Loss of Cdc13 causes genome instability by a deficiency in replication-dependent telomere capping.

Loss of Cdc13 causes genome instability by a deficiency in replication-dependent telomere capping.

In budding yeast, Cdc13, Stn1, and Ten1 form the telomere-binding heterotrimer CST complex. Here we investigate the role of Cdc13/CST in maintaining genome stability by using a Chr VII disome system that can generate recombinants, chromosome loss, and enigmatic unstable chromosomes. In cells express...

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Main Authors: Rachel E Langston, Dominic Palazzola, Erin Bonnell, Raymund J Wellinger, Ted Weinert
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2020-04-01
Series:PLoS Genetics
Online Access:https://doi.org/10.1371/journal.pgen.1008733
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spelling doaj-086e256930e04d55be311ba70fa6f8462021-04-21T13:52:38ZengPublic Library of Science (PLoS)PLoS Genetics1553-73901553-74042020-04-01164e100873310.1371/journal.pgen.1008733Loss of Cdc13 causes genome instability by a deficiency in replication-dependent telomere capping.Rachel E LangstonDominic PalazzolaErin BonnellRaymund J WellingerTed WeinertIn budding yeast, Cdc13, Stn1, and Ten1 form the telomere-binding heterotrimer CST complex. Here we investigate the role of Cdc13/CST in maintaining genome stability by using a Chr VII disome system that can generate recombinants, chromosome loss, and enigmatic unstable chromosomes. In cells expressing a temperature sensitive CDC13 allele, cdc13F684S, unstable chromosomes frequently arise from problems in or near a telomere. We found that, when Cdc13 is defective, passage through S phase causes Exo1-dependent ssDNA and unstable chromosomes that are then the source for additional chromosome instability events (e.g. recombinants, chromosome truncations, dicentrics, and/or chromosome loss). We observed that genome instability arises from a defect in Cdc13's function during DNA replication, not Cdc13's putative post-replication telomere capping function. The molecular nature of the initial unstable chromosomes formed by a Cdc13-defect involves ssDNA and does not involve homologous recombination nor non-homologous end joining; we speculate the original unstable chromosome may be a one-ended double strand break. This system defines a link between Cdc13's function during DNA replication and genome stability in the form of unstable chromosomes, that then progress to form other chromosome changes.https://doi.org/10.1371/journal.pgen.1008733
collection DOAJ
language English
format Article
sources DOAJ
author Rachel E Langston
Dominic Palazzola
Erin Bonnell
Raymund J Wellinger
Ted Weinert
spellingShingle Rachel E Langston
Dominic Palazzola
Erin Bonnell
Raymund J Wellinger
Ted Weinert
Loss of Cdc13 causes genome instability by a deficiency in replication-dependent telomere capping.
PLoS Genetics
author_facet Rachel E Langston
Dominic Palazzola
Erin Bonnell
Raymund J Wellinger
Ted Weinert
author_sort Rachel E Langston
title Loss of Cdc13 causes genome instability by a deficiency in replication-dependent telomere capping.
title_short Loss of Cdc13 causes genome instability by a deficiency in replication-dependent telomere capping.
title_full Loss of Cdc13 causes genome instability by a deficiency in replication-dependent telomere capping.
title_fullStr Loss of Cdc13 causes genome instability by a deficiency in replication-dependent telomere capping.
title_full_unstemmed Loss of Cdc13 causes genome instability by a deficiency in replication-dependent telomere capping.
title_sort loss of cdc13 causes genome instability by a deficiency in replication-dependent telomere capping.
publisher Public Library of Science (PLoS)
series PLoS Genetics
issn 1553-7390
1553-7404
publishDate 2020-04-01
description In budding yeast, Cdc13, Stn1, and Ten1 form the telomere-binding heterotrimer CST complex. Here we investigate the role of Cdc13/CST in maintaining genome stability by using a Chr VII disome system that can generate recombinants, chromosome loss, and enigmatic unstable chromosomes. In cells expressing a temperature sensitive CDC13 allele, cdc13F684S, unstable chromosomes frequently arise from problems in or near a telomere. We found that, when Cdc13 is defective, passage through S phase causes Exo1-dependent ssDNA and unstable chromosomes that are then the source for additional chromosome instability events (e.g. recombinants, chromosome truncations, dicentrics, and/or chromosome loss). We observed that genome instability arises from a defect in Cdc13's function during DNA replication, not Cdc13's putative post-replication telomere capping function. The molecular nature of the initial unstable chromosomes formed by a Cdc13-defect involves ssDNA and does not involve homologous recombination nor non-homologous end joining; we speculate the original unstable chromosome may be a one-ended double strand break. This system defines a link between Cdc13's function during DNA replication and genome stability in the form of unstable chromosomes, that then progress to form other chromosome changes.
url https://doi.org/10.1371/journal.pgen.1008733
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