| Literature DB >> 35491813 |
Juan Song1,2, Gisela Nilsson1, Yiran Xu2, Aura Zelco1, Eridan Rocha-Ferreira3, Yafeng Wang4,5, Xiaoli Zhang2, Shan Zhang2,5, Joakim Ek1, Henrik Hagberg3, Changlian Zhu2,5, Xiaoyang Wang1,2,3.
Abstract
Germinal matrix hemorrhage (GMH) is a common complication in preterm infants and is associated with high risk of adverse neurodevelopmental outcomes. We used a rat GMH model and performed RNA sequencing to investigate the signaling pathways and biological processes following hemorrhage. GMH induced brain injury characterized by early hematoma and subsequent tissue loss. At 6 hours after GMH, gene expression indicated an increase in mitochondrial activity such as ATP metabolism and oxidative phosphorylation along with upregulation of cytoprotective pathways and heme metabolism. At 24 hours after GMH, the expression pattern suggested an increase in cell cycle progression and downregulation of neurodevelopmental-related pathways. At 72 hours after GMH, there was an increase in genes related to inflammation and an upregulation of ferroptosis. Hemoglobin components and genes related to heme metabolism and ferroptosis such as Hmox1, Alox15, and Alas2 were among the most upregulated genes. We observed dysregulation of processes involved in development, mitochondrial function, cholesterol biosynthesis, and inflammation, all of which contribute to neurodevelopmental deterioration following GMH. This study is the first temporal transcriptome profile providing a comprehensive overview of the molecular mechanisms underlying brain injury following GMH, and it provides useful guidance in the search for therapeutic interventions.Entities:
Keywords: Germinal matrix hemorrhage; RNA-sequencing; ferroptosis; mitochondria; neurodevelopment
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Year: 2022 PMID: 35491813 PMCID: PMC9441725 DOI: 10.1177/0271678X221098811
Source DB: PubMed Journal: J Cereb Blood Flow Metab ISSN: 0271-678X Impact factor: 6.960