthony R, Sweeten Thayne L, Johnson Randall C, Odell Dennis, Westover Jonna B, Bray-Ward Patricia, Ward David C, Davies Christopher J, Thomas Aaron J, Croen Lisa A, Benson Michael
Center for Persons with Disabilities, Utah State University Logan, UT, USA.
Biology Department, Utah State University Brigham City, UT, USA.
Front Neurosci. 2016 Oct 20;10:463. doi: 10.3389/fnins.2016.00463. eCollection 2016.
The "common variant-common disease" hypothesis was proposed to explain diseases with strong inheritance. This model suggests that a genetic disease is the result of the combination of several common genetic variants. Common genetic variants are described as a 5% frequency differential between diseased vs. matched control populations. This theory was recently supported by an epidemiology paper stating that about 50% of genetic risk for autism resides in common variants. However, rare variants, rather than common variants, have been found in numerous genome wide genetic studies and many have concluded that the "common variant-common disease" hypothesis is incorrect. One interpretation is that rare variants are major contributors to genetic diseases and autism involves the interaction of many rare variants, especially in the brain. It is obvious there is much yet to be learned about autism genetics. Evidence has been mounting over the years indicating immune involvement in autism, particularly the HLA genes on chromosome 6 and KIR genes on chromosome 19. These two large multigene complexes have important immune functions and have been shown to interact to eliminate unwanted virally infected and malignant cells. HLA proteins have important functions in antigen presentation in adaptive immunity and specific epitopes on HLA class I proteins act as cognate ligands for KIR receptors in innate immunity. Data suggests that HLA alleles and KIR activating genes/haplotypes are common variants in different autism populations. For example, class I allele (HLA-A2 and HLA-G 14 bp-indel) frequencies are significantly increased by more than 5% over control populations (). The HLA-DR4 Class II and shared epitope frequencies are significantly above the control populations (). Three activating KIR genes: 3DS1, 2DS1, and 2DS2 have increased frequencies of 15, 22, and 14% in autism populations, respectively. There is a 6% increase in total activating KIR genes in autism over control subjects. And, more importantly there is a 12% increase in activating KIR genes and their cognate HLA alleles over control populations (Torres et al., 2012a). These data suggest the interaction of HLA ligand/KIR receptor pairs encoded on two different chromosomes is more significant as a ligand/receptor complex than separately in autism.
“常见变异-常见疾病”假说是为解释具有强遗传性的疾病而提出的。该模型表明,一种遗传性疾病是几种常见基因变异共同作用的结果。常见基因变异的定义是患病群体与匹配的对照群体之间存在5%的频率差异。最近一篇流行病学论文支持了这一理论,该论文指出,约50%的自闭症遗传风险存在于常见变异中。然而,在众多全基因组遗传研究中发现的是罕见变异而非常见变异,许多研究得出结论,“常见变异-常见疾病”假说是错误的。一种解释是,罕见变异是遗传疾病的主要成因,自闭症涉及许多罕见变异的相互作用,尤其是在大脑中。显然,关于自闭症遗传学仍有许多有待了解之处。多年来,越来越多的证据表明免疫因素与自闭症有关,特别是6号染色体上的HLA基因和19号染色体上的KIR基因。这两个大型多基因复合体具有重要的免疫功能,并且已显示它们相互作用以清除不需要的病毒感染细胞和恶性细胞。HLA蛋白在适应性免疫的抗原呈递中具有重要功能,HLA I类蛋白上的特定表位作为天然免疫中KIR受体的同源配体。数据表明,HLA等位基因和KIR激活基因/单倍型在不同自闭症群体中是常见变异。例如,I类等位基因(HLA-A2和HLA-G 14 bp插入/缺失)的频率比对照群体显著增加超过5%()。HLA-DR4 II类和共享表位频率显著高于对照群体()。三个激活KIR基因:3DS1、2DS1和2DS2在自闭症群体中的频率分别增加了15%、22%和14%。自闭症群体中激活KIR基因的总数比对照受试者增加了6%。更重要的是,与对照群体相比,激活KIR基因及其同源HLA等位基因增加了12%(Torres等人,2012a)。这些数据表明,在自闭症中,由两条不同染色体编码的HLA配体/KIR受体对作为配体/受体复合物的相互作用比单独作用更为显著。
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