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Oct 28, 2022;10 (11):

MicroRNA Profiling Shows a Time-Dependent Regulation within the First 2 Months Post-Birth and after Mild Neonatal Hypoxia in the Hippocampus from Mice.

Aisling Leavy, Gary P Brennan, Eva M Jimenez-Mateos
Author Information
  1. Aisling Leavy: Discipline of Physiology, School of Medicine, Trinity College Dublin, The University of Dublin, D02 R590 Dublin, Ireland. ORCID
  2. Gary P Brennan: Conway Institute, School of Biomolecular and Biomedical Science, University College Dublin, Belfield, D04 C7X2 Dublin, Ireland. ORCID
  3. Eva M Jimenez-Mateos: Discipline of Physiology, School of Medicine, Trinity College Dublin, The University of Dublin, D02 R590 Dublin, Ireland.
PMID: 36359259 DOI: 10.3390/biomedicines10112740

Abstract

Brain development occurs until adulthood, with time-sensitive processes happening during embryo development, childhood, and puberty. During early life and childhood, dynamic changes in the brain are critical for physiological brain maturation, and these changes are tightly regulated by the expression of specific regulatory genetic elements. Early life insults, such as hypoxia, can alter the course of brain maturation, resulting in lifelong neurodevelopmental conditions. MicroRNAs are small non-coding RNAs, which regulate and coordinate gene expression. It is estimated that one single microRNA can regulate the expression of hundreds of protein-coding genes.. Uncovering the miRNome and microRNA-regulated transcriptomes may help to understand the patterns of genes regulating brain maturation, and their contribution to neurodevelopmental pathologies following hypoxia at Postnatal day 7. Here, using a PCR-based platform, we analyzed the microRNA profile postnatally in the hippocampus of control mice at postnatal day 8, 14, and 42 and after hypoxia at postnatal day 7, to elucidate the set of microRNAs which may be key for postnatal hippocampus maturation. We observed that microRNAs can be divided in four groups based on their temporal expression. Further after an early life insult, hypoxia at P7, 15 microRNAs showed a misregulation over time, including Let7a. We speculated that the transcriptional regulator c-myc is a contributor to this process. In conclusion, here, we observed that microRNAs are regulated postnatally in the hippocampus and alteration of their expression after hypoxia at birth may be regulated by the transcriptional regulator c-myc.

Keywords

hippocampus hypoxia microRNAs1

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Grants

  1. 13/SIRG/2114 (T)/Science Foundation Ireland
  2. 18/SIRG/5646/Science Foundation Ireland
Journal Article
Article has an altmetric score of 4

Word Cloud

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