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Puzzling role of genetic risk factors in human longevity: “risk alleles” as pro-longevity variants

Complex diseases are major contributors to human mortality in old age. Paradoxically, many genetic variants that have been associated with increased risks of such diseases are found in genomes of long-lived people, and do not seem to compromise longevity. Here we argue that trade-off-like and condit...

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Autores principales: Ukraintseva, Svetlana, Yashin, Anatoliy, Arbeev, Konstantin, Kulminski, Alexander, Akushevich, Igor, Wu, Deqing, Joshi, Gaurang, Land, Kenneth C., Stallard, Eric
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Springer Netherlands 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4724477/
https://www.ncbi.nlm.nih.gov/pubmed/26306600
http://dx.doi.org/10.1007/s10522-015-9600-1
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author Ukraintseva, Svetlana
Yashin, Anatoliy
Arbeev, Konstantin
Kulminski, Alexander
Akushevich, Igor
Wu, Deqing
Joshi, Gaurang
Land, Kenneth C.
Stallard, Eric
author_facet Ukraintseva, Svetlana
Yashin, Anatoliy
Arbeev, Konstantin
Kulminski, Alexander
Akushevich, Igor
Wu, Deqing
Joshi, Gaurang
Land, Kenneth C.
Stallard, Eric
author_sort Ukraintseva, Svetlana
collection PubMed
description Complex diseases are major contributors to human mortality in old age. Paradoxically, many genetic variants that have been associated with increased risks of such diseases are found in genomes of long-lived people, and do not seem to compromise longevity. Here we argue that trade-off-like and conditional effects of genes can play central role in this phenomenon and in determining longevity. Such effects may occur as result of: (i) antagonistic influence of gene on the development of different health disorders; (ii) change in the effect of gene on vulnerability to death with age (especially, from “bad” to “good”); (iii) gene–gene interaction; and (iv) gene–environment interaction, among other factors. A review of current knowledge provides many examples of genetic factors that may increase the risk of one disease but reduce chances of developing another serious health condition, or improve survival from it. Factors that may increase risk of a major disease but attenuate manifestation of physical senescence are also discussed. Overall, available evidence suggests that the influence of a genetic variant on longevity may be negative, neutral or positive, depending on a delicate balance of the detrimental and beneficial effects of such variant on multiple health and aging related traits. This balance may change with age, internal and external environments, and depend on genetic surrounding. We conclude that trade-off-like and conditional genetic effects are very common and may result in situations when a disease “risk allele” can also be a pro-longevity variant, depending on context. We emphasize importance of considering such effects in both aging research and disease prevention.
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spelling pubmed-47244772016-02-22 Puzzling role of genetic risk factors in human longevity: “risk alleles” as pro-longevity variants Ukraintseva, Svetlana Yashin, Anatoliy Arbeev, Konstantin Kulminski, Alexander Akushevich, Igor Wu, Deqing Joshi, Gaurang Land, Kenneth C. Stallard, Eric Biogerontology Review Article Complex diseases are major contributors to human mortality in old age. Paradoxically, many genetic variants that have been associated with increased risks of such diseases are found in genomes of long-lived people, and do not seem to compromise longevity. Here we argue that trade-off-like and conditional effects of genes can play central role in this phenomenon and in determining longevity. Such effects may occur as result of: (i) antagonistic influence of gene on the development of different health disorders; (ii) change in the effect of gene on vulnerability to death with age (especially, from “bad” to “good”); (iii) gene–gene interaction; and (iv) gene–environment interaction, among other factors. A review of current knowledge provides many examples of genetic factors that may increase the risk of one disease but reduce chances of developing another serious health condition, or improve survival from it. Factors that may increase risk of a major disease but attenuate manifestation of physical senescence are also discussed. Overall, available evidence suggests that the influence of a genetic variant on longevity may be negative, neutral or positive, depending on a delicate balance of the detrimental and beneficial effects of such variant on multiple health and aging related traits. This balance may change with age, internal and external environments, and depend on genetic surrounding. We conclude that trade-off-like and conditional genetic effects are very common and may result in situations when a disease “risk allele” can also be a pro-longevity variant, depending on context. We emphasize importance of considering such effects in both aging research and disease prevention. Springer Netherlands 2015-08-26 2016 /pmc/articles/PMC4724477/ /pubmed/26306600 http://dx.doi.org/10.1007/s10522-015-9600-1 Text en © Springer Science+Business Media Dordrecht 2015
spellingShingle Review Article
Ukraintseva, Svetlana
Yashin, Anatoliy
Arbeev, Konstantin
Kulminski, Alexander
Akushevich, Igor
Wu, Deqing
Joshi, Gaurang
Land, Kenneth C.
Stallard, Eric
Puzzling role of genetic risk factors in human longevity: “risk alleles” as pro-longevity variants
title Puzzling role of genetic risk factors in human longevity: “risk alleles” as pro-longevity variants
title_full Puzzling role of genetic risk factors in human longevity: “risk alleles” as pro-longevity variants
title_fullStr Puzzling role of genetic risk factors in human longevity: “risk alleles” as pro-longevity variants
title_full_unstemmed Puzzling role of genetic risk factors in human longevity: “risk alleles” as pro-longevity variants
title_short Puzzling role of genetic risk factors in human longevity: “risk alleles” as pro-longevity variants
title_sort puzzling role of genetic risk factors in human longevity: “risk alleles” as pro-longevity variants
topic Review Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4724477/
https://www.ncbi.nlm.nih.gov/pubmed/26306600
http://dx.doi.org/10.1007/s10522-015-9600-1
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