4.7 Article

Identification of aberrant innate and adaptive immunity based on changes in global gene expression in the blood of adults with autism spectrum disorder

Journal

JOURNAL OF NEUROINFLAMMATION
Volume 18, Issue 1, Pages -

Publisher

BMC
DOI: 10.1186/s12974-021-02154-7

Keywords

Gene expression; RNA-sequencing; Autism spectrum disorder; WGCNA; Gene ontology; Innate immunity; Adaptive immunity

Funding

  1. Health and Labour Science Research Grant from the Japanese Ministry of Health, Labour and Welfare
  2. Japanese Ministry of Education, Culture, Sports, Science and Technology (JSPS KAKENHI Grant) [18H02752, 18K07564, 20K16628]
  3. Grants-in-Aid for Scientific Research [20K16628, 18K07564, 18H02752] Funding Source: KAKEN

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This study identified significant gene expression changes in the blood of adults with ASD, particularly in genes related to the immune system. The replication cohort confirmed these findings, suggesting a potential link between dysregulated gene expressions and the pathogenesis of ASD.
Background Autism spectrum disorder (ASD) is characterized as a neurodevelopmental disorder, and one of the main hypotheses regarding its cause is genetic factors. A previous meta-analysis of seven microarray studies and one RNA sequencing (RNA-seq) study using the blood of children with ASD identified dysregulation of gene expressions relevant to the immune system. In this study, we explored changes in global gene expression as the phenotype of ASD in the blood of adults with ASD. Methods We recruited an RNA-seq cohort (ASD vs. control; n = 6 each) and a replication cohort (ASD vs. control; n = 19 each) and conducted RNA-seq to explore changes in global gene expression. We then subjected the significantly up- and downregulated genes to gene ontology (GO) and core analyses. Weighted gene correlation network analysis (WGCNA) was performed with all 11,617 genes detected in RNA-seq to identify the ASD-specific gene network. Results In total, 117 significantly up- and 83 significantly downregulated genes were detected in the ASD compared with the control group, respectively (p < 0.05 and q < 0.05). GO analysis revealed that the aberrant innate and adaptive immunity were more obvious in the 117 upregulated than in the 83 downregulated genes. WGCNA with core analysis revealed that one module including many immune-related genes was associated with the natural killer cell signaling pathway. In the results for the replication cohort, significant changes with same trend found in RNA-seq data were confirmed for MAFB (p = 0.046), RPSAP58 (p = 0.030), and G2MK (p = 0.004). Limitations The sample size was relatively small in both the RNA-seq and replication cohorts. This study examined the mRNA expression level, so the interaction between mRNA and protein remains unclear. The expression changes between children and adults with ASD were not compared because only adults with ASD were targeted. Conclusions The dysregulated gene expressions confirmed in the blood of adults with ASD were relevant to the dysfunction of innate and adaptive immunity. These findings may aid in understanding the pathogenesis of ASD.

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