Samia M. Ltaief, Wared Nour-Eldine, Nimshitha Pavathuparambil Abdul Manaph, Ti-Myen Tan, Nur Diana Anuar, Ilham Bensmail, Jilbin George, Houari B. Abdesselem, Abeer R. Al-Shammari
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We identified differential protein expression of 16 autoantibodies in ASD, which were correlated with differential gene expression of these markers in independent ASD cohorts. Meanwhile, we identified a distinct list of 33 autoantibodies associated with ASD severity; several of which were correlated with maternal age and birth weight in ASD. In addition, we found dysregulated numbers of circulating B cells and activated HLADR+ B cells in ASD, which were correlated with altered levels of several autoantibodies. Further in-depth analysis of B cell subpopulations revealed an increased frequency of activated naïve B cells in ASD, as well as an association of resting naïve B cells and transitional B cells with ASD severity. Pathway enrichment analysis revealed disrupted MAPK signaling in ASD, suggesting a potential relevance of this pathway to altered autoantibodies and B cell dysfunction in ASD. 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引用次数: 0
摘要
自闭症谱系障碍(ASD)是一种神经发育障碍,其特点是社会交往和沟通能力受损,以及出现刻板和重复行为。以往的研究已提供了 ASD 免疫系统失调的确凿证据;然而,对 ASD 患者自身抗体谱的研究却很有限。本研究旨在利用高通量的KoRectly Expressed(KREX)i-Ome蛋白芯片技术,筛查一组明确定义的ASD幼儿(100人)及其匹配对照组(60人)的血浆自身抗体。我们发现了16种自身抗体在ASD中的差异蛋白表达,这些差异蛋白表达与独立ASD队列中这些标记物的差异基因表达相关。同时,我们还发现了33种与ASD严重程度相关的自身抗体,其中有几种与ASD患者的母体年龄和出生体重相关。此外,我们还发现 ASD 中循环 B 细胞和活化的 HLADR+ B 细胞数量失调,这与几种自身抗体水平的改变有关。对B细胞亚群的进一步深入分析显示,ASD患者中活化的幼稚B细胞频率增加,静息的幼稚B细胞和过渡性B细胞也与ASD的严重程度有关。通路富集分析显示,MAPK 信号在 ASD 中被破坏,这表明该通路可能与 ASD 中自身抗体的改变和 B 细胞功能障碍有关。最后,我们发现,与ASD严重程度相关的八种自身抗体的组合显示曲线下面积(ROC-AUC)为0.937(95% CI = 0.890, 0.983; p
Dysregulated plasma autoantibodies are associated with B cell dysfunction in young Arab children with autism spectrum disorder in Qatar
Autism spectrum disorder (ASD) is a neurodevelopmental disorder characterized by impaired social interaction and communication, as well as the occurrence of stereotyped and repetitive behaviors. Previous studies have provided solid evidence of dysregulated immune system in ASD; however, limited studies have investigated autoantibody profiles in individuals with ASD. This study aims to screen plasma autoantibodies in a well-defined cohort of young children with ASD (n = 100) and their matched controls (n = 60) utilizing a high-throughput KoRectly Expressed (KREX) i-Ome protein-array technology. We identified differential protein expression of 16 autoantibodies in ASD, which were correlated with differential gene expression of these markers in independent ASD cohorts. Meanwhile, we identified a distinct list of 33 autoantibodies associated with ASD severity; several of which were correlated with maternal age and birth weight in ASD. In addition, we found dysregulated numbers of circulating B cells and activated HLADR+ B cells in ASD, which were correlated with altered levels of several autoantibodies. Further in-depth analysis of B cell subpopulations revealed an increased frequency of activated naïve B cells in ASD, as well as an association of resting naïve B cells and transitional B cells with ASD severity. Pathway enrichment analysis revealed disrupted MAPK signaling in ASD, suggesting a potential relevance of this pathway to altered autoantibodies and B cell dysfunction in ASD. Finally, we found that a combination of eight autoantibodies associated with ASD severity showed an area under the curve (ROC-AUC) of 0.937 (95% CI = 0.890, 0.983; p < 0.001), which demonstrated the diagnostic accuracy of the eight-marker signature in the severity classification of ASD cases. Overall, this study determined dysregulated autoantibody profiles and B cell dysfunction in children with ASD and identified an eight-autoantibody panel for ASD severity classification.
期刊介绍:
AUTISM RESEARCH will cover the developmental disorders known as Pervasive Developmental Disorders (or autism spectrum disorders – ASDs). The Journal focuses on basic genetic, neurobiological and psychological mechanisms and how these influence developmental processes in ASDs.
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