Interaction Between the FOXO1A-209 Genotype and Tea Drinking Is Significantly Associated with Reduced Mortality at Advanced Ages.

dc.contributor.author

Zeng, Y

dc.contributor.author

Chen, H

dc.contributor.author

Ni, T

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Ruan, R

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Nie, C

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Liu, X

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Feng, L

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Zhang, F

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Lu, J

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Li, J

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Li, Y

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Tao, W

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Gregory, SG

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Gottschalk, W

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Lutz, MW

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Land, KC

dc.contributor.author

Yashin, A

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Tan, Q

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Yang, Z

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Bolund, L

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Ming, Q

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Yang, H

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Min, J

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Willcox, DC

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Willcox, BJ

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Gu, J

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Hauser, E

dc.contributor.author

Tian, X

dc.contributor.author

Vaupel, JW

dc.coverage.spatial

United States

dc.date.accessioned

2017-06-01T18:21:20Z

dc.date.available

2017-06-01T18:21:20Z

dc.date.issued

2016-06

dc.description.abstract

On the basis of the genotypic/phenotypic data from Chinese Longitudinal Healthy Longevity Survey (CLHLS) and Cox proportional hazard model, the present study demonstrates that interactions between carrying FOXO1A-209 genotypes and tea drinking are significantly associated with lower risk of mortality at advanced ages. Such a significant association is replicated in two independent Han Chinese CLHLS cohorts (p = 0.028-0.048 in the discovery and replication cohorts, and p = 0.003-0.016 in the combined dataset). We found the associations between tea drinking and reduced mortality are much stronger among carriers of the FOXO1A-209 genotype compared to non-carriers, and drinking tea is associated with a reversal of the negative effects of carrying FOXO1A-209 minor alleles, that is, from a substantially increased mortality risk to substantially reduced mortality risk at advanced ages. The impacts are considerably stronger among those who carry two copies of the FOXO1A minor allele than those who carry one copy. On the basis of previously reported experiments on human cell models concerning FOXO1A-by-tea-compounds interactions, we speculate that results in the present study indicate that tea drinking may inhibit FOXO1A-209 gene expression and its biological functions, which reduces the negative impacts of FOXO1A-209 gene on longevity (as reported in the literature) and offers protection against mortality risk at oldest-old ages. Our empirical findings imply that the health outcomes of particular nutritional interventions, including tea drinking, may, in part, depend upon individual genetic profiles, and the research on the effects of nutrigenomics interactions could potentially be useful for rejuvenation therapies in the clinic or associated healthy aging intervention programs.

dc.identifier

https://www.ncbi.nlm.nih.gov/pubmed/26414954

dc.identifier.eissn

1557-8577

dc.identifier.uri

https://hdl.handle.net/10161/14659

dc.language

eng

dc.publisher

Mary Ann Liebert, Inc., publishers

dc.relation.ispartof

Rejuvenation Res

dc.relation.isversionof

10.1089/rej.2015.1737

dc.subject

Age Factors

dc.subject

Aged, 80 and over

dc.subject

Aging

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Cause of Death

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China

dc.subject

Female

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Forkhead Box Protein O1

dc.subject

Gene Frequency

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Gene-Environment Interaction

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Genotype

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Heterozygote

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Homozygote

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Humans

dc.subject

Male

dc.subject

Phenotype

dc.subject

Protective Factors

dc.subject

Risk Assessment

dc.subject

Risk Factors

dc.subject

Survival Analysis

dc.title

Interaction Between the FOXO1A-209 Genotype and Tea Drinking Is Significantly Associated with Reduced Mortality at Advanced Ages.

dc.type

Journal article

duke.contributor.orcid

Gregory, SG|0000-0002-7805-1743

duke.contributor.orcid

Gottschalk, W|0000-0001-6760-2338

duke.contributor.orcid

Lutz, MW|0000-0001-8809-5574

duke.contributor.orcid

Land, KC|0000-0002-9551-7314

duke.contributor.orcid

Hauser, E|0000-0003-0367-9189

pubs.author-url

https://www.ncbi.nlm.nih.gov/pubmed/26414954

pubs.begin-page

195

pubs.end-page

203

pubs.issue

3

pubs.organisational-group

Basic Science Departments

pubs.organisational-group

Center for Population Health & Aging

pubs.organisational-group

Center for the Study of Aging and Human Development

pubs.organisational-group

Clinical Science Departments

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Duke

pubs.organisational-group

Duke Cancer Institute

pubs.organisational-group

Duke Molecular Physiology Institute

pubs.organisational-group

Duke Population Research Center

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Duke Population Research Institute

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Institutes and Centers

pubs.organisational-group

Institutes and Provost's Academic Units

pubs.organisational-group

Medicine

pubs.organisational-group

Medicine, Geriatrics

pubs.organisational-group

Molecular Genetics and Microbiology

pubs.organisational-group

Neurology

pubs.organisational-group

Neurology, Behavioral Neurology

pubs.organisational-group

Neurology, MS & Neuroimmunology

pubs.organisational-group

Sanford School of Public Policy

pubs.organisational-group

School of Medicine

pubs.organisational-group

Social Science Research Institute

pubs.organisational-group

University Institutes and Centers

pubs.publication-status

Published

pubs.volume

19

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