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HLA-G(∗)14bp 插入/缺失多态性与自闭症谱系障碍的发展有关。

An HLA-G(∗)14bp insertion/deletion polymorphism associates with the development of autistic spectrum disorders.

机构信息

Don C. Gnocchi Foundation IRCCS, Milan, Italy.

Don C. Gnocchi Foundation IRCCS, Milan, Italy.

出版信息

Brain Behav Immun. 2015 Feb;44:207-12. doi: 10.1016/j.bbi.2014.10.002. Epub 2014 Oct 18.

DOI:10.1016/j.bbi.2014.10.002
PMID:25451607
Abstract

HLA-G expressed by the trophoblast ligates KIR molecules expressed by maternal NK cells at the uterine fetal/maternal interface: this interaction is involved in generating immune tolerance during pregnancy. A 14-bp insertion in the HLA-G 3'-UTR associates with significantly reduced levels of both HLA-G mRNA and soluble HLA-G, thus hampering the efficacy of HLA-G-mediated immune tolerance during pregnancy. Because prenatal immune activation is suggested to play an important role in the onset of autistic spectrum disorders (ASD) we performed an in-depth evaluation of HLA-G polymorphisms in a well-characterized cohort of Italian families of ASD children. Results showed that frequency of both homozygous 14bp+/14bp+ genotype and 14bp+ allele was significantly higher in ASD children and their mothers compared to controls (p<0.05 in all cases); analysis of the frequency of transmission of the 14bp+ allele from parents to ASD children and their non-ASD siblings showed that the 14bp+ allele was more frequently transmitted (T) to ASD children, whereas it was preferentially not transmitted (NT) to the non-ASD siblings (overall discrepancy: p=0.02; OR: 2.6, 95% CI: 1.1-6.4). Results herein suggest that HLA-G polymorphisms are associated with ASD development, possibly as a consequence of prenatal immune activation. These data infer that the immune alterations seen in ASD are associated with the maternal-fetal interaction alone, and reinforce the observation that different genetic backgrounds characterize ASD children and their non-ASD siblings.

摘要

滋养层细胞表达的 HLA-G 与母体 NK 细胞表达的 KIR 分子在子宫胎儿/母体界面结合:这种相互作用参与了怀孕期间的免疫耐受的产生。HLA-G 3'UTR 中的 14 个碱基插入与 HLA-G mRNA 和可溶性 HLA-G 的水平显著降低相关,从而阻碍了 HLA-G 介导的怀孕期间免疫耐受的效果。因为产前免疫激活被认为在自闭症谱系障碍(ASD)的发病中起重要作用,我们在一组意大利 ASD 儿童的特征明确的家族中对 HLA-G 多态性进行了深入评估。结果表明,在 ASD 儿童及其母亲中,纯合子 14bp+/14bp+基因型和 14bp+等位基因的频率明显高于对照组(所有情况下均为 p<0.05);对来自父母的 14bp+等位基因向 ASD 儿童及其非 ASD 兄弟姐妹的传递频率进行分析表明,14bp+等位基因更频繁地传递(T)给 ASD 儿童,而优先不传递(NT)给非 ASD 兄弟姐妹(总体差异:p=0.02;OR:2.6,95%CI:1.1-6.4)。本研究结果表明,HLA-G 多态性与 ASD 的发展相关,可能是产前免疫激活的结果。这些数据推断,ASD 中观察到的免疫改变仅与母婴相互作用有关,并进一步证实了不同的遗传背景特征描述了 ASD 儿童及其非 ASD 兄弟姐妹的观点。

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