<i>APOE</i>Alleles and Extreme Human Longevity

Sebastiani, Paola; Gurinovich, Anastasia; Nygaard, Marianne; Sasaki, Takashi; Sweigart, Benjamin; Bae, Harold; Andersen, Stacy L.; Villa, Francesco; Atzmon, Gil; Christensen, Kaare; Arai, Yasumichi; Barzilai, Nir; Puca, Annibale Alessandro; Christiansen, Lene; Hirose, Nobuyoshi; Perls, Thomas T.

doi:10.1093/gerona/gly174

Cited by 113 publications

(94 citation statements)

References 51 publications

(68 reference statements)

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“…Table displays characteristics of the NECS patients included in the analysis. We enriched the sample selection of carriers of the e 2 e 2 genotype of APOE that is more prevalent in healthy agers and centenarians (Sebastiani et al, ). The ages of study participants varied between 45 years and 114 years, but mean age per genotype groups was comparable.…”

Section: Resultsmentioning

confidence: 99%

“…The e 3 allele is the “neutral allele” in many ethnicities, while e 2 is the least common allele that emerged as a longevity variant when Schachter et al noted an increased frequency of e 2 in French centenarians (Schachter et al, ). Since then, several studies have provided evidence that e 2 has a beneficial neuroprotective effect (Kim et al, ), decreases neuroinflammation (Dorey, Chang, Liu, Yang, & Zhang, ), and promotes longevity (Sebastiani, Bae, et al, ; Sebastiani, Gurinovich, et al, ; Sebastiani et al, ) and healthy aging (Kulminski et al, ; Wu & Zhao, ). Therefore, we hypothesize that targets of this allele may lead to the discovery of treatments that help maintain good cognitive function and escape cognitive impairment with aging.…”

Section: Introductionmentioning

confidence: 99%

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A serum protein signature of APOE genotypes in centenarians

et al. 2019

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The discovery of treatments to prevent or delay dementia and Alzheimer's disease is a priority. The gene APOE is associated with cognitive change and late‐onset Alzheimer's disease, and epidemiological studies have provided strong evidence that the e 2 allele of APOE has a neuroprotective effect, it is associated with increased longevity and an extended healthy lifespan in centenarians. In this study, we correlated APOE genotype data of 222 participants of the New England Centenarian Study, including 75 centenarians, 82 centenarian offspring, and 65 controls, comprising 55 carriers of APOE e 2, with aptamer‐based serum proteomics (SomaLogic technology) of 4,785 human proteins corresponding to 4,137 genes. We discovered a signature of 16 proteins that associated with different APOE genotypes and replicated the signature in three independent studies. We also show that the protein signature tracks with gene expression profiles in brains of late‐onset Alzheimer's disease versus healthy controls. Finally, we show that seven of these proteins correlate with cognitive function patterns in longitudinally collected data. This analysis in particular suggests that Baculoviral IAP repeat containing two (BIRC2) is a novel biomarker of neuroprotection that associates with the neuroprotective allele of APOE. Therefore, targeting APOE e 2 molecularly may preserve cognitive function.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

A serum protein signature of APOE genotypes in centenarians

et al. 2019

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“…[ 22,23 ] Subjects with APOE4 genotype have substantially decreased extreme longevity unlike subjects with E2E3 genotype. [ 24 ] Though increased risk of AD pathology conferred by the APOE4 genotype has been studied, the basal metabolomic differences on “normal” aging remain to be elucidated and represent a significant opportunity.…”

Section: Application Of Metabolomics For Biomarker Discovery In Agingmentioning

confidence: 99%

The Aging Metabolome—Biomarkers to Hub Metabolites

Sharma

Ramanathan

2020

Proteomics

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Aging biology is intimately associated with dysregulated metabolism, which is one of the hallmarks of aging. Aging‐related pathways such as mTOR and AMPK, which are major targets of anti‐aging interventions including rapamcyin, metformin, and exercise, either directly regulate or intersect with metabolic pathways. In this review, numerous candidate bio‐markers of aging that have emerged using metabolomics are outlined. Metabolomics studies also reveal that not all metabolites are created equally. A set of core “hub” metabolites are emerging as central mediators of aging. The hub metabolites reviewed here are nicotinamide adenine dinucleotide, reduced nicotinamide dinucleotide phosphate, α‐ketoglutarate, and β‐hydroxybutyrate. These “hub” metabolites have signaling and epigenetic roles along with their canonical roles as co‐factors or intermediates of carbon metabolism. Together these hub metabolites suggest a central role of the TCA cycle in signaling and metabolic dysregulation associated with aging.

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“…Até o momento, estudos longitudinais De forma robusta, estudos demonstram efeito protetor do alelo ε2 para sobrevivência e longevidade, além de associação com redução de níveis de colesterol e doenças cardiovasculares, neuroproteção contra doença de Alzheimer e morte neuronal, redução de risco de acidente vascular cerebral em homens, redução de câncer gástrico e algumas doenças infecciosas, proteção celular do estresse oxidativo e morte celular, além de melhora de reparo ao DNA celular. Por outro lado, exemplificando o efeito pleitrópico do gene APOE, dados menos consistentes sugerem associação da presença do alelo ε2 com aumento de incidência de pneumonia, redução de densidade óssea e aumento de osteoporose, e risco aumentado de câncer de cólon(Rosvall et al, 2009; Kulminski et al, 2016; Souza et al, 2017;Sebastiani et al, 2018;Bos et al, 2018 Bos et al, ). 2016Bos et al, 2018).…”

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“…O alelo APOE ε4, por sua vez, está fortemente relacionado a fenótipos de doenças relacionadas ao envelhecimento, especialmente doença de Alzheimer e doenças cardiovasculares. Estudos demonstram associação positiva com aumento de mortalidade e redução de expectativa de vida, aumento de colesterol total e LDL-colesterol, risco aumentado de doença ateromatosa (de grandes vasos, doença coronariana e cerebrovascular), de hipertensão arterial sistêmica, de diabetes não insulino-dependente, de progressão de nefropatia diabética e glomerulopatias, de arritmias cardíacas e de demências, em especial doença de Alzheimer(Rea et al, 2001;Bahia et al, 2008; Kulminski et al, 2016;Tindale et al, 2017;Bos et al, 2018; Shi et al, 2018;Sebastiani et al, 2018;Liehn et al, 2018). No metabolismo celular, APOE ε4 está associado com aumento de estresse oxidativo, disfunção de macrófagos e inflamação, menor retirada de colesterol dos neurônios, aumento de neuroinflamação e de morte celular(Dose et al, …”

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Preditores do envelhecimento saudável: fatores epigenéticos e o gene APOE

Hojaij¹

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APOEAlleles and Extreme Human Longevity

Cited by 113 publications

References 51 publications

A serum protein signature of APOE genotypes in centenarians

A serum protein signature of APOE genotypes in centenarians

The Aging Metabolome—Biomarkers to Hub Metabolites

Preditores do envelhecimento saudável: fatores epigenéticos e o gene APOE

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