Volume 21 No 1 (2023)
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Liraglutide improves cognitive outcome of diabetic sepsis-surviving 4 rats; possible involvement of tumor necrosis factor alpha and 5 hippocampal synaptic markers
Enas Elsisi, Nahed Salah El din , Basma Emad Aboulhoda , Laila Ahmed Rashed and Sarah Mahmoud Gamal
Abstract
Diabetes mellitus and sepsis are major causes of cognitive decline. Liraglutide (LIRA) is a GLP-1 agonist with potential beneficial effects on the CNS. The purpose of our study is to investigate the possible effect of liraglutide on post-sepsis cognitive decline in diabetic rats. Male albino rats were divided into five groups: Control group (C), Diabetes group (D), Diabetic-Septic group (DS), Diabetes-Sepsis LIRA-treated group (DS-ttt), Diabetic-septic pretreated group (DS-pre). After sepsis induction, DS-pre group showed significantly higher survival rate in comparison to DS and DS-ttt groups. At the end of experimental period, cognitive tests; (Y-maze) and Novel Object Recognition (NOR) test revealed significantly decreased percentage of correct alternations and discrimination index (DI), respectively, in D and DS groups and a significant increase in the LIRA treated groups (DS-ttt) and (DS-pre). In the hippocampus, inflammatory marker (TNF- α) increased, while synaptic function markers (CREB) and synaptophysin decreased significantly in D and DS groups. In these groups multiple degenerative changes in all hippocampal regions were found on H & E staining. LIRA treatment improved all these abnormalities. In conclusion, these findings suggest a possible role of LIRA in improvement of cognitive function in diabetic rats surviving sepsis; this effect could be mediated via modulation of inflammatory markers, insulin signaling in the hippocampus, synaptic function alteration, and microglial or astrocytic cells changes.
Keywords
Sepsis, Diabetes, Liraglutide, glucagon like peptide-1, hippocampu
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