线粒体功能障碍与自闭症:自闭症儿童与 mtDNA 缺失的综合遗传分析。
Mitochondrial dysfunction and autism: comprehensive genetic analyses of children with autism and mtDNA deletion.
机构信息
Institute of Genomic Medicine and Rare Disorders, Semmelweis University, Tömő Str. 25-29, Budapest, 1083, Hungary.
Department of Genetics, Cell- and Immunobiology, Semmelweis University, Nagyvárad tér 4, Budapest, 1089, Hungary.
出版信息
Behav Brain Funct. 2018 Feb 20;14(1):4. doi: 10.1186/s12993-018-0135-x.
BACKGROUND
The etiology of autism spectrum disorders (ASD) is very heterogeneous. Mitochondrial dysfunction has been described in ASD; however, primary mitochondrial disease has been genetically proven in a small subset of patients. The main goal of the present study was to investigate correlations between mitochondrial DNA (mtDNA) changes and alterations of genes associated with mtDNA maintenance or ASD.
METHODS
Sixty patients with ASD and sixty healthy individuals were screened for common mtDNA mutations. Next generation sequencing was performed on patients with major mtDNA deletions (mtdel-ASD) using two gene panels to investigate nuclear genes that are associated with ASD or are responsible for mtDNA maintenance. Cohorts of healthy controls, ASD patients without mtDNA alterations, and patients with mitochondrial disorders (non-ASD) harbouring mtDNA deletions served as comparison groups.
RESULTS
MtDNA deletions were confirmed in 16.6% (10/60) of patients with ASD (mtdel-ASD). In 90% of this mtdel-ASD children we found rare SNVs in ASD-associated genes (one of those was pathogenic). In the intergenomic panel of this cohort one likely pathogenic variant was present. In patients with mitochondrial disease in genes responsible for mtDNA maintenance pathogenic mutations and variants of uncertain significance (VUS) were detected more frequently than those found in patients from the mtdel-ASD or other comparison groups. In healthy controls and in patients without a mtDNA deletion, only VUS were detected in both panel.
CONCLUSIONS
MtDNA alterations are more common in patients with ASD than in control individuals. MtDNA deletions are not isolated genetic alterations found in ASD; they coexist either with other ASD-associated genetic risk factors or with alterations in genes responsible for intergenomic communication. These findings indicate that mitochondrial dysfunction is not rare in ASD. The occurring mtDNA deletions in ASD may be mostly a consequence of the alterations of the causative culprit genes for autism or genes responsible for mtDNA maintenance, or because of the harmful effect of environmental factors.
背景
自闭症谱系障碍(ASD)的病因非常复杂。已经有研究描述了 ASD 中的线粒体功能障碍,但只有一小部分患者的疾病被证明是由原发性线粒体疾病引起的。本研究的主要目的是调查线粒体 DNA(mtDNA)变化与与 mtDNA 维持或 ASD 相关的基因改变之间的相关性。
方法
对 60 名 ASD 患者和 60 名健康个体进行常见 mtDNA 突变筛查。对有大片段 mtDNA 缺失(mtdel-ASD)的患者进行下一代测序,使用两个基因panel 检测与 ASD 相关或负责 mtDNA 维持的核基因。健康对照组、无 mtDNA 改变的 ASD 患者和有 mtDNA 缺失的线粒体疾病(非 ASD)患者作为对照组。
结果
在 60 名 ASD 患者中,有 16.6%(10/60)的患者存在 mtDNA 缺失(mtdel-ASD)。在这 10 名 mtdel-ASD 患儿中,我们发现了 90%与 ASD 相关的基因中罕见的 SNVs(其中一个是致病性的)。在该队列的基因组间 panel 中,存在一个可能的致病性突变。在负责 mtDNA 维持的基因中有致病性突变和意义未明的变异(VUS)的线粒体疾病患者中,比在 mtdel-ASD 或其他对照组患者中更频繁地检测到这些突变。在健康对照组和无 mtDNA 缺失的患者中,两个 panel 中仅检测到 VUS。
结论
mtDNA 改变在 ASD 患者中比在对照组中更为常见。mtDNA 缺失不是 ASD 中孤立的遗传改变;它们要么与其他 ASD 相关的遗传风险因素共存,要么与负责基因组间通讯的基因改变共存。这些发现表明,线粒体功能障碍在 ASD 中并不罕见。ASD 中发生的 mtDNA 缺失可能主要是由于 ASD 的致病基因或负责 mtDNA 维持的基因的改变,或由于环境因素的有害影响。
Zotero 插件