APOE2: protective mechanism and therapeutic implications for Alzheimer’s disease

Li, Zonghua; Shue, Francis; Zhao, Na; Shinohara, Mitsuru; Bu, Guojun

doi:10.1186/s13024-020-00413-4

Cited by 123 publications

(126 citation statements)

References 348 publications

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“…Noteworthy, APOE e2 has been identified as a longevity variant, associated with beneficial effects on cognition, and accumulating evidence suggested it protects against AD (reviewed in [ 61 ]). While the mechanisms driving its protective effect remain unclear, potential therapeutic strategies designed to leverage the protective effect of APOE e2, such as viral-mediated overexpression of APOE e2 and gene-editing conversion of APOE e4 to e2, hold promise as treatment options for AD.…”

Section: The Apoe Locus Is the Strongest Genetimentioning

confidence: 99%

“…With that said, APOE e2 increases the risk of other diseases, including neurological disorders; thus, long-term safety concerns should be carefully evaluated when considering treatments inspired by the protective role of e2 in AD. This topic has been extensively reviewed elsewhere [ 61 , 62 ] and is outside the scope of this review.…”

Section: The Apoe Locus Is the Strongest Genetimentioning

confidence: 99%

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APOE: The New Frontier in the Development of a Therapeutic Target towards Precision Medicine in Late-Onset Alzheimer’s

Yang

Kantor

Chiba‐Falek

2021

IJMS

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Alzheimer’s disease (AD) has a critical unmet medical need. The consensus around the amyloid cascade hypothesis has been guiding pre-clinical and clinical research to focus mainly on targeting beta-amyloid for treating AD. Nevertheless, the vast majority of the clinical trials have repeatedly failed, prompting the urgent need to refocus on other targets and shifting the paradigm of AD drug development towards precision medicine. One such emerging target is apolipoprotein E (APOE), identified nearly 30 years ago as one of the strongest and most reproduceable genetic risk factor for late-onset Alzheimer’s disease (LOAD). An exploration of APOE as a new therapeutic culprit has produced some very encouraging results, proving that the protein holds promise in the context of LOAD therapies. Here, we review the strategies to target APOE based on state-of-the-art technologies such as antisense oligonucleotides, monoclonal antibodies, and gene/base editing. We discuss the potential of these initiatives in advancing the development of novel precision medicine therapies to LOAD.

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Section: The Apoe Locus Is the Strongest Genetimentioning

confidence: 99%

Section: The Apoe Locus Is the Strongest Genetimentioning

confidence: 99%

APOE: The New Frontier in the Development of a Therapeutic Target towards Precision Medicine in Late-Onset Alzheimer’s

Yang

Kantor

Chiba‐Falek

2021

IJMS

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“…Homozygous carriers for APOE4 are 8-12 times more likely to develop AD than non-carriers (Michaelson, 2014). In contrast, individuals carrying the ε2 allele of APOE ( APOE2 ) have reduced risk of developing AD, supporting that it is neuroprotective against AD development (Conejero-Goldberg et al, 2014; Huang and Mahley, 2014; Huynh et al, 2017; Li et al, 2020). While APOE functions to mediate lipid transfer between cells, the APOE4 variant has reduced lipid transport capacity (Hatters et al, 2006; Liu et al, 2017).…”

Section: Introductionmentioning

confidence: 99%

Neuronal ROS-Induced Glial Lipid Droplet Formation is Altered by Loss of Alzheimer’s Disease-associated Genes

Moulton

Barish

Ralhan

et al. 2021

Preprint

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A growing list of Alzheimers disease (AD) genetic risk factors is being identified, but the contribution of these genetic mutations to disease remains largely unknown. Accumulating data support a role of lipid dysregulation and excessive ROS in the etiology of AD. Here, we identified cell-specific roles for eight AD risk-associated genes in ROS-induced glial lipid droplet (LD) formation. We demonstrate that ROS-induced glial LD formation requires two ABCA transporters (ABCA1 and ABCA7) in neurons, the APOE receptor (LRP1), endocytic genes (PICALM, CD2AP, and AP2A2) in glia, and retromer genes (VPS26 and VPS35) in both neurons and glia. Moreover, ROS strongly enhances Aβ42-toxicity in flies and Aβ42-plaque formation in mice. Finally, an ABCA1-activating peptide restores glial LD formation in the APOE4-associated loss of LD. This study places AD risk factors in a neuron-to-glia lipid transfer pathway with a critical role in protecting neurons from ROS-induced toxicity.

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“…Human APOE genotype plays an important role in the homeostasis of the central nervous system and has long been linked to neurodegenerative disorders ( Huang, 2006 ; Mahley et al, 2007 ; Yamazaki et al, 2019 ; Chen et al, 2020 ; Lanfranco et al, 2020 ; Lewandowski et al, 2020 ; Li et al, 2020 ). For example, APOE4 is associated with greater cognitive decline in aging, poorer outcomes following stroke and traumatic brain injury, and is a major genetic risk factor for Alzheimer’s disease compared to APOE3 (reviewed in Mahley et al, 2007 ; Liu et al, 2013 ; Flowers and Rebeck, 2020 ).…”

Section: Introductionmentioning

confidence: 99%

Autocrine Effects of Brain Endothelial Cell-Produced Human Apolipoprotein E on Metabolism and Inflammation in vitro

Marottoli

Trevino

Geng

et al. 2021

Front. Cell Dev. Biol.

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Reports of APOE4-associated neurovascular dysfunction during aging and in neurodegenerative disorders has led to ongoing research to identify underlying mechanisms. In this study, we focused on whether the APOE genotype of brain endothelial cells modulates their own phenotype. We utilized a modified primary mouse brain endothelial cell isolation protocol that enabled us to perform experiments without subculture. Through initial characterization we found, that compared to APOE3, APOE4 brain endothelial cells produce less apolipoprotein E (apoE) and have altered metabolic and inflammatory gene expression profiles. Further analysis revealed APOE4 brain endothelial cultures have higher preference for oxidative phosphorylation over glycolysis and, accordingly, higher markers of mitochondrial activity. Mitochondrial activity generates reactive oxygen species, and, with APOE4, there were higher mitochondrial superoxide levels, lower levels of antioxidants related to heme and glutathione and higher markers/outcomes of oxidative damage to proteins and lipids. In parallel, or resulting from reactive oxygen species, there was greater inflammation in APOE4 brain endothelial cells including higher chemokine levels and immune cell adhesion under basal conditions and after low-dose lipopolysaccharide (LPS) treatment. In addition, paracellular permeability was higher in APOE4 brain endothelial cells in basal conditions and after high-dose LPS treatment. Finally, we found that a nuclear receptor Rev-Erb agonist, SR9009, improved functional metabolic markers, lowered inflammation and modulated paracellular permeability at baseline and following LPS treatment in APOE4 brain endothelial cells. Together, our data suggest that autocrine signaling of apoE in brain endothelial cells represents a novel cellular mechanism for how APOE regulates neurovascular function.

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APOE2: protective mechanism and therapeutic implications for Alzheimer’s disease

Cited by 123 publications

References 348 publications

APOE: The New Frontier in the Development of a Therapeutic Target towards Precision Medicine in Late-Onset Alzheimer’s

APOE: The New Frontier in the Development of a Therapeutic Target towards Precision Medicine in Late-Onset Alzheimer’s

Neuronal ROS-Induced Glial Lipid Droplet Formation is Altered by Loss of Alzheimer’s Disease-associated Genes

Autocrine Effects of Brain Endothelial Cell-Produced Human Apolipoprotein E on Metabolism and Inflammation in vitro

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