A Preliminary Study to Investigate the Genetic Background of Longevity Based on Whole-Genome Sequence Data of Two Methuselah Dogs

Aging is the largest risk factor in many diseases and mortality alike. As the elderly population is expected to increase at an accelerating rate in the future, these phenomena will pose a growing socio-economic burden on societies. To successfully cope with this challenge, a deeper understanding of...

Descripción completa

Detalles Bibliográficos
Autores principales: Jónás, Dávid, Sándor, Sára, Tátrai, Kitti, Egyed, Balázs, Kubinyi, Enikö
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Genetics
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7176982/
https://www.ncbi.nlm.nih.gov/pubmed/32373156
http://dx.doi.org/10.3389/fgene.2020.00315
_version_ 1783525118635409408
author Jónás, Dávid
Sándor, Sára
Tátrai, Kitti
Egyed, Balázs
Kubinyi, Enikö
author_facet Jónás, Dávid
Sándor, Sára
Tátrai, Kitti
Egyed, Balázs
Kubinyi, Enikö
author_sort Jónás, Dávid
collection PubMed
description Aging is the largest risk factor in many diseases and mortality alike. As the elderly population is expected to increase at an accelerating rate in the future, these phenomena will pose a growing socio-economic burden on societies. To successfully cope with this challenge, a deeper understanding of aging is crucial. In many aspects, the companion dog is an increasingly popular model organism to study aging, with the promise of producing results that are more applicable to humans than the findings that come from the studies of classical model organisms. In this preliminary study we used the whole-genome sequence of two extremely old dogs – age: 22 and 27 years (or 90–135% more, than the average lifespan of dogs) – in order to make the first steps to understand the genetic background of extreme longevity in dogs. We identified more than ∼80 1000 novel SNPs in the two dogs (7500 of which overlapped between them) when compared to three publicly available canine SNP databases, which included SNP information from850 dogs. Most novel mutations (∼52000 SNPs) were identified at non-coding regions, while 4.6% of the remaining SNPs (n∼1600) were at exons, including 670 missense variants – 76 of which overlapped between the two animals – across 472 genes. Based on their gene ontologies, these genes were related – among others – to gene transcription/translation and its regulation, to immune response and the nervous system in general. We also detected 12 loss-of-function mutations, although their actual effect is unclear. Several genetic pathways were also identified, which pathways may be tempting candidates to be investigated in large sample sizes in order to confirm their relevance in extreme longevity in dogs (and possibly, in humans). We hypothesize a possible link between extreme longevity and the regulation of gene transcription/translation, which hypothesis should be further investigated in the future. This phenomenon could define an interesting direction for future research aiming to better understand longevity. The presented preliminary results highlight the utility of the companion dog in the study of the genetic background of longevity and aging.
format Online
Article
Text
id pubmed-7176982
institution National Center for Biotechnology Information
language English
publishDate 2020
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-71769822020-05-05 A Preliminary Study to Investigate the Genetic Background of Longevity Based on Whole-Genome Sequence Data of Two Methuselah Dogs Jónás, Dávid Sándor, Sára Tátrai, Kitti Egyed, Balázs Kubinyi, Enikö Front Genet Genetics Aging is the largest risk factor in many diseases and mortality alike. As the elderly population is expected to increase at an accelerating rate in the future, these phenomena will pose a growing socio-economic burden on societies. To successfully cope with this challenge, a deeper understanding of aging is crucial. In many aspects, the companion dog is an increasingly popular model organism to study aging, with the promise of producing results that are more applicable to humans than the findings that come from the studies of classical model organisms. In this preliminary study we used the whole-genome sequence of two extremely old dogs – age: 22 and 27 years (or 90–135% more, than the average lifespan of dogs) – in order to make the first steps to understand the genetic background of extreme longevity in dogs. We identified more than ∼80 1000 novel SNPs in the two dogs (7500 of which overlapped between them) when compared to three publicly available canine SNP databases, which included SNP information from850 dogs. Most novel mutations (∼52000 SNPs) were identified at non-coding regions, while 4.6% of the remaining SNPs (n∼1600) were at exons, including 670 missense variants – 76 of which overlapped between the two animals – across 472 genes. Based on their gene ontologies, these genes were related – among others – to gene transcription/translation and its regulation, to immune response and the nervous system in general. We also detected 12 loss-of-function mutations, although their actual effect is unclear. Several genetic pathways were also identified, which pathways may be tempting candidates to be investigated in large sample sizes in order to confirm their relevance in extreme longevity in dogs (and possibly, in humans). We hypothesize a possible link between extreme longevity and the regulation of gene transcription/translation, which hypothesis should be further investigated in the future. This phenomenon could define an interesting direction for future research aiming to better understand longevity. The presented preliminary results highlight the utility of the companion dog in the study of the genetic background of longevity and aging. Frontiers Media S.A. 2020-04-16 /pmc/articles/PMC7176982/ /pubmed/32373156 http://dx.doi.org/10.3389/fgene.2020.00315 Text en Copyright © 2020 Jónás, Sándor, Tátrai, Egyed and Kubinyi. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Genetics
Jónás, Dávid
Sándor, Sára
Tátrai, Kitti
Egyed, Balázs
Kubinyi, Enikö
A Preliminary Study to Investigate the Genetic Background of Longevity Based on Whole-Genome Sequence Data of Two Methuselah Dogs
title A Preliminary Study to Investigate the Genetic Background of Longevity Based on Whole-Genome Sequence Data of Two Methuselah Dogs
title_full A Preliminary Study to Investigate the Genetic Background of Longevity Based on Whole-Genome Sequence Data of Two Methuselah Dogs
title_fullStr A Preliminary Study to Investigate the Genetic Background of Longevity Based on Whole-Genome Sequence Data of Two Methuselah Dogs
title_full_unstemmed A Preliminary Study to Investigate the Genetic Background of Longevity Based on Whole-Genome Sequence Data of Two Methuselah Dogs
title_short A Preliminary Study to Investigate the Genetic Background of Longevity Based on Whole-Genome Sequence Data of Two Methuselah Dogs
title_sort preliminary study to investigate the genetic background of longevity based on whole-genome sequence data of two methuselah dogs
topic Genetics
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7176982/
https://www.ncbi.nlm.nih.gov/pubmed/32373156
http://dx.doi.org/10.3389/fgene.2020.00315
work_keys_str_mv AT jonasdavid apreliminarystudytoinvestigatethegeneticbackgroundoflongevitybasedonwholegenomesequencedataoftwomethuselahdogs
AT sandorsara apreliminarystudytoinvestigatethegeneticbackgroundoflongevitybasedonwholegenomesequencedataoftwomethuselahdogs
AT tatraikitti apreliminarystudytoinvestigatethegeneticbackgroundoflongevitybasedonwholegenomesequencedataoftwomethuselahdogs
AT egyedbalazs apreliminarystudytoinvestigatethegeneticbackgroundoflongevitybasedonwholegenomesequencedataoftwomethuselahdogs
AT kubinyieniko apreliminarystudytoinvestigatethegeneticbackgroundoflongevitybasedonwholegenomesequencedataoftwomethuselahdogs
AT jonasdavid preliminarystudytoinvestigatethegeneticbackgroundoflongevitybasedonwholegenomesequencedataoftwomethuselahdogs
AT sandorsara preliminarystudytoinvestigatethegeneticbackgroundoflongevitybasedonwholegenomesequencedataoftwomethuselahdogs
AT tatraikitti preliminarystudytoinvestigatethegeneticbackgroundoflongevitybasedonwholegenomesequencedataoftwomethuselahdogs
AT egyedbalazs preliminarystudytoinvestigatethegeneticbackgroundoflongevitybasedonwholegenomesequencedataoftwomethuselahdogs
AT kubinyieniko preliminarystudytoinvestigatethegeneticbackgroundoflongevitybasedonwholegenomesequencedataoftwomethuselahdogs

Ejemplares similares