A genome‐wide screen identifies genes that suppress the accumulation of spontaneous mutations in young and aged yeast cells

To ensure proper transmission of genetic information, cells need to preserve and faithfully replicate their genome, and failure to do so leads to genome instability, a hallmark of both cancer and aging. Defects in genes involved in guarding genome stability cause several human progeroid syndromes, a...

Descripción completa

Detalles Bibliográficos
Autores principales: Novarina, Daniele, Janssens, Georges E., Bokern, Koen, Schut, Tim, van Oerle, Noor C., Kazemier, Hinke G., Veenhoff, Liesbeth M., Chang, Michael
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2019
Materias:
Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6996960/
https://www.ncbi.nlm.nih.gov/pubmed/31854076
http://dx.doi.org/10.1111/acel.13084
_version_ 1783493599882641408
author Novarina, Daniele
Janssens, Georges E.
Bokern, Koen
Schut, Tim
van Oerle, Noor C.
Kazemier, Hinke G.
Veenhoff, Liesbeth M.
Chang, Michael
author_facet Novarina, Daniele
Janssens, Georges E.
Bokern, Koen
Schut, Tim
van Oerle, Noor C.
Kazemier, Hinke G.
Veenhoff, Liesbeth M.
Chang, Michael
author_sort Novarina, Daniele
collection PubMed
description To ensure proper transmission of genetic information, cells need to preserve and faithfully replicate their genome, and failure to do so leads to genome instability, a hallmark of both cancer and aging. Defects in genes involved in guarding genome stability cause several human progeroid syndromes, and an age‐dependent accumulation of mutations has been observed in different organisms, from yeast to mammals. However, it is unclear whether the spontaneous mutation rate changes during aging and whether specific pathways are important for genome maintenance in old cells. We developed a high‐throughput replica‐pinning approach to screen for genes important to suppress the accumulation of spontaneous mutations during yeast replicative aging. We found 13 known mutation suppression genes, and 31 genes that had no previous link to spontaneous mutagenesis, and all acted independently of age. Importantly, we identified PEX19, encoding an evolutionarily conserved peroxisome biogenesis factor, as an age‐specific mutation suppression gene. While wild‐type and pex19Δ young cells have similar spontaneous mutation rates, aged cells lacking PEX19 display an elevated mutation rate. This finding suggests that functional peroxisomes may be important to preserve genome integrity specifically in old cells.
format Online
Article
Text
id pubmed-6996960
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher John Wiley and Sons Inc.
record_format MEDLINE/PubMed
spelling pubmed-69969602020-02-05 A genome‐wide screen identifies genes that suppress the accumulation of spontaneous mutations in young and aged yeast cells Novarina, Daniele Janssens, Georges E. Bokern, Koen Schut, Tim van Oerle, Noor C. Kazemier, Hinke G. Veenhoff, Liesbeth M. Chang, Michael Aging Cell Original Articles To ensure proper transmission of genetic information, cells need to preserve and faithfully replicate their genome, and failure to do so leads to genome instability, a hallmark of both cancer and aging. Defects in genes involved in guarding genome stability cause several human progeroid syndromes, and an age‐dependent accumulation of mutations has been observed in different organisms, from yeast to mammals. However, it is unclear whether the spontaneous mutation rate changes during aging and whether specific pathways are important for genome maintenance in old cells. We developed a high‐throughput replica‐pinning approach to screen for genes important to suppress the accumulation of spontaneous mutations during yeast replicative aging. We found 13 known mutation suppression genes, and 31 genes that had no previous link to spontaneous mutagenesis, and all acted independently of