The Free Radical Scavenger N-Tert-Butyl-α-Phenylnitrone (PBN) Administered to Immature Rats During Status Epilepticus Alters Neurogenesis and Has Variable Effects, Both Beneficial and Detrimental, on Long-Term Outcomes

The Free Radical Scavenger N-Tert-Butyl-α-Phenylnitrone (PBN) Administered to Immature Rats During Status Epilepticus Alters Neurogenesis and Has Variable Effects, Both Beneficial and Detrimental, on Long-Term Outcomes

Status epilepticus (SE), especially in immature animals, is known to produce recurrent spontaneous seizures and behavioral comorbidities later in life. The cause of these adverse long-term outcomes is unknown, but it has been hypothesized that free radicals produced by SE may play a role. We tested...

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Published in:Frontiers in cellular neuroscience Vol. 12; p. 266
Main Authors: Kubová, Hana, Folbergrová, Jaroslava, Rejchrtová, Jana, Tsenov, Grygoriy, Pařízková, Martina, Burchfiel, James, Mikulecká, Anna, Mareš, Pavel
Format: Journal Article
Language:English
Published: Switzerland Frontiers Research Foundation 28-08-2018
Frontiers Media S.A
Subjects:
adult neurogenesis
Anxiety
Cognitive ability
Convulsions & seizures
EEG
Epilepsy
epileptic comorbidities
free radical scavenger
Free radicals
Granule cells
Hippocampus
Hypotheses
juvenile rats
Laboratory animals
Lithium chloride
Long-term effects
Memory
N-tert-Butyl-a-phenylnitrone
Neurogenesis
Neuropathology
neuroprotection
Neuroscience
Physiology
Pilocarpine
Seizures
Spatial memory
Studies
United States > US
epilepsy
adult neurogenesis
epileptic comorbidities
free radical scavenger
juvenile rats
neuroprotection
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Summary:Status epilepticus (SE), especially in immature animals, is known to produce recurrent spontaneous seizures and behavioral comorbidities later in life. The cause of these adverse long-term outcomes is unknown, but it has been hypothesized that free radicals produced by SE may play a role. We tested this hypothesis by treating immature (P25) rats with the free radical scavenger N-tert-butyl-α-phenylnitrone (PBN) at the time of lithium chloride (LiCl)/pilocarpine (PILO)-induced SE. Later, long-term outcomes were assessed. Cognitive impairment (spatial memory) was tested in the Morris water maze (MWM). Emotional disturbances were assessed by the capture test (aggressiveness) and elevated plus maze's (EPM) test (anxiety). Next, the presence and severity of spontaneous seizures were assessed by continuous video/EEG monitoring for 5 days. Finally, immunochemistry, stereology and morphology were used to assess the effects of PBN on hippocampal neuropathology and neurogenesis. PBN treatment modified the long-term effects of SE in varying ways, some beneficial and some detrimental. Beneficially, PBN protected against severe anatomical damage in the hippocampus and associated spatial memory impairment. Detrimentally, PBN treated animals had more severe seizures later in life. PBN also made animals more aggressive and more anxious. Correlating with these detrimental long-term outcomes, PBN significantly modified post-natal neurogenesis. Treated animals had significantly increased numbers of mature granule cells (GCs) ectopically located in the dentate hilus (DH). These results raise the possibility that abnormal neurogenesis may significantly contribute to the development of post-SE epilepsy and behavioral comorbidities.
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Reviewed by: Roberta Monterazzo Cysneiros, Mackenzie Presbyterian University, Brazil; Luiz E. Mello, Federal University of São Paulo, Brazil
Edited by: Antonio Gambardella, Università degli Studi Magna Græcia di Catanzaro, Italy
ISSN:1662-5102
1662-5102
DOI:10.3389/fncel.2018.00266