| Literature DB >> 36195640 |
Jiayuan Xu1, Xianyou Xia2, Qiaojun Li3, Yan Dou1, Xinjun Suo1, Zuhao Sun1, Nana Liu1, Yating Han2, Xiaodi Sun1, Yukun He4, Wen Qin1, Shijie Zhang4, Tobias Banaschewski5, Herta Flor6,7, Antoine Grigis8, Penny Gowland9, Andreas Heinz10, Rüdiger Brühl11, Jean-Luc Martinot12, Eric Artiges13, Frauke Nees5,6,14, Tomáš Paus15, Luise Poustka16, Sarah Hohmann5, Henrik Walter10, Pak Chung Sham17, Gunter Schumann18,19, Xudong Wu20,21, Mulin Jun Li22,23, Chunshui Yu24,25.
Abstract
Human hippocampal volume has been separately associated with single nucleotide polymorphisms (SNPs), DNA methylation and gene expression, but their causal relationships remain largely unknown. Here, we aimed at identifying the causal relationships of SNPs, DNA methylation, and gene expression that are associated with hippocampal volume by integrating cross-omics analyses with genome editing, overexpression and causality inference. Based on structural neuroimaging data and blood-derived genome, transcriptome and methylome data, we prioritized a possibly causal association across multiple molecular phenotypes: rs1053218 mutation leads to cg26741686 hypermethylation, thus leads to overactivation of the associated ANKRD37 gene expression in blood, a gene involving hypoxia, which may result in the reduction of human hippocampal volume. The possibly causal relationships from rs1053218 to cg26741686 methylation to ANKRD37 expression obtained from peripheral blood were replicated in human hippocampal tissue. To confirm causality, we performed CRISPR-based genome and epigenome-editing of rs1053218 homologous alleles and cg26741686 methylation in mouse neural stem cell differentiation models, and overexpressed ANKRD37 in mouse hippocampus. These in-vitro and in-vivo experiments confirmed that rs1053218 mutation caused cg26741686 hypermethylation and ANKRD37 overexpression, and cg26741686 hypermethylation favored ANKRD37 overexpression, and ANKRD37 overexpression reduced hippocampal volume. The pairwise relationships of rs1053218 with hippocampal volume, rs1053218 with cg26741686 methylation, cg26741686 methylation with ANKRD37 expression, and ANKRD37 expression with hippocampal volume could be replicated in an independent healthy young (n = 443) dataset and observed in elderly people (n = 194), and were more significant in patients with late-onset Alzheimer's disease (n = 76). This study revealed a novel causal molecular association mechanism of ANKRD37 with human hippocampal volume, which may facilitate the design of prevention and treatment strategies for hippocampal impairment.Entities:
Year: 2022 PMID: 36195640 DOI: 10.1038/s41380-022-01800-7
Source DB: PubMed Journal: Mol Psychiatry ISSN: 1359-4184 Impact factor: 13.437