Defects in the GINS complex increase the instability of repetitive sequences via a recombination-dependent mechanism.

Defects in the GINS complex increase the instability of repetitive sequences via a recombination-dependent mechanism.

Faithful replication and repair of DNA lesions ensure genome maintenance. During replication in eukaryotic cells, DNA is unwound by the CMG helicase complex, which is composed of three major components: the Cdc45 protein, Mcm2-7, and the GINS complex. The CMG in complex with DNA polymerase epsilon (...

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Main Authors: Malgorzata Jedrychowska, Milena Denkiewicz-Kruk, Malgorzata Alabrudzinska, Adrianna Skoneczna, Piotr Jonczyk, Michal Dmowski, Iwona J Fijalkowska
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2019-12-01
Series:PLoS Genetics
Online Access:https://doi.org/10.1371/journal.pgen.1008494
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spelling doaj-4e4502278d9841618e31147cc67f253b2021-04-21T13:47:46ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042019-12-011512e100849410.1371/journal.pgen.1008494Defects in the GINS complex increase the instability of repetitive sequences via a recombination-dependent mechanism.Malgorzata JedrychowskaMilena Denkiewicz-KrukMalgorzata AlabrudzinskaAdrianna SkonecznaPiotr JonczykMichal DmowskiIwona J FijalkowskaFaithful replication and repair of DNA lesions ensure genome maintenance. During replication in eukaryotic cells, DNA is unwound by the CMG helicase complex, which is composed of three major components: the Cdc45 protein, Mcm2-7, and the GINS complex. The CMG in complex with DNA polymerase epsilon (CMG-E) participates in the establishment and progression of the replisome. Impaired functioning of the CMG-E was shown to induce genomic instability and promote the development of various diseases. Therefore, CMG-E components play important roles as caretakers of the genome. In Saccharomyces cerevisiae, the GINS complex is composed of the Psf1, Psf2, Psf3, and Sld5 essential subunits. The Psf1-1 mutant form fails to interact with Psf3, resulting in impaired replisome assembly and chromosome replication. Here, we show increased instability of repeat tracts (mononucleotide, dinucleotide, trinucleotide and longer) in yeast psf1-1 mutants. To identify the mechanisms underlying this effect, we analyzed repeated sequence instability using derivatives of psf1-1 strains lacking genes involved in translesion synthesis, recombination, or mismatch repair. Among these derivatives, deletion of RAD52, RAD51, MMS2, POL32, or PIF1 significantly decreased DNA repeat instability. These results, together with the observed increased amounts of single-stranded DNA regions and Rfa1 foci suggest that recombinational mechanisms make important contributions to repeat tract instability in psf1-1 cells. We propose that defective functioning of the CMG-E complex in psf1-1 cells impairs the progression of DNA replication what increases the contribution of repair mechanisms such as template switch and break-induced replication. These processes require sequence homology search which in case of a repeated DNA tract may result in misalignment leading to its expansion or contraction.https://doi.org/10.1371/journal.pgen.1008494
collection DOAJ
language English
format Article
sources DOAJ
author Malgorzata Jedrychowska
Milena Denkiewicz-Kruk
Malgorzata Alabrudzinska
Adrianna Skoneczna
Piotr Jonczyk
Michal Dmowski
Iwona J Fijalkowska
spellingShingle Malgorzata Jedrychowska
Milena Denkiewicz-Kruk
Malgorzata Alabrudzinska
Adrianna Skoneczna
Piotr Jonczyk
Michal Dmowski
Iwona J Fijalkowska
Defects in the GINS complex increase the instability of repetitive sequences via a recombination-dependent mechanism.
PLoS Genetics
author_facet Malgorzata Jedrychowska
Milena Denkiewicz-Kruk
Malgorzata Alabrudzinska
Adrianna Skoneczna
Piotr Jonczyk
Michal Dmowski
Iwona J Fijalkowska
author_sort Malgorzata Jedrychowska
title Defects in the GINS complex increase the instability of repetitive sequences via a recombination-dependent mechanism.
title_short Defects in the GINS complex increase the instability of repetitive sequences via a recombination-dependent mechanism.
title_full Defects in the GINS complex increase the instability of repetitive sequences via a recombination-dependent mechanism.
title_fullStr Defects in the GINS complex increase the instability of repetitive sequences via a recombination-dependent mechanism.
title_full_unstemmed Defects in the GINS complex increase the instability of repetitive sequences via a recombination-dependent mechanism.
title_sort defects in the gins complex increase the instability of repetitive sequences via a recombination-dependent mechanism.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2019-12-01
description Faithful replication and repair of DNA lesions ensure genome maintenance. During replication in eukaryotic cells, DNA is unwound by the CMG helicase complex, which is composed of three major components: the Cdc45 protein, Mcm2-7, and the GINS complex. The CMG in complex with DNA polymerase epsilon (CMG-E) participates in the establishment and progression of the replisome. Impaired functioning of the CMG-E was shown to induce genomic instability and promote the development of various diseases. Therefore, CMG-E components play important roles as caretakers of the genome. In Saccharomyces cerevisiae, the GINS complex is composed of the Psf1, Psf2, Psf3, and Sld5 essential subunits. The Psf1-1 mutant form fails to interact with Psf3, resulting in impaired replisome assembly and chromosome replication. Here, we show increased instability of repeat tracts (mononucleotide, dinucleotide, trinucleotide and longer) in yeast psf1-1 mutants. To identify the mechanisms underlying this effect, we analyzed repeated sequence instability using derivatives of psf1-1 strains lacking genes involved in translesion synthesis, recombination, or mismatch repair. Among these derivatives, deletion of RAD52, RAD51, MMS2, POL32, or PIF1 significantly decreased DNA repeat instability. These results, together with the observed increased amounts of single-stranded DNA regions and Rfa1 foci suggest that recombinational mechanisms make important contributions to repeat tract instability in psf1-1 cells. We propose that defective functioning of the CMG-E complex in psf1-1 cells impairs the progression of DNA replication what increases the contribution of repair mechanisms such as template switch and break-induced replication. These processes require sequence homology search which in case of a repeated DNA tract may result in misalignment leading to its expansion or contraction.
url https://doi.org/10.1371/journal.pgen.1008494
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