AUTHOR=Mohammadnejad Afsaneh , Li Weilong , Lund Jesper Beltoft , Li Shuxia , Larsen Martin J. , Mengel-From Jonas , Michel Tanja Maria , Christiansen Lene , Christensen Kaare , Hjelmborg Jacob , Baumbach Jan , Tan Qihua 

TITLE=Global Gene Expression Profiling and Transcription Factor Network Analysis of Cognitive Aging in Monozygotic Twins

JOURNAL=Frontiers in Genetics

VOLUME=12

YEAR=2021

URL=https://www.frontiersin.org/journals/genetics/articles/10.3389/fgene.2021.675587

DOI=10.3389/fgene.2021.675587

ISSN=1664-8021

ABSTRACT=<p>Cognitive aging is one of the major problems worldwide, especially as people get older. This study aimed to perform global gene expression profiling of cognitive function to identify associated genes and pathways and a novel transcriptional regulatory network analysis to identify important regulons. We performed single transcript analysis on 400 monozygotic twins using an assumption-free generalized correlation coefficient (GCC), linear mixed-effect model (LME) and kinship model and identified six probes (one significant at the standard FDR &lt; 0.05 while the other results were suggestive with 0.18 ≤ FDR ≤ 0.28). We combined the GCC and linear model results to cover diverse patterns of relationships, and meaningful and novel genes like <italic>APOBEC3G, H6PD, SLC45A1, GRIN3B</italic>, and <italic>PDE4D</italic> were detected. Our exploratory study showed the downregulation of all these genes with increasing cognitive function or vice versa except the <italic>SLC45A1</italic> gene, which was upregulated with increasing cognitive function. Linear models found only <italic>H6PD</italic> and <italic>SLC45A1</italic>, the other genes were captured by GCC. Significant functional pathways (FDR &lt; 3.95e-10) such as focal adhesion, ribosome, cysteine and methionine metabolism, Huntington's disease, eukaryotic translation elongation, nervous system development, influenza infection, metabolism of RNA, and cell cycle were identified. A total of five regulons (FDR&lt; 1.3e-4) were enriched in a transcriptional regulatory analysis in which <italic>CTCF</italic> and <italic>REST</italic> were activated and <italic>SP3, SRF</italic>, and <italic>XBP1</italic> were repressed regulons. The genome-wide transcription analysis using both assumption-free GCC and linear models identified important genes and biological pathways implicated in cognitive performance, cognitive aging, and neurological diseases. Also, the regulatory network analysis revealed significant activated and repressed regulons on cognitive function.</p>