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Series GSE269543 Query DataSets for GSE269543
Status Public on Jul 10, 2024
Title Multi-omics Analysis Revealing the Impact of Excessive Maternal Folate Supplementation on Offspring Brain Development [spatial transcriptome]
Organism Mus musculus
Experiment type Other
Summary Folate is crucial for diverse biological processes including neurogenesis. While folate supplementation during pregnancy is standard for preventing neural tube defects (NTDs), concerns are growing over the potential risks of excessive maternal intake. In this study, we employed spatial transcriptomics and single-nucleus multi-omics techniques to investigate the impact of increased maternal folate intake on offspring brain development. Elevated folate intake broadly affected gene pathways linked to neurogenesis and neuronal axon myelination across multiple brain regions. Furthermore, specific gene expression alterations related to learning and memory processes emerged in thalamic and ventricular regions. Single-nucleus multi-omics analysis revealed that maturing excitatory neurons in dentate gyrus are particularly vulnerable to suboptimal maternal folate intake. Aberrant gene expression and chromatin accessibility changes were primarily centered on pathways governing ribosomal biogenesis, which is critical for synaptic formation. Altogether, our findings provide novel insights into how excessive maternal folate supplementation affects offspring brain development, notably by influencing gene expression and chromatin accessibility.
 
Overall design Adult female mice (8-12 weeks old) were randomly assigned to either a control folic acid (FA) diet (2mg/kg) or an excessive FA diet (20mg/kg) for two weeks before mating with males. These diets were maintained throughout pregnancy and lactation. Pups were harvested on postnatal day 21 (P21). To profile spatial transcriptome, the mouse brains were freshly isolated to prepare FFPE tissue blocks, then coronally sectioned and placed onto the Visium slides for Visium Spatial Gene Expression library preparation. To simultaneously profile the transcriptome and chromatin accessibility at single cell resolution, hippocampus tissues were micro-dissected from the freshly isolated mouse brain tissues for single nuclei suspension preparation and subsequently loaded onto the Chromium iX using the single nucleus multiome kit from 10x genomics. Single nucleus RNA-seq (snRNA-seq) and single nucleus ATAC-seq (snATAC-seq) libraries were simultaneously constructed from the same nucleus following the manufactures' instructions.
 
Contributor(s) Xu X, Lin Y, Xie H
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Submission date Jun 11, 2024
Last update date Jul 10, 2024
Contact name Hehuang Xie
Organization name Virginia Tech
Street address Mail Stop: 0477,Biomedical Science(MC0477),Steger Hall Virginia Tech
City Blacksburg
ZIP/Postal code 24061
Country USA
 
Platforms (1)
GPL24247 Illumina NovaSeq 6000 (Mus musculus)
Samples (4)
GSM8321863 MF, coronal, rep1
GSM8321864 MF, coronal, rep2
GSM8321865 HF, coronal, rep1
Relations
BioProject PRJNA1122482

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Supplementary file Size Download File type/resource
GSE269543_RAW.tar 272.1 Mb (http)(custom) TAR (of CSV, JPG, JSON, MTX, PNG, TSV)
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Raw data are available in SRA

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