2013
DOI: 10.1515/revneuro-2013-0034
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New animal models of Alzheimer’s disease that display insulin desensitization in the brain

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Cited by 27 publications
(23 citation statements)
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“…This AD animal model also develops insulin desensitization in the brain, caused by STZ injections (Dhull et al, 2012;Lester-Coll et al, 2006;Plaschke, Mueller, & Hoyer, 2010;Salkovic-Petrisic & Hoyer, 2007). STZ enhances tau phosphorylation in the brain and that drugs developed for T2DM have protective effects in this model (Gao, Liu, Jiang, Ding, & Li, 2014;Gao, Liu, Li, & Hoelscher, 2013;Lester-Coll et al, 2006;Li et al, 2012;Shi et al, 2017). We therefore wanted to test whether the novel dual agonist DA5-CH has neuroprotective and restorative properties in the icv.-STZ-treated rat model of AD.…”
Section: Introductionmentioning
confidence: 99%
“…This AD animal model also develops insulin desensitization in the brain, caused by STZ injections (Dhull et al, 2012;Lester-Coll et al, 2006;Plaschke, Mueller, & Hoyer, 2010;Salkovic-Petrisic & Hoyer, 2007). STZ enhances tau phosphorylation in the brain and that drugs developed for T2DM have protective effects in this model (Gao, Liu, Jiang, Ding, & Li, 2014;Gao, Liu, Li, & Hoelscher, 2013;Lester-Coll et al, 2006;Li et al, 2012;Shi et al, 2017). We therefore wanted to test whether the novel dual agonist DA5-CH has neuroprotective and restorative properties in the icv.-STZ-treated rat model of AD.…”
Section: Introductionmentioning
confidence: 99%
“…Studies using transgenic AD mice models revealed that the transgenic mice exhibited hippocampal insulin resistance [11]. Leptin-deficient mice, a T2DM model, displayed impaired cerebral insulin signaling and cognitive impairments after treating with high-fat-diet [12, 13]. Postmortem study of AD brains indicated significant increase of insulin receptor substrate-1 (IRS-1) phosphorylation at serine residues, marker of insulin resistance.…”
Section: Introductionmentioning
confidence: 99%
“…Alzheimer's disease involves multifactorial brain changes including problems with amyloid and tau processing, neuronal degeneration, insulin dysregulation, synaptic loss, chronic inflammation, oxidative stress, and accumulation of metals [1][2][3]. The disruption of metal homeostasis has led to the suggested use of metal-binding agents as a potential therapeutic strategy [3].…”
Section: Introductionmentioning
confidence: 99%