Decrease in Oxidative Stress Parameters after Post‐Ischaemic Recombinant Human Erythropoietin Administration in the Hippocampus of Rats Exposed to Focal Cerebral Ischaemia

Mršić-Pelčić, Jasenka; Pilipović, Kristina; Pelčić, Goran; Vitezić, Dinko; Župan, Gordana

doi:10.1111/bcpt.12833

Cited by 11 publications

(7 citation statements)

References 81 publications

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“…Decreased GPx2 mRNA level in brain tissue may indicate that 1.5 h after hypoxia the level of oxidative stress is reduced by NADA. A reduced levels of ROS and a decrease in GPx activity in rat brains were observed in the recent studies of pre-treatment with metabotropic glutamate receptors agonist (Bratek et al, 2018) and recombinant human erythropoietin (Mršić-Pelčić et al, 2017). The authors suggest that the protective effects of the therapeutic agents determined by the inhibition of ROS production and reduction of oxidative stress.…”

Section: Discussionmentioning

confidence: 86%

Early‐life N‐arachidonoyl‐dopamine exposure increases antioxidant capacity of the brain tissues and reduces functional deficits after neonatal hypoxia in rats

Sukhanova

Sebentsova

Khukhareva

et al. 2019

Intl J of Devlp Neuroscience

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Perinatal hypoxia‐ischemia is one of the most common causes of perinatal brain injury and subsequent neurological disorders in children. The aim of this work was to evaluate the potential antioxidant and neuroprotective effects of N‐arachidonoyl‐dopamine (NADA) in the model of acute neonatal hypoxia (ANH) in rat pups. Male and female Wistar rats were exposed to a hypoxic condition (8% oxygen for 120 min) at postnatal day 2 (P2). Transcription factor HIF1‐α and glutathione peroxidases GPx2 and GPx4 gene expression was increased in rat brains in the hypoxic group compared to control 1.5 h but not 4 days after ANH. There were no post‐hypoxic changes in reduced (GSH) and oxidised (GSSG) glutathione levels in the brain of rat pups 1.5 h and 4 d after hypoxia. Hypoxic rats displayed retarded performance in the righting reflex and the negative geotaxis tests. ANH resulted in increased ambulation in Open field test and impaired retention in the Barnes maze task under stressful conditions as compared with the control group. Treatment with NADA significantly attenuated the delayed development of sensorimotor reflexes and stress‐evoked disruption of memory retention in hypoxic rats but had no effect on the hypoxia‐induced hyperactivity. In rats exposed to hypoxia, treatment with NADA decreased GPx2 gene expression and increased GSH/GSSG ratio in whole brains 1.5 h after ANH. These results suggest that the long‐lasting beneficial effects of NADA on hypoxia‐induced neurobehavioural deficits are mediated, at least in part, by its antioxidant properties.

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Section: Discussionmentioning

confidence: 86%

Early‐life N‐arachidonoyl‐dopamine exposure increases antioxidant capacity of the brain tissues and reduces functional deficits after neonatal hypoxia in rats

Sukhanova

Sebentsova

Khukhareva

et al. 2019

Intl J of Devlp Neuroscience

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“…Thus, it was shown that MCAO followed by 24 h of reperfusion causes significant neuronal damage in various brain regions. The predominant affected areas are mostly striatum and cortex due to the lack of collateral blood supply (2,18,19). It was described also that immunoreactivity for NeuN decrease significantly following MCAO (20), causing massive corticostriatal lesion with the peak of the damage 12-24 h following reperfusion (20,21).…”

Section: Discussionmentioning

confidence: 99%

“…However, most of the experimental research in various animal models that examined the neuroprotective effects of different doses of rhEpo on brain damage, proposed 5000 IU/kg of rhEpo as optimal dosage (32). It was also shown that rhEpo applied at various time-periods ranging from pre-treatment to up to 24 h after ischemia, exerts the best results when applied within the first 3 h after induction of ischemia (18).…”

Section: Discussionmentioning

confidence: 99%

Neuroprotective Effect of the Recombinant Human Erythropoietin in the Enthorinal Cortex and Thalamus of Rats Exposed to Focal Cerebral Ischemia

