Coordination of Rad1–Rad10 interactions with Msh2–Msh3, Saw1 and RPA is essential for functional 3′ non-homologous tail removal

Double strand DNA break repair (DSBR) comprises multiple pathways. A subset of DSBR pathways, including single strand annealing, involve intermediates with 3′ non-homologous tails that must be removed to complete repair. In Saccharomyces cerevisiae, Rad1–Rad10 is the structure-specific endonuclease...

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Autores principales: Eichmiller, Robin, Medina-Rivera, Melisa, DeSanto, Rachel, Minca, Eugen, Kim, Christopher, Holland, Cory, Seol, Ja-Hwan, Schmit, Megan, Oramus, Diane, Smith, Jessica, Gallardo, Ignacio F, Finkelstein, Ilya J, Lee, Sang Eun, Surtees, Jennifer A
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2018
Materias:
Genome Integrity, Repair and Replication
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6007489/
https://www.ncbi.nlm.nih.gov/pubmed/29660012
http://dx.doi.org/10.1093/nar/gky254
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author Eichmiller, Robin
Medina-Rivera, Melisa
DeSanto, Rachel
Minca, Eugen
Kim, Christopher
Holland, Cory
Seol, Ja-Hwan
Schmit, Megan
Oramus, Diane
Smith, Jessica
Gallardo, Ignacio F
Finkelstein, Ilya J
Lee, Sang Eun
Surtees, Jennifer A
author_facet Eichmiller, Robin
Medina-Rivera, Melisa
DeSanto, Rachel
Minca, Eugen
Kim, Christopher
Holland, Cory
Seol, Ja-Hwan
Schmit, Megan
Oramus, Diane
Smith, Jessica
Gallardo, Ignacio F
Finkelstein, Ilya J
Lee, Sang Eun
Surtees, Jennifer A
author_sort Eichmiller, Robin
collection PubMed
description Double strand DNA break repair (DSBR) comprises multiple pathways. A subset of DSBR pathways, including single strand annealing, involve intermediates with 3′ non-homologous tails that must be removed to complete repair. In Saccharomyces cerevisiae, Rad1–Rad10 is the structure-specific endonuclease that cleaves the tails in 3′ non-homologous tail removal (3′ NHTR). Rad1–Rad10 is also an essential component of the nucleotide excision repair (NER) pathway. In both cases, Rad1–Rad10 requires protein partners for recruitment to the relevant DNA intermediate. Msh2–Msh3 and Saw1 recruit Rad1–Rad10 in 3′ NHTR; Rad14 recruits Rad1–Rad10 in NER. We created two rad1 separation-of-function alleles, rad1R203A,K205A and rad1R218A; both are defective in 3′ NHTR but functional in NER. In vitro, rad1R203A,K205A was impaired at multiple steps in 3′ NHTR. The rad1R218A in vivo phenotype resembles that of msh2- or msh3-deleted cells; recruitment of rad1R218A–Rad10 to recombination intermediates is defective. Interactions among rad1R218A–Rad10 and Msh2–Msh3 and Saw1 are altered and rad1R218A–Rad10 interactions with RPA are compromised. We propose a model in which Rad1–Rad10 is recruited and positioned at the recombination intermediate through interactions, between Saw1 and DNA, Rad1–Rad10 and Msh2–Msh3, Saw1 and Msh2–Msh3 and Rad1–Rad10 and RPA. When any of these interactions is altered, 3′ NHTR is impaired.
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spelling pubmed-60074892018-07-05 Coordination of Rad1–Rad10 interactions with Msh2–Msh3, Saw1 and RPA is essential for functional 3′ non-homologous tail removal Eichmiller, Robin Medina-Rivera, Melisa DeSanto, Rachel Minca, Eugen Kim, Christopher Holland, Cory Seol, Ja-Hwan Schmit, Megan Oramus, Diane Smith, Jessica Gallardo, Ignacio F Finkelstein, Ilya J Lee, Sang Eun Surtees, Jennifer A Nucleic Acids Res Genome Integrity, Repair and Replication Double strand DNA break repair (DSBR) comprises multiple pathways. A subset of DSBR pathways, including single strand annealing, involve intermediates with 3′ non-homologous tails that must be removed to complete repair. In Saccharomyces cerevisiae, Rad1–Rad10 is the structure-specific endonuclease that cleaves the tails in 3′ non-homologous tail removal (3′ NHTR). Rad1–Rad10 is also an essential component of the nucleotide excision repair (NER) pathway. In both cases, Rad1–Rad10 requires protein partners for recruitment to the relevant DNA intermediate. Msh2–Msh3 and Saw1 recruit Rad1–Rad10 in 3′ NHTR; Rad14 recruits Rad1–Rad10 in NER. We created two rad1 separation-of-function alleles, rad1R203A,K205A and rad1R218A; both are defective in 3′ NHTR but functional in NER. In vitro, rad1R203A,K205A was impaired at multiple steps in 3′ NHTR. The rad1R218A in vivo phenotype resembles that of msh2- or msh3-deleted cells; recruitment of rad1R218A–Rad10 to recombination intermediates is defective. Interactions among rad1R218A–Rad10 and Msh2–Msh3 and Saw1 are altered and rad1R218A–Rad10 interactions with RPA are compromised. We propose a model in which Rad1–Rad10 is recruited and positioned at the recombination intermediate through interactions, between Saw1 and DNA, Rad1–Rad10 and Msh2–Msh3, Saw1 and Msh2–Msh3 and Rad1–Rad10 and RPA. When any of these interactions is altered, 3′ NHTR is impaired. Oxford University Press 2018-06-01 2018-04-06 /pmc/articles/PMC6007489/ /pubmed/29660012 http://dx.doi.org/10.1093/nar/gky254 Text en © The Author(s) 2018. Published by Oxford University Press on behalf of Nucleic Acids Research. http://creativecommons.org/licenses/by-nc/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License (http://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Genome Integrity, Repair and Replication
Eichmiller, Robin
Medina-Rivera, Melisa
DeSanto, Rachel
Minca, Eugen
Kim, Christopher
Holland, Cory
Seol, Ja-Hwan
Schmit, Megan
Oramus, Diane
Smith, Jessica
Gallardo, Ignacio F
Finkelstein, Ilya J
Lee, Sang Eun
Surtees, Jennifer A
Coordination of Rad1–Rad10 interactions with Msh2–Msh3, Saw1 and RPA is essential for functional 3′ non-homologous tail removal
title Coordination of Rad1–Rad10 interactions with Msh2–Msh3, Saw1 and RPA is essential for functional 3′ non-homologous tail removal
title_full Coordination of Rad1–Rad10 interactions with Msh2–Msh3, Saw1 and RPA is essential for functional 3′ non-homologous tail removal
title_fullStr Coordination of Rad1–Rad10 interactions with Msh2–Msh3, Saw1 and RPA is essential for functional 3′ non-homologous tail removal
title_full_unstemmed Coordination of Rad1–Rad10 interactions with Msh2–Msh3, Saw1 and RPA is essential for functional 3′ non-homologous tail removal
title_short Coordination of Rad1–Rad10 interactions with Msh2–Msh3, Saw1 and RPA is essential for functional 3′ non-homologous tail removal
title_sort coordination of rad1–rad10 interactions with msh2–msh3, saw1 and rpa is essential for functional 3′ non-homologous tail removal
topic Genome Integrity, Repair and Replication
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6007489/
https://www.ncbi.nlm.nih.gov/pubmed/29660012
http://dx.doi.org/10.1093/nar/gky254
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