4.5 Article

Differential regulation of hippocampal transcriptome by circulating estrogen

期刊

FUNCTIONAL & INTEGRATIVE GENOMICS
卷 23, 期 4, 页码 -

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SPRINGER HEIDELBERG
DOI: 10.1007/s10142-023-01234-6

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Estrogen; Spines; Hippocampus; Estrous cycle

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This study examined the effect of estrogen (E2) on gene expression in the hippocampus of female rats by using RNA-seq technology. The results showed differential expression of 238 genes between the proestrus and diestrus stages, indicating that E2 levels may regulate the transcription process of these genes. Functional analysis revealed that genes involved in neuroactive ligand-receptor interaction, antigen processing, cell adhesion molecules, and presentation were upregulated during the proestrus stage, while genes related to bile secretion, coagulation cascades, osteoclast differentiation, cysteine and methionine metabolism were upregulated during the diestrus stage.
Estrogen (E2) modulates the synaptic structure and plasticity in the hippocampus. Previous studies showed that E2 fluctuations during various phases of the menstrual cycle produce subtle neurosynaptic changes that impact women's behavior, emotion, and cognitive functions. In this study, we explored the transcriptome of the hippocampus via RNA-seq (RNA-sequencing) between proestrus (PE) and diestrus (DE) stages in young female rats to determine the effect of E2 of PE and DE stages on hippocampal gene expression. We identified 238 genes (at 1.5-fold-change selection criteria, FDR adjusted p-value < 0.05) as differentially expressed genes (DEGs) that responded to E2 between PE and DE stages. Functional analysis based on Gene Ontology (GO) revealed that a higher E2 level corresponded to an increase in gene transcription among most of the DEGs, suggesting biological mechanisms operating differentially in the hippocampus of female rats between PE and DE stages in the estrus cycle; while analysis with Kyoto Encyclopedia of Genes and Genomes database (KEGG) found that the DEGs involving neuroactive ligand-receptor interaction, antigen processing, cell adhesion molecules, and presentation were upregulated in PE stage, whereas DEGs in pathways relating to bile secretion, coagulation cascades, osteoclast differentiation, cysteine and methionine metabolism were upregulated in DE stage of the estrus cycle. The high-fold expression of DEGs was confirmed by a follow-up quantitative real-time PCR. Our findings in this current study have provided fundamental information for further dissection of neuro-molecular mechanisms in the hippocampus in response to E2 fluctuation and its relationship with disorders.

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