Impact of neonatal iron deficiency on hippocampal DNA methylation and gene transcription in a porcine biomedical model of cognitive development

Kyle M Schachtschneider; Yingkai Liu; Laurie A Rund; Ole Madsen; Rodney W Johnson; Martien A M Groenen; Lawrence B Schook

doi:10.1186/s12864-016-3216-y

Impact of neonatal iron deficiency on hippocampal DNA methylation and gene transcription in a porcine biomedical model of cognitive development

BMC Genomics. 2016 Nov 3;17(1):856. doi: 10.1186/s12864-016-3216-y.

Authors

Kyle M Schachtschneider^{1

2}, Yingkai Liu^{1

3}, Laurie A Rund¹, Ole Madsen², Rodney W Johnson¹, Martien A M Groenen², Lawrence B Schook^{4

5}

Affiliations

¹ Department of Animal Sciences, University of Illinois, 1201 W Gregory Drive, Urbana, IL, 61801, USA.
² Animal Breeding and Genomics Centre, Wageningen University, P.O. Box 338, Wageningen, 6700AH, The Netherlands.
³ College of Animal Science and Technology, Sichuan Agricultural University, Wenjiang, Huimin Road #221, Chengdu, 610000, China.
⁴ Department of Animal Sciences, University of Illinois, 1201 W Gregory Drive, Urbana, IL, 61801, USA. schook@illinois.edu.
⁵ Institute for Genomic Biology, University of Illinois, 1206 W Gregory Drive, Urbana, IL, 61801, USA. schook@illinois.edu.

Abstract

Background: Iron deficiency is a common childhood micronutrient deficiency that results in altered hippocampal function and cognitive disorders. However, little is known about the mechanisms through which neonatal iron deficiency results in long lasting alterations in hippocampal gene expression and function. DNA methylation is an epigenetic mark involved in gene regulation and altered by environmental factors. In this study, hippocampal DNA methylation and gene expression were assessed via reduced representation bisulfite sequencing and RNA-seq on samples from a previous study reporting reduced hippocampal-based learning and memory in a porcine biomedical model of neonatal iron deficiency.

Results: In total 192 differentially expressed genes (DEGs) were identified between the iron deficient and control groups. GO term and pathway enrichment analysis identified DEGs associated with hypoxia, angiogenesis, increased blood brain barrier (BBB) permeability, and altered neurodevelopment and function. Of particular interest are genes previously implicated in cognitive deficits and behavioral disorders in humans and mice, including HTR2A, HTR2C, PAK3, PRSS12, and NETO1. Altered genome-wide DNA methylation was observed across 0.5 million CpG and 2.4 million non-CpG sites. In total 853 differentially methylated (DM) CpG and 99 DM non-CpG sites were identified between groups. Samples clustered by group when comparing DM non-CpG sites, suggesting high conservation of non-CpG methylation in response to neonatal environment. In total 12 DM sites were associated with 9 DEGs, including genes involved in angiogenesis, neurodevelopment, and neuronal function.

Conclusions: Neonatal iron deficiency leads to altered hippocampal DNA methylation and gene regulation involved in hypoxia, angiogenesis, increased BBB permeability, and altered neurodevelopment and function. Together, these results provide new insights into the mechanisms through which neonatal iron deficiency results in long lasting reductions in cognitive development in humans.

Keywords: Angiogenesis; DNA methylation; Gene expression; Hypoxia; Neonatal iron deficiency; Neurodevelopment; Porcine biomedical model; RNA-seq; RRBS.

MeSH terms

Animals
Animals, Newborn
Blood-Brain Barrier / metabolism
Cluster Analysis
Cognition / physiology*
CpG Islands
DNA Methylation*
Female
Gene Expression Profiling
Gene Expression Regulation*
High-Throughput Nucleotide Sequencing
Hippocampus / metabolism*
Iron / metabolism
Iron Deficiencies*
Neovascularization, Physiologic
Neurogenesis / genetics
Permeability
Phenotype
Swine
Transcription, Genetic*

Substances

Iron

Grants and funding

R01 HD069899/HD/NICHD NIH HHS/United States