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HLA-G 编码区多态性在自闭症谱系障碍中呈偏倚分布。

HLA-G coding region polymorphism is skewed in autistic spectrum disorders.

机构信息

Don C. Gnocchi Foundation IRCCS, Milano, Italy.

Don C. Gnocchi Foundation IRCCS, Milano, Italy.

出版信息

Brain Behav Immun. 2018 Jan;67:308-313. doi: 10.1016/j.bbi.2017.09.007. Epub 2017 Sep 18.

DOI:10.1016/j.bbi.2017.09.007
PMID:28923404
Abstract

Different isoforms of HLA-G protein are endowed with a differential ability to induce allogenic tolerance during pregnancy. As prenatal immune activation is suggested to play a role in the onset of autistic spectrum disorders (ASD), we evaluated HLA G01:01-01:06 allelic polymorphism in a cohort of Italian children affected by ASD (N=111) their mothers (N=81), and their healthy siblings (N=39). DNA sequencing analysis of HLA-G exon 2, 3 and 4 was used to obtain HLA-G allelic frequencies; alleles distribution was compared with that of two control groups of Caucasoid couples of multiparous women and their partners from Brazil and Denmark. HLA-G distribution was significantly different in ASD children compared to both control groups (Brazilian p=1×10; Danish p=1×10). Since HLA-G distribution was similar in the two control groups, their data were pooled. Results indicated that HLA-G01:01 was significantly less frequent (p=1×10; OR:0.5, 95%CI: 0.3-0.7) whereas HLA-G01:05N was significantly more frequent (p=2×10; OR:7.3, 95%CI: 2.4-26.6) in ASD children compared to combined controls. Finally, no clear pattern emerged when HLA-G allelic distribution was analyzed in healthy sibs. Notably, HLA-G allelic distribution found in ASD mothers was similar to that observed in the control subgroup of women with recurrent miscarriages, whilst it was significantly different compared to women without miscarriages (p=6×10 df=12). Since HLA-G01:01 is associated with the elicitation of KIR-mediated tolerogenic responses and HLA-G01:05N correlates with NK cells activation, results herein indicate that an immune activating milieu during pregnancy is more likely observed in association with the development of ASD, similarly to what occurs in women with recurrent miscarriages.

摘要

不同的 HLA-G 蛋白异构体在怀孕期间具有诱导同种异体耐受的不同能力。由于产前免疫激活被认为在自闭症谱系障碍(ASD)的发病中起作用,我们评估了意大利 ASD 患儿(n=111)及其母亲(n=81)和健康兄弟姐妹(n=39)队列中 HLA-G01:01-01:06 等位基因多态性。使用 HLA-G 外显子 2、3 和 4 的 DNA 测序分析来获得 HLA-G 等位基因频率;比较等位基因分布与来自巴西和丹麦的白种人多产妇女及其伴侣的两个对照组。与两个对照组相比,ASD 患儿的 HLA-G 分布明显不同(巴西 p=1×10;丹麦 p=1×10)。由于两个对照组的 HLA-G 分布相似,因此将他们的数据合并。结果表明,与合并对照组相比,HLA-G01:01 明显较少(p=1×10;OR:0.5,95%CI:0.3-0.7),而 HLA-G01:05N 明显较多(p=2×10;OR:7.3,95%CI:2.4-26.6)。最后,在健康同胞中分析 HLA-G 等位基因分布时,没有出现明显的模式。值得注意的是,ASD 母亲的 HLA-G 等位基因分布与复发性流产妇女的对照组亚组观察到的分布相似,而与无流产的妇女明显不同(p=6×10 df=12)。由于 HLA-G01:01 与 KIR 介导的耐受反应的诱导有关,而 HLA-G01:05N 与 NK 细胞的激活相关,因此结果表明,在 ASD 发生过程中,妊娠期间更可能出现免疫激活环境,与复发性流产妇女的情况类似。

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