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Erschienen in: Metabolic Brain Disease 6/2017

21.08.2017 | Short Communication

Concurrent assessment of calpain and caspase3 activities in brains of mice with acetaminophen-induced acute hepatic encephalopathy

verfasst von: Bahareh Shabrang, Akram Jamshidzadeh, Mojtaba Farjam, Azin Ebrahimpour, Omid Koohi-Hosseinabadi

Erschienen in: Metabolic Brain Disease | Ausgabe 6/2017

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Abstract

To develop pharmacological therapy for acute hepatic encephalopathy (AHE), understanding the molecular basis for cell injury is essential. Excitotoxic neural cell injury mediated by calpain as a post- receptor mechanism has been proposed as a player in neuronal injury in AHE. Concurrent assessment of Calpain and Caspase3 activities in the brain of AHE mice in acetaminophen- induced mourine model was performed. After induction of AHE by acetaminophen in mice, the model was confirmed by histopathological, biochemical and behavioural studies. The brains were removed, western blot analysis was done and the relative activity of calpain and caspase was estimated and compared to control group calpain but not caspase 3 activity was significantly increased in the AHE group compared to the control brains. Experimentally, this finding is the first to report. Increased calpain activity in liver has been previously reported. To translate both finding it can be suggested that calpain inhibition can be an investigational intervention in saving lives in AHE. To confirm the results, besides more advanced toxicodynamic studies on acetaminophen, the results should be confirmed in other models of AHE in future.
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Metadaten
Titel
Concurrent assessment of calpain and caspase3 activities in brains of mice with acetaminophen-induced acute hepatic encephalopathy
verfasst von
Bahareh Shabrang
Akram Jamshidzadeh
Mojtaba Farjam
Azin Ebrahimpour
Omid Koohi-Hosseinabadi
Publikationsdatum
21.08.2017
Verlag
Springer US
Erschienen in
Metabolic Brain Disease / Ausgabe 6/2017
Print ISSN: 0885-7490
Elektronische ISSN: 1573-7365
DOI
https://doi.org/10.1007/s11011-017-0096-z

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