DNA polymerase stalling at structured DNA constrains the expansion of short tandem repeats

DNA polymerase stalling at structured DNA constrains the expansion of short tandem repeats

Abstract Background Short tandem repeats (STRs) contribute significantly to de novo mutagenesis, driving phenotypic diversity and genetic disease. Although highly diverse, their repetitive sequences induce DNA polymerase slippage and stalling, leading to length and sequence variation. However, curre...

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Bibliographic Details
Main Authors: Pierre Murat, Guillaume Guilbaud, Julian E. Sale
Format: Article
Language:English
Published: BMC 2020-08-01
Series:Genome Biology
Subjects:
Short tandem repeat
DNA secondary structure
Polymerase stalling
Genome instability
Genome evolution
Online Access:http://link.springer.com/article/10.1186/s13059-020-02124-x
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spelling doaj-309d32f111bb43d0b8ebe7ee1237d1502020-11-25T02:58:47ZengBMCGenome Biology1474-760X2020-08-0121112610.1186/s13059-020-02124-xDNA polymerase stalling at structured DNA constrains the expansion of short tandem repeatsPierre Murat0Guillaume Guilbaud1Julian E. Sale2MRC Laboratory of Molecular BiologyMRC Laboratory of Molecular BiologyMRC Laboratory of Molecular BiologyAbstract Background Short tandem repeats (STRs) contribute significantly to de novo mutagenesis, driving phenotypic diversity and genetic disease. Although highly diverse, their repetitive sequences induce DNA polymerase slippage and stalling, leading to length and sequence variation. However, current studies of DNA synthesis through STRs are restricted to a handful of selected sequences, limiting our broader understanding of their evolutionary behaviour and hampering the characterisation of the determinants of their abundance and stability in eukaryotic genomes. Results We perform a comprehensive analysis of DNA synthesis at all STR permutations and interrogate the impact of STR sequence and secondary structure on their genomic representation and mutability. To do this, we developed a high-throughput primer extension assay that allows monitoring of the kinetics and fidelity of DNA synthesis through 20,000 sequences comprising all STR permutations in different lengths. By combining these measurements with population-scale genomic data, we show that the response of a model replicative DNA polymerase to variously structured DNA is sufficient to predict the complex genomic behaviour of STRs, including abundance and mutational constraints. We demonstrate that DNA polymerase stalling at DNA structures induces error-prone DNA synthesis, which constrains STR expansion. Conclusions Our data support a model in which STR length in eukaryotic genomes results from a balance between expansion due to polymerase slippage at repeated DNA sequences and point mutations caused by error-prone DNA synthesis at DNA structures.http://link.springer.com/article/10.1186/s13059-020-02124-xShort tandem repeatDNA secondary structurePolymerase stallingGenome instabilityGenome evolution
collection DOAJ
language English
format Article
sources DOAJ
author Pierre Murat
Guillaume Guilbaud
Julian E. Sale
spellingShingle Pierre Murat
Guillaume Guilbaud
Julian E. Sale
DNA polymerase stalling at structured DNA constrains the expansion of short tandem repeats
Genome Biology
Short tandem repeat
DNA secondary structure
Polymerase stalling
Genome instability
Genome evolution
author_facet Pierre Murat
Guillaume Guilbaud
Julian E. Sale
author_sort Pierre Murat
title DNA polymerase stalling at structured DNA constrains the expansion of short tandem repeats
title_short DNA polymerase stalling at structured DNA constrains the expansion of short tandem repeats
title_full DNA polymerase stalling at structured DNA constrains the expansion of short tandem repeats
title_fullStr DNA polymerase stalling at structured DNA constrains the expansion of short tandem repeats
title_full_unstemmed DNA polymerase stalling at structured DNA constrains the expansion of short tandem repeats
title_sort dna polymerase stalling at structured dna constrains the expansion of short tandem repeats
publisher BMC
series Genome Biology
issn 1474-760X
publishDate 2020-08-01
description Abstract Background Short tandem repeats (STRs) contribute significantly to de novo mutagenesis, driving phenotypic diversity and genetic disease. Although highly diverse, their repetitive sequences induce DNA polymerase slippage and stalling, leading to length and sequence variation. However, current studies of DNA synthesis through STRs are restricted to a handful of selected sequences, limiting our broader understanding of their evolutionary behaviour and hampering the characterisation of the determinants of their abundance and stability in eukaryotic genomes. Results We perform a comprehensive analysis of DNA synthesis at all STR permutations and interrogate the impact of STR sequence and secondary structure on their genomic representation and mutability. To do this, we developed a high-throughput primer extension assay that allows monitoring of the kinetics and fidelity of DNA synthesis through 20,000 sequences comprising all STR permutations in different lengths. By combining these measurements with population-scale genomic data, we show that the response of a model replicative DNA polymerase to variously structured DNA is sufficient to predict the complex genomic behaviour of STRs, including abundance and mutational constraints. We demonstrate that DNA polymerase stalling at DNA structures induces error-prone DNA synthesis, which constrains STR expansion. Conclusions Our data support a model in which STR length in eukaryotic genomes results from a balance between expansion due to polymerase slippage at repeated DNA sequences and point mutations caused by error-prone DNA synthesis at DNA structures.
topic Short tandem repeat
DNA secondary structure
Polymerase stalling
Genome instability
Genome evolution
url http://link.springer.com/article/10.1186/s13059-020-02124-x
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AT julianesale dnapolymerasestallingatstructureddnaconstrainstheexpansionofshorttandemrepeats
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