Calretinin Interneurons are Early Targets of Extracellular Amyloid-β Pathology in PS1/AβPP Alzheimer Mice Hippocampus

Baglietto‐Vargas, David; Moreno-González, Inés; Sánchez-Varo, Raquel; Jiménez, Sebastián; Trujillo‐Estrada, Laura; Sánchez-Mejías, Elisabeth; Torres, M.; Romero-Acebal, Manuel; Ruano, Diego; Vizuete, Marisa; Vitórica, Javier; Gutiérrez, Antonia

doi:10.3233/jad-2010-100066

Cited by 83 publications

(76 citation statements)

References 45 publications

(71 reference statements)

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“…This lack of evident changes in GABAergic terminals is in line with the recent report showing that the number of GABAergic neurons is not altered in early phases of AD (Krantic et al, 2012) being only modified at later stages of AD (Hardy et al, 1987b;Bell et al, 2003León-Espinosa et al, 2012). However, this finding should not hinder the evidence that there are early changes in the activity of GABAergic neurons in early AD (Baglietto-Vargas et al, 2010;Verret et al, 2012), typified by a desynchronization of hippocampal circuits (reviewed in Palop and Mucke, 2010) which correction with levetiracetam results in the preservation of memory performance (Sanchez et al, 2012). Since this is proposed to result from the dysfunction of particular populations of interneurons (BagliettoVargas et al, 2010;Verret et al, 2012), it is possible that putative changes in the presynaptic density and function of these particular populations may not be measurable with a global marker of GABAergic terminals such as vGAT.…”

Section: Discussionsupporting

confidence: 91%

“…Indeed, the cholinergic hypothesis of AD assumes a particular susceptibility of cholinergic neurons (reviewed in Q1 Bartus et al, 1982;Auld et al, 2002), reflecting a primary affection of cholinergic terminals in cortical regions early in AD (Hu et al, 2003). More recently, several studies have suggested a particular vulnerability of glutamatergic synapses Kirvell et al, 2006;Kashani et al, 2008;Minkeviciene et al, 2008;Proctor et al, 2010), whereas other studies have instead reported that it is GABAergic neurons that are initially affected in early AD (Agarwal et al, 2008;Baglietto-Vargas et al, 2010;Verret et al, 2012).…”

Section: Introductionmentioning

confidence: 97%

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Predominant loss of glutamatergic terminal markers in a β-amyloid peptide model of Alzheimer's disease

et al. 2014

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Section: Discussionsupporting

confidence: 91%

Section: Introductionmentioning

confidence: 97%

Predominant loss of glutamatergic terminal markers in a β-amyloid peptide model of Alzheimer's disease

et al. 2014

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“…Immunohistochemistry against DCX, a commonly used neuroblast marker that correlates well with the number of newly generated neurons in the hippocampus (Brown et al, 2003), supported these observations. Our data are in line with previously published studies demonstrating altered neurogenesis in AD (Baglietto-Vargas et al, 2010;Moon et al, 2014;Tatebayashi, 2003).…”

Section: Calretinin Immunoreactivitysupporting

confidence: 95%

Vulnerability of calbindin, calretinin and parvalbumin in a transgenic/knock-in APPswe/PS1dE9 mouse model of Alzheimer disease together with disruption of hippocampal neurogenesis

Verdaguer

Brox

Петров

et al. 2015

Experimental Gerontology

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“…In this sense, the selective inhibitory effect of A␤ oligomers (NGF Ͼ IGF-1 ϭ insulin Ͼ BDNF) might contribute to this decreased signal and, in consequence, be implicated in the preferential vulnerability of the cholinergic system observed in AD. It has also been demonstrated that A␤ oligomers could directly bind to p75NTR (55,58) producing the formation of neuritic dystrophies (also observed in our model) (30,59,60) and the activation of c-Jun kinases mediating cell degeneration (61). Thus, the appearance of A␤ oligomers could actively decrease the trophic support, interacting with trophic receptors (this work), and/or increase the toxic signaling activating death receptors such as p75NTR.…”

