Identification and modification of amyloid-independent phenotypes of APOE4 mice

DiBattista, Amanda M.; Dumanis, Sonya B.; Newman, Joshua; Rebeck, G. William

doi:10.1016/j.expneurol.2016.04.014

Cited by 23 publications

(35 citation statements)

References 60 publications

(92 reference statements)

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“…Their inhibition at the middle age using ibuprofen can cause the pronounced life extending effect that we observed in the present study. Additionally, ibuprofen can regulate the activity of the protein apolipoprotein E that associated with the neurodegenerative processes in mammalian brain, including development of Alzheimer's and Parkinson's diseases, through the COX-2 inhibition and PPAR-γ activation (Melton et al, 2003; Lichtenstein et al, 2010; DiBattista et al, 2016). Investigations on transgenic fruit flies demonstrated that this effect can influence the lifespan and aging rate (Lichtenstein et al, 2010).…”

Section: Discussionmentioning

confidence: 99%

Geroprotective and Radioprotective Activity of Quercetin, (-)-Epicatechin, and Ibuprofen in Drosophila melanogaster

et al. 2016

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The modulation of longevity genes and aging-associated signaling pathways using pharmacological agents is one of the potential ways to prolong the lifespan and increase the vitality of an organism. Phytochemicals flavonoids and non-steroidal anti-inflammatory drugs have a large potential as geroprotectors. The goal of the present study was to investigate the effects of long-term and short-term consumption of quercetin, (-)-epicatechin, and ibuprofen on the lifespan, resistance to stress factors (paraquat, hyperthermia, γ-radiation, and starvation), as well as age-dependent physiological parameters (locomotor activity and fecundity) of Drosophila melanogaster. The long-term treatment with quercetin and (-)-epicatechin didn't change or decreased the lifespan of males and females. In contrast, the short-term treatment with flavonoids had a beneficial effect and stimulated the resistance to paraquat and acute γ-irradiation. The short-term ibuprofen consumption had a positive effect on the lifespan of females when it was carried out at the middle age (30–40 days), and to the survival of flies under conditions of oxidative and genotoxic stresses. However, it didn't change the lifespan of males and females after the treatment during first 10 days of an imago life. Additionally, quercetin, (-)-epicatechin, and ibuprofen decreased the spontaneous locomotor activity of males, but had no effect of stimulated the physical activity and fecundity of females. Revealed quercetin, (-)-epicatechin, and ibuprofen activity can be associated with the stimulation of stress response mechanisms through the activation of pro-longevity pathways, or the induction of hormesis.

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Section: Discussionmentioning

confidence: 99%

Geroprotective and Radioprotective Activity of Quercetin, (-)-Epicatechin, and Ibuprofen in Drosophila melanogaster

et al. 2016

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“…We have identified biochemical differences in modified versions of brain APOE: unmodified APOE is solubilized only in the presence of detergent and modified APOE is solubilized in saline (65). The ratio of these different forms is altered by APOE genotypes in mouse and human brains (65). The APOE isoform effects on APOE levels and on dimer formation support lossof-function explanations for the effects of APOE4, with APOE4 less able to clear debris and deliver lipids than APOE2 or APOE3.…”

Section: The Effects Of Apoe Genotype On Apoe Levels and Posttranslatmentioning

confidence: 87%

“…Finally, the APOE protein is modified by O-glycosylation (64), and to a greater extent in the CNS than in the periphery (26). We have identified biochemical differences in modified versions of brain APOE: unmodified APOE is solubilized only in the presence of detergent and modified APOE is solubilized in saline (65). The ratio of these different forms is altered by APOE genotypes in mouse and human brains (65).…”

Section: The Effects Of Apoe Genotype On Apoe Levels and Posttranslatmentioning

confidence: 99%

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The role of APOE on lipid homeostasis and inflammation in normal brains

Rebeck

2017

Journal of Lipid Research

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105

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The role of APOE in the risk of Alzheimer's disease (AD) has largely focused on its effects on AD pathological processes. However, there are increasing data that genotype affects processes in normal brains. Studies of young cognitively normal humans show effects of genotype on brain structure and activity. Studies of normal knock-in mice show effects of genotype on brain structure, neuronal markers, and behavior. APOE interactions with molecules important for lipid efflux and lipid endocytosis underlie effects of genotype on neuroinflammation and lipoprotein composition. These effects provide important targets for new therapies for reduction of the risk of AD before any signs of pathogenesis.

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“…We thus analyzed human apoE-targeted replacement (apoE-TR) (12)(13)(14) and Apoe-knockout (15) mice to examine whether the effects of APOE on lifespan can indeed be observed in the absence of AD. In the absence of overexpressing mutant APP or mutant MAPT gene, these mice do not display remarkable amyloid or tau deposition such as those seen in AD (10,19,20). In the survival mouse cohort (n=118), due to the regulation of our animal experiment, we euthanized mice (33.9% of total animals) when they showed severe age-related symptoms including severe weakness, masses, significant skin lesions etc.…”

Section: Apoe2 Benefits Lifespan In Animal Models Associated With Prmentioning

confidence: 99%

APOE2promotes longevity independent of Alzheimer’s disease

Shinohara¹,

Kanekiyo²,

Tachibana

et al. 2020

Preprint

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ObjectiveAlthough apolipoprotein E (APOE) allele associates with longevity, its mechanism is not understood. The protective effects of APOE2 and the deleterious effects of APOE4 on Alzheimer’s disease (AD) risk may confound APOE effects on longevity.MethodsWe analyzed a large number of subjects from the National Alzheimer’s Coordinating Center (NACC), and animal models expressing human apoE isoforms in the absence of AD.ResultsClinically, the APOE2 allele was associated with longer lifespan, while APOE4 associated with shorter lifespan, compared to the common APOE3 allele. This effect was also seen irrespective of clinical AD status, and in subjects with little amyloid pathology or after adjustment for AD-related pathologies. In animal studies, apoE2-TR mice also exhibited longer lifespan, while apoE4 showed some trends of shorter lifespan. Notably, old apoE2-TR mice kept activity measured by open field assay, associated with longer lifespan. Evidence of preserved activity in APOE2 carrier was also obtained in clinical records. In animal studies, higher levels of apoE2 in brain and plasma were correlated with activity. Moreover, lower levels of total cholesterol in the brain and higher levels of high-density lipoprotein cholesterol and triglycerides in the plasma of apoE2-TR mice were associated with apoE levels and more activity.InterpretationAPOE2 can contribute to longevity independent of AD. Preserved activity would be an early-observable feature of apoE2-mediated longevity, where higher levels of apoE2 and its-associated lipid metabolism might be involved.

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Identification and modification of amyloid-independent phenotypes of APOE4 mice

Cited by 23 publications

References 60 publications

Geroprotective and Radioprotective Activity of Quercetin, (-)-Epicatechin, and Ibuprofen in Drosophila melanogaster

Geroprotective and Radioprotective Activity of Quercetin, (-)-Epicatechin, and Ibuprofen in Drosophila melanogaster

The role of APOE on lipid homeostasis and inflammation in normal brains

APOE2promotes longevity independent of Alzheimer’s disease

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