Long-term changes in metabolic brain network drive memory impairments in rats following neonatal hypoxia-ischemia
•In vivo microPET-FDG imaging assess the neuroplasticity of neonatal HI animal model.•Preservation of brain metabolism is dissociated of cognitive deficits in HI model.•Changes in brain volume correlate positively with hypometabolism in brain regions.•Memory impairments is associated with long-term...
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Veröffentlicht in: | Neurobiology of learning and memory 2020-05, Vol.171, p.107207-107207, Article 107207 |
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Zusammenfassung: | •In vivo microPET-FDG imaging assess the neuroplasticity of neonatal HI animal model.•Preservation of brain metabolism is dissociated of cognitive deficits in HI model.•Changes in brain volume correlate positively with hypometabolism in brain regions.•Memory impairments is associated with long-term changes in MBN in neonatal HI rats.•MBN based on microPET-FDG is sensitive in revealing changes in brain functionality.
Hypoxia and cerebral ischemia (HI) events are capable of triggering important changes in brain metabolism, including glucose metabolism abnormalities, which may be related to the severity of the insult. Using positron emission microtomography (microPET) with [18F]fluorodeoxyglucose (18F-FDG), this study proposes to assess abnormalities of brain glucose metabolism in adult rats previously submitted to the neonatal HI model. We hypothesize that cerebral metabolic outcomes will be associated with cognitive deficits and magnitude of brain injury.
Seven-day-old rats were subjected to an HI model, induced by permanent occlusion of the right common carotid artery and systemic hypoxia. 18F-FDG-microPET was used to assess regional and whole brain glucose metabolism in rats at 60 postnatal days (PND 60). An interregional cross-correlation matrix was utilized to construct metabolic brain networks (MBN). Rats were also subjected to the Morris Water Maze (MWM) to evaluate spatial memory and their brains were processed for volumetric evaluation.
Brain glucose metabolism changes were observed in adult rats after neonatal HI insult, limited to the right brain hemisphere. However, not all HI animals exhibited significant cerebral hypometabolism. Hippocampal glucose metabolism was used to stratify HI animals into HI hypometabolic (HI-h) and HI non-hypometabolic (HI non-h) groups. The HI-h group had drastic MBN disturbance, cognitive deficit, and brain tissue loss, concomitantly. Conversely, HI non-h rats had normal brain glucose metabolism and brain tissue preserved, but also presented MBN changes and spatial memory impairment. Furthermore, data showed that brain glucose metabolism correlated with cognitive deficits and brain volume outcomes.
Our findings demonstrated that long-term changes in MBN drive memory impairments in adult rats subjected to neonatal hypoxic ischemia, using in vivo imaging microPET-FDG. The MBN analyses identified glucose metabolism abnormalities in HI non-h animals, which were not detected by conventional 18F-FDG standardized uptake valu |
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ISSN: | 1074-7427 1095-9564 |
DOI: | 10.1016/j.nlm.2020.107207 |