Mršić-Pelčić¹,

Maja²,

Pelčić³

et al. 2020

EJOH

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Objective: Neuroprotective potential of recombinant human erythropoietin (rhEpo) was reported in various experimental models of brain damage but the exact mechanism of its effect is still unclear. In the present study, the effect of rhEpo administration on the level of neuronal loss and neurodegenerative changes in the dorsolateral band of the entorhinal cortex and ventral posteriomedial nucleus of the thalamus in rats following focal cerebral ischemia was examined.Methods: Focal cerebral ischemia was induced in male Hanover Wistar rats (250-350 g) by right middle cerebral artery occlusion (MCAO) model for 1 h. After 23 h of reperfusion, ischemic animals were sacrificed and the neuronal damage was detected using the Fluoro Jade B fluorescent staining to detect neurodegeneration, together with NeuN immunostaining used to detect neuronal loss. Ischemic animals received either vehicle or rhEpo (5000 IU/kg, intraperitoneally) 3 hrs after MCAO, and were sacrificed 21 h later. Sham operated; vehicle treated animals served as the control group.Results: Administration of rhEpo significantly increased the NeuN immunoreactivity in the entorhinal cortex compared to the neuronal loss detected in ischemic, non-treated animals and decreased the number of Fluoro Jade B positive neurons in comparison to neuronal damage detected in ischemic, nontreated animals. The effect of rhEpo treatment in thalamus was not significant.

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“…Apparent signs of apoptosis induction were observed in the rat hippocampus one day after MCAO [24]. The death of hippocampal cells via apoptosis was confirmed by the decrease in the expression of anti apop totic protein Bcl 2, as well as by the upregulated expres BIOCHEMISTRY (Moscow) sion of the pro apoptotic protein BAX [25] and the apop tosis executing enzyme caspase 3 in the hippocampus [22,26]. The increase in the number of apoptotic cells was accompanied with pronounced changes in the expression of mRNAs for the NMDA receptor sub units [27].…”

Section: Rapid Responses Of the Hippocampus To The Ischemic Damagementioning

confidence: 91%

“…As established using microdialysis, the extracellular level of glutamate in the rat hippocampus increased within the first minutes of ischemia [21]. The first evidences of the so called delayed death of neurons in this structure were detected later than in the cortex and the striatum [22], as a rule, between 12 h and seven days after the ischemia, with the peak levels on day 4 [23]. Apparent signs of apoptosis induction were observed in the rat hippocampus one day after MCAO [24].…”

Section: Rapid Responses Of the Hippocampus To The Ischemic Damagementioning

confidence: 96%

Changes in Gene Expression and Neuroinflammation in the Hippocampus after Focal Brain Ischemia: Involvement in the Long-Term Cognitive and Mental Disorders

Шишкина

Калинина

Gulyaeva

et al. 2021

Biochemistry Moscow

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Ischemic brain injuries are accompanied by the long-term changes in gene expression in the hippocampus, the limbic system structure, involved in the regulation of key aspects of the higher nervous activity, such as cognitive functions and emotions. The altered expression of genes and proteins encoded by them may be related to the development of post-ischemic psycho-emotional and cognitive disturbances. Activation of neuroinflammation following stroke in the hippocampus has been suggested to play an essential role in induction of long-lasting consequences. Identification of changes in the gene expression patterns after ischemia and investigation of the dynamics of these changes in the hippocampus are the necessary first steps toward understanding molecular pathways responsible for the development of post-stroke cognitive impairments and mental pathologies.

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Decrease in Oxidative Stress Parameters after Post‐Ischaemic Recombinant Human Erythropoietin Administration in the Hippocampus of Rats Exposed to Focal Cerebral Ischaemia

Cited by 11 publications

References 81 publications

Early‐life N‐arachidonoyl‐dopamine exposure increases antioxidant capacity of the brain tissues and reduces functional deficits after neonatal hypoxia in rats

Early‐life N‐arachidonoyl‐dopamine exposure increases antioxidant capacity of the brain tissues and reduces functional deficits after neonatal hypoxia in rats

Neuroprotective Effect of the Recombinant Human Erythropoietin in the Enthorinal Cortex and Thalamus of Rats Exposed to Focal Cerebral Ischemia

Changes in Gene Expression and Neuroinflammation in the Hippocampus after Focal Brain Ischemia: Involvement in the Long-Term Cognitive and Mental Disorders

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