age. Importantly, we identified PEX19, encoding an evolutionarily conserved peroxisome biogenesis factor, as an age‐specific mutation suppression gene. While wild‐type and pex19Δ young cells have similar spontaneous mutation rates, aged cells lacking PEX19 display an elevated mutation rate. This finding suggests that functional peroxisomes may be important to preserve genome integrity specifically in old cells. John Wiley and Sons Inc. 2019-12-18 2020-02 /pmc/articles/PMC6996960/ /pubmed/31854076 http://dx.doi.org/10.1111/acel.13084 Text en © 2019 The Authors. Aging Cell published by Anatomical Society and John Wiley & Sons Ltd This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Articles
Novarina, Daniele
Janssens, Georges E.
Bokern, Koen
Schut, Tim
van Oerle, Noor C.
Kazemier, Hinke G.
Veenhoff, Liesbeth M.
Chang, Michael
A genome‐wide screen identifies genes that suppress the accumulation of spontaneous mutations in young and aged yeast cells
title A genome‐wide screen identifies genes that suppress the accumulation of spontaneous mutations in young and aged yeast cells
title_full A genome‐wide screen identifies genes that suppress the accumulation of spontaneous mutations in young and aged yeast cells
title_fullStr A genome‐wide screen identifies genes that suppress the accumulation of spontaneous mutations in young and aged yeast cells
title_full_unstemmed A genome‐wide screen identifies genes that suppress the accumulation of spontaneous mutations in young and aged yeast cells
title_short A genome‐wide screen identifies genes that suppress the accumulation of spontaneous mutations in young and aged yeast cells
title_sort genome‐wide screen identifies genes that suppress the accumulation of spontaneous mutations in young and aged yeast cells
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6996960/
https://www.ncbi.nlm.nih.gov/pubmed/31854076
http://dx.doi.org/10.1111/acel.13084
work_keys_str_mv AT novarinadaniele agenomewidescreenidentifiesgenesthatsuppresstheaccumulationofspontaneousmutationsinyoungandagedyeastcells
AT janssensgeorgese agenomewidescreenidentifiesgenesthatsuppresstheaccumulationofspontaneousmutationsinyoungandagedyeastcells
AT bokernkoen agenomewidescreenidentifiesgenesthatsuppresstheaccumulationofspontaneousmutationsinyoungandagedyeastcells
AT schuttim agenomewidescreenidentifiesgenesthatsuppresstheaccumulationofspontaneousmutationsinyoungandagedyeastcells
AT vanoerlenoorc agenomewidescreenidentifiesgenesthatsuppresstheaccumulationofspontaneousmutationsinyoungandagedyeastcells
AT kazemierhinkeg agenomewidescreenidentifiesgenesthatsuppresstheaccumulationofspontaneousmutationsinyoungandagedyeastcells
AT veenhoffliesbethm agenomewidescreenidentifiesgenesthatsuppresstheaccumulationofspontaneousmutationsinyoungandagedyeastcells
AT changmichael agenomewidescreenidentifiesgenesthatsuppresstheaccumulationofspontaneousmutationsinyoungandagedyeastcells
AT novarinadaniele genomewidescreenidentifiesgenesthatsuppresstheaccumulationofspontaneousmutationsinyoungandagedyeastcells
AT janssensgeorgese genomewidescreenidentifiesgenesthatsuppresstheaccumulationofspontaneousmutationsinyoungandagedyeastcells
AT bokernkoen genomewidescreenidentifiesgenesthatsuppresstheaccumulationofspontaneousmutationsinyoungandagedyeastcells
AT schuttim genomewidescreenidentifiesgenesthatsuppresstheaccumulationofspontaneousmutationsinyoungandagedyeastcells
AT vanoerlenoorc genomewidescreenidentifiesgenesthatsuppresstheaccumulationofspontaneousmutationsinyoungandagedyeastcells
AT kazemierhinkeg genomewidescreenidentifiesgenesthatsuppresstheaccumulationofspontaneousmutationsinyoungandagedyeastcells
AT veenhoffliesbethm genomewidescreenidentifiesgenesthatsuppresstheaccumulationofspontaneousmutationsinyoungandagedyeastcells
AT changmichael genomewidescreenidentifiesgenesthatsuppresstheaccumulationofspontaneousmutationsinyoungandagedyeastcells

Ejemplares similares