Section: Discussionsupporting

confidence: 62%

Age-dependent Accumulation of Soluble Amyloid β (Aβ) Oligomers Reverses the Neuroprotective Effect of Soluble Amyloid Precursor Protein-α (sAPPα) by Modulating Phosphatidylinositol 3-Kinase (PI3K)/Akt-GSK-3β Pathway in Alzheimer Mouse Model

Jiménez

Torres

Vizuete

et al. 2011

Journal of Biological Chemistry

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170

157

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Neurotrophins, activating the PI3K/Akt signaling pathway, control neuronal survival and plasticity. Alterations in NGF, BDNF, IGF-1, or insulin signaling are implicated in the pathogenesis of Alzheimer disease. We have previously characterized a bigenic PS1؋APP transgenic mouse displaying early hippocampal A␤ deposition (3 to 4 months) but late (17 to 18 months) neurodegeneration of pyramidal cells, paralleled to the accumulation of soluble A␤ oligomers. We hypothesized that PI3K/Akt/GSK-3␤ signaling pathway could be involved in this apparent age-dependent neuroprotective/neurodegenerative status. In fact, our data demonstrated that, as compared with age-matched nontransgenic controls, the Ser-9 phosphorylation of GSK-3␤ was increased in the 6-month PS1؋APP hippocampus, whereas in aged PS1؋APP animals (18 months), GSK-3␤ phosphorylation levels displayed a marked decrease. Using N2a and primary neuronal cell cultures, we demonstrated that soluble amyloid precursor protein-␣ (sAPP␣), the predominant APP-derived fragment in young PS1؋APP mice, acting through IGF-1 and/or insulin receptors, activated the PI3K/Akt pathway, phosphorylated the GSK-3␤ activity, and in consequence, exerted a neuroprotective action. On the contrary, several oligomeric A␤ forms, present in the soluble fractions of aged PS1؋APP mice, inhibited the induced phosphorylation of Akt/GSK-3␤ and decreased the neuronal survival. Furthermore, synthetic A␤ oligomers blocked the effect mediated by different neurotrophins (NGF, BDNF, insulin, and IGF-1) and sAPP␣, displaying high selectivity for NGF. In conclusion, the age-dependent appearance of APP-derived soluble factors modulated the PI3K/Akt/GSK-3␤ signaling pathway through the major neurotrophin receptors. sAPP␣ stimulated and A␤ oligomers blocked the prosurvival signaling. Our data might provide insights into the selective vulnerability of specific neuronal groups in Alzheimer disease.The molecular mechanisms underlying the selective neurodegeneration in Alzheimer disease (AD) 5 remain unclear. Amyloid-␤ (A␤) peptides, proteolytically excised from the amyloid precursor protein (APP), are considered the primary pathological agents in AD. However, their precise modes of action, toxic conformational forms, and molecular targets are still controversial (for review see Ref. 1). Transgenic mouse models, overexpressing mutated forms of human APP, are widely used to study AD pathogenesis. These models develop extensive A␤ deposition in the disease-vulnerable brain regions (such as hippocampus); however, neurons are well protected until late ages. The factors and pathways maintaining neuronal integrity at young/middle ages in these AD models and those inducing neurodegeneration in the aged animals remains to be defined.NGF, BDNF, IGF-1, and insulin are trophic factors critical for neuronal survival and plasticity, underlying memory, and learning (2-4) and could be implicated in AD development.

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Calretinin Interneurons are Early Targets of Extracellular Amyloid-β Pathology in PS1/AβPP Alzheimer Mice Hippocampus

Cited by 83 publications

References 45 publications

Predominant loss of glutamatergic terminal markers in a β-amyloid peptide model of Alzheimer's disease

Predominant loss of glutamatergic terminal markers in a β-amyloid peptide model of Alzheimer's disease

Vulnerability of calbindin, calretinin and parvalbumin in a transgenic/knock-in APPswe/PS1dE9 mouse model of Alzheimer disease together with disruption of hippocampal neurogenesis

Age-dependent Accumulation of Soluble Amyloid β (Aβ) Oligomers Reverses the Neuroprotective Effect of Soluble Amyloid Precursor Protein-α (sAPPα) by Modulating Phosphatidylinositol 3-Kinase (PI3K)/Akt-GSK-3β Pathway in Alzheimer Mouse Model

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