Amelioration of BPSD-Like Phenotype and Cognitive Decline in SAMP8 Mice Model Accompanied by Molecular Changes after Treatment with I2-Imidazoline Receptor Ligand MCR5

Rodríguez-Arévalo

Bagán

et al. 2021

British J Pharmacology

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Background and Purpose: The development of effective therapeutic strategies against Alzheimer's disease (AD) remains a challenge. I 2 imidazoline receptor ligands have a neuroprotective role in AD. Moreover, co-treatment of AChE inhibitors with neuroprotective agents have shown better effects on the prevention of dementia.Here, we assessed the potential therapeutic effect of the I 2 ligand, donepezil and their combination in 5XFAD mice. Experimental Approach: 5XFAD female mice were treated with low doses (1 mgÁkg À1 Áday À1 ) of LSL60101, donepezil and donepezil plus LSL60101, during 4 weeks per os. Novel object recognition, Morris water maze, open field, elevated plus maze and three-chamber tests were used to evaluate the cognitive and behavioural status after treatment. The effects on AD-like pathology were assessed with immunohistochemistry, western blot, ELISA and qPCR. Key Results: Chronic low-dose treatment with LSL60101 and donepezil reversed cognitive deficits and impaired social behaviour. LSL60101 treatment did not affect anxiety-like behaviour in contrast to donepezil. In the 5XFAD brains, LSL60101 and donepezil/LSL60101 treatments attenuated amyloid-β pathology by decreasing amyloid-β 40 and amyloid-β 42 levels, amyloid-β plaque number and tau hyperphosphorylation. These alterations were accompanied by reduced microglia marker Iba-1 levels and increased Trem2 gene expression. LSL60101 and donepezil decreased glial fibrillary acidic protein (GFAP) astrocytic marker reactivity. However, only LSL60101 and donepezil/LSL60101 treatments significantly increased the synaptic marker levels of post-synaptic density protein 95 and synaptophysin. Conclusion and Implications:Chronic low-dose treatment with selective I 2 -ligands can be an effective treatment for AD and provide insights into combination treatments for symptomatic and disease-modifying drugs.

Section: Discussionsupporting

confidence: 57%

Disease‐modifying treatment with I₂ imidazoline receptor ligand LSL60101 in an Alzheimer's disease mouse model: a comparative study with donepezil

Rodríguez-Arévalo

Bagán

et al. 2021

British J Pharmacology

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“…On the other hand, inflammatory gene expression increase (Ιλ-1β, Ιλ-6, and Ccl12 ) was observed after treatment with I2-IR ligand LSL60101 but not with donepezil. Interestingly, this is further supported by a significant upregulation of Trem2 gene expression determined in the LSL60101 treated mice, further confirming the neuroinflammatory modulation by I2-IR ligand LSL60101(Hwang et al, 2010;Griñán-Ferré et al, 2019;Vasilopoulou et al, 2020a). Furthermore, increased Trem2 expression has been shown to reprogram microglia responsivity mediating microglial cytokine release, migration and clearance of Aβ deposits, ameliorating neuropathological and behavioural deficits of AD mouse models(Lee et al, 2018;Zhao et al, 2018).…”

supporting

confidence: 57%

Disease-modifying treatment with I2 imidazoline receptor ligand LSL60101 in an Alzheimer’s disease mouse model : A Comparative study with donepezil

Rodríguez-Arévalo

Bagán

et al. 2020

Preprint

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Background and Purpose: The development of effective therapeutic strategies against Alzheimer’s disease (AD) remains a challenge. I2 Imidazoline receptors (I2-IR) ligands have a neuroprotective role in AD. While co-treatment of acetylcholinesterase inhibitors with neuroprotective agents have shown better effects on the prevention of dementia. Here, we assessed the potential therapeutic effect of the I2-IR ligand LSL60101, donepezil and their combination in 5XFAD mice. Experimental Approach: 5XFAD female mice were treated with low doses of LSL60101 (1mg/kg/day), donepezil (1mg/kg/day), and donepezil plus LSL60101 (1+1mg/kg/day), during 4 weeks per os. Novel object recognition, Morris water maze, open field, elevated plus maze and three-chamber tests were employed to evaluate the cognitive and behavioural status of the mice after treatment. The effects of the treatments on AD-like pathology were assessed with immunohistochemistry, Western blot and qPCR. Key results: Chronic low-dose treatment with LSL60101 and donepezil reversed cognitive deficits and impaired social behaviour. LSL60101 treatment did not affect anxiety-like behaviour in contrast to donepezil. In the 5XFAD brains, LSL60101 and donepezil/LSL60101 treatments decreased Aβ-pathology and Tau hyperphosphorylation, and these alterations were accompanied by decreased microglia marker Iba-1 levels and increased Trem2 gene expression. LSL60601 and donepezil decreased glial fibrillary acidic protein (GFAP) astrocytic marker reactivity. However, only LSL60601 treatment significantly increased the levels of the synaptic markers post-density 95 (PSD95) and synaptophysin (SYN). Conclusion and implications: Our results suggest that chronic low dose treatment with selective I2-IR ligands can be an effective treatment for AD and provide insights into combination treatments of symptomatic and disease-modifying drugs

“…In vitro studies corroborate that I2-IR ligands exert their action on the glial cells by suppressing astrocytic activation induced by lipopolysaccharide (LPS) and decreasing TNF-α levels [ 13 ]. Consistent with these changes, the recently described I2-IR ligands MCR5 and B06 decrease the expression of proinflammatory markers, such as TNF-α, IL-1β and interleukin 6 (IL-6), and promote synaptic plasticity in a mouse model of aging and neurodegeneration [ 14 , 15 , 16 ]. Interestingly, I2-IR have been found dysregulated in patients with neurodegenerative diseases, such as Alzheimer’s disease (AD) [ 17 , 18 ].…”

Section: Introductionmentioning

confidence: 79%

“…Of note, activation of the NF-κβ pathway is closely related to neurodegeneration and particularly to AD [ 35 ], while its inhibition has been shown to improve cognitive deficits in in vivo models of AD [ 49 ]. In turn, reductions in NF-κβ-regulated genes, such as Il-1β , Cox2 and Tnf-α , were observed after treatments with selective I2-IR ligands, delivering neuroprotection in mouse models of aging neurodegeneration and AD [ 14 , 15 , 16 , 39 ]. Therefore, downregulation of the NF-κβ pathway by LSL60101 might partially account for the altered gene expression of inflammatory markers and further explain its neuroprotective effect in this AD mouse model.…”

Section: Discussionmentioning

confidence: 99%

Microarray Analysis Revealed Inflammatory Transcriptomic Changes after LSL60101 Treatment in 5XFAD Mice Model

Escolano

Pallàs

et al. 2021

Genes

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I2-IR have been found dysregulated in patients with neurodegenerative diseases, such as Alzheimer’s disease (AD), in which the importance of neuroinflammation in the establishment and maintenance of cognitive decline is well-documented. To research the implication of I2-IR in neuroinflammatory pathways altered in AD, we determined the expression profile of genes associated with inflammation in the 5XFAD model treated with LSL60101, a well-established I2-IR ligand. Thus, we performed a qPCR array containing 84 inflammation-related genes. Hierarchical clustering analysis revealed three gene clusters, suggesting that treatment with LSL60101 affects the gene expression associated with inflammation in the 5XFAD model. Furthermore, we evaluated the functions of the three clusters; thereby performing a pathway enrichment analysis using the GO database. As we expected, clusters 2 and 3 showed alterations in the inflammatory response, chemotaxis and the chemokine-mediated signaling pathway, among others. To validate previous results from the gene profiling analysis, the expression levels of a representative subset of mRNAs were selected according to the intensity of the observed changes and their biological relevance. Interestingly, changes induced by LSL60101 in the 5XFAD model were validated for several genes. These results suggest that treatment with LSL60101 in the 5XFAD model reverses the inflammatory process during the development of AD.