Precarious maintenance of simple DNA repeats in eukaryotes

Neil, Alexander J.; Kim, Jane C.; Mirkin, Sergei M.

doi:10.1002/bies.201700077

Cited by 32 publications

(38 citation statements)

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“…tract) (Usdin et al 2015;Neil et al 2017;Polleys et al 2017;Polyzos and McMurray 2017). We and others have also shown that trinucleotide repeat can induce mutagenesis at a distance (RIM-repeat induced mutagenesis) and trigger CGRs (Shah et al 2012;Saini et al 2013;Tang et al 2013).…”

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confidence: 85%

Nanopore sequencing of complex genomic rearrangements in yeast reveals mechanisms of repeat-mediated double-strand break repair

et al. 2017

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Improper DNA double-strand break (DSB) repair results in complex genomic rearrangements (CGRs) in many cancers and various congenital disorders in humans. Trinucleotide repeat sequences, such as (GAA)n repeats in Friedreich's ataxia, (CTG)n repeats in myotonic dystrophy, and (CGG)n repeats in fragile X syndrome, are also subject to double-strand breaks within the repetitive tract followed by DNA repair. Mapping the outcomes of CGRs is important for understanding their causes and potential phenotypic effects. However, high-resolution mapping of CGRs has traditionally been a laborious and highly skilled process. Recent advances in long-read DNA sequencing technologies, specifically Nanopore sequencing, have made possible the rapid identification of CGRs with single base pair resolution. Here, we have used whole-genome Nanopore sequencing to characterize several CGRs that originated from naturally occurring DSBs at (GAA)n microsatellites in Saccharomyces cerevisiae. These data gave us important insights into the mechanisms of DSB repair leading to CGRs.

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confidence: 85%

Nanopore sequencing of complex genomic rearrangements in yeast reveals mechanisms of repeat-mediated double-strand break repair

et al. 2017

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“…Recent literature has suggested that DSB may be responsible for large scale expansion in nondividing cells providing a potential mechanism for modification of repeat length and phenotypic variability [90,91]. DSB repair have two major repair pathways: homologous recombination repair (HRR) and nonhomologous end joining (NHEJ) [92].…”

Section: Double-strand Dna Repairmentioning

confidence: 99%

“…While mature postmitotic neurones in G0/G1 rely upon error prone NHEJ, break-induced replication (BIR) of homologous recombination can cause large-scale expansion in a CAG tract repeat cellular model in vitro [31,91]. Importantly, BIR may also occur in nondividing neurons and drive disease progression [91]. BIR is then initiated when a one-ended DSB undergoes 5 0 strand resection followed by invasion into a homologous sequence.…”

Section: Double-strand Dna Repairmentioning

confidence: 99%

“…Homologous recombination uses a sister chromatid as a template to repair a DSB, whereas NHEJ ligates together the two DNA ends with little or no processing [43,46]. While mature postmitotic neurones in G0/G1 rely upon error prone NHEJ, break-induced replication (BIR) of homologous recombination can cause large-scale expansion in a CAG tract repeat cellular model in vitro [31,91]. The TNR expansion occurs during fork stalling resulting from hairpin formation on the single-stranded DNA template.…”

Section: Double-strand Dna Repairmentioning

confidence: 99%

“…This newly invaded strand containing the repetitive tract then serves as a primer for DNA synthesis using DNA polymerase delta (Pold). Importantly, BIR may also occur in nondividing neurons and drive disease progression [91]. A number of autosomal recessive ataxias are driven by genetic mutations in DSB repair genes involved in homologous recombination.…”

Section: Double-strand Dna Repairmentioning

confidence: 99%

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DNA repair in trinucleotide repeat ataxias

et al. 2018

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The inherited cerebellar ataxias comprise of a genetic heterogeneous group of disorders. Pathogenic expansions of cytosine-adenine-guanine (CAG) encoding polyglutamine tracts account for the largest proportion of autosomal dominant cerebellar ataxias, while GAA expansion in the first introns of frataxin gene