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Interconverting Conformations of Slipped-DNA Junctions Formed by Trinucleotide Repeats Affect Repair Outcome

[Image: see text] Expansions of (CTG)·(CAG) repeated DNAs are the mutagenic cause of 14 neurological diseases, likely arising through the formation and processing of slipped-strand DNAs. These transient intermediates of repeat length mutations are formed by out-of-register mispairing of repeat units...

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Autores principales: Slean, Meghan M., Reddy, Kaalak, Wu, Bin, Nichol Edamura, Kerrie, Kekis, Mariana, Nelissen, Frank H. T., Aspers, Ruud L. E. G., Tessari, Marco, Schärer, Orlando D., Wijmenga, Sybren S., Pearson, Christopher E.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Chemical Society 2013
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3566650/
https://www.ncbi.nlm.nih.gov/pubmed/23339280
http://dx.doi.org/10.1021/bi301369b
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author Slean, Meghan M.
Reddy, Kaalak
Wu, Bin
Nichol Edamura, Kerrie
Kekis, Mariana
Nelissen, Frank H. T.
Aspers, Ruud L. E. G.
Tessari, Marco
Schärer, Orlando D.
Wijmenga, Sybren S.
Pearson, Christopher E.
author_facet Slean, Meghan M.
Reddy, Kaalak
Wu, Bin
Nichol Edamura, Kerrie
Kekis, Mariana
Nelissen, Frank H. T.
Aspers, Ruud L. E. G.
Tessari, Marco
Schärer, Orlando D.
Wijmenga, Sybren S.
Pearson, Christopher E.
author_sort Slean, Meghan M.
collection PubMed
description [Image: see text] Expansions of (CTG)·(CAG) repeated DNAs are the mutagenic cause of 14 neurological diseases, likely arising through the formation and processing of slipped-strand DNAs. These transient intermediates of repeat length mutations are formed by out-of-register mispairing of repeat units on complementary strands. The three-way slipped-DNA junction, at which the excess repeats slip out from the duplex, is a poorly understood feature common to these mutagenic intermediates. Here, we reveal that slipped junctions can assume a surprising number of interconverting conformations where the strand opposite the slip-out either is fully base paired or has one or two unpaired nucleotides. These unpaired nucleotides can also arise opposite either of the nonslipped junction arms. Junction conformation can affect binding by various structure-specific DNA repair proteins and can also alter correct nick-directed repair levels. Junctions that have the potential to contain unpaired nucleotides are repaired with a significantly higher efficiency than constrained fully paired junctions. Surprisingly, certain junction conformations are aberrantly repaired to expansion mutations: misdirection of repair to the non-nicked strand opposite the slip-out leads to integration of the excess slipped-out repeats rather than their excision. Thus, slipped-junction structure can determine whether repair attempts lead to correction or expansion mutations.
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spelling pubmed-35666502013-02-08 Interconverting Conformations of Slipped-DNA Junctions Formed by Trinucleotide Repeats Affect Repair Outcome Slean, Meghan M. Reddy, Kaalak Wu, Bin Nichol Edamura, Kerrie Kekis, Mariana Nelissen, Frank H. T. Aspers, Ruud L. E. G. Tessari, Marco Schärer, Orlando D. Wijmenga, Sybren S. Pearson, Christopher E. Biochemistry [Image: see text] Expansions of (CTG)·(CAG) repeated DNAs are the mutagenic cause of 14 neurological diseases, likely arising through the formation and processing of slipped-strand DNAs. These transient intermediates of repeat length mutations are formed by out-of-register mispairing of repeat units on complementary strands. The three-way slipped-DNA junction, at which the excess repeats slip out from the duplex, is a poorly understood feature common to these mutagenic intermediates. Here, we reveal that slipped junctions can assume a surprising number of interconverting conformations where the strand opposite the slip-out either is fully base paired or has one or two unpaired nucleotides. These unpaired nucleotides can also arise opposite either of the nonslipped junction arms. Junction conformation can affect binding by various structure-specific DNA repair proteins and can also alter correct nick-directed repair levels. Junctions that have the potential to contain unpaired nucleotides are repaired with a significantly higher efficiency than constrained fully paired junctions. Surprisingly, certain junction conformations are aberrantly repaired to expansion mutations: misdirection of repair to the non-nicked strand opposite the slip-out leads to integration of the excess slipped-out repeats rather than their excision. Thus, slipped-junction structure can determine whether repair attempts lead to correction or expansion mutations. American Chemical Society 2013-01-22 2013-02-05 /pmc/articles/PMC3566650/ /pubmed/23339280 http://dx.doi.org/10.1021/bi301369b Text en Copyright © 2013 American Chemical Society http://pubs.acs.org This is an open-access article distributed under the ACS AuthorChoice Terms & Conditions. Any use of this article, must conform to the terms of that license which are available at http://pubs.acs.org.
spellingShingle Slean, Meghan M.
Reddy, Kaalak
Wu, Bin
Nichol Edamura, Kerrie
Kekis, Mariana
Nelissen, Frank H. T.
Aspers, Ruud L. E. G.
Tessari, Marco
Schärer, Orlando D.
Wijmenga, Sybren S.
Pearson, Christopher E.
Interconverting Conformations of Slipped-DNA Junctions Formed by Trinucleotide Repeats Affect Repair Outcome
title Interconverting Conformations of Slipped-DNA Junctions Formed by Trinucleotide Repeats Affect Repair Outcome
title_full Interconverting Conformations of Slipped-DNA Junctions Formed by Trinucleotide Repeats Affect Repair Outcome
title_fullStr Interconverting Conformations of Slipped-DNA Junctions Formed by Trinucleotide Repeats Affect Repair Outcome
title_full_unstemmed Interconverting Conformations of Slipped-DNA Junctions Formed by Trinucleotide Repeats Affect Repair Outcome
title_short Interconverting Conformations of Slipped-DNA Junctions Formed by Trinucleotide Repeats Affect Repair Outcome
title_sort interconverting conformations of slipped-dna junctions formed by trinucleotide repeats affect repair outcome
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3566650/
https://www.ncbi.nlm.nih.gov/pubmed/23339280
http://dx.doi.org/10.1021/bi301369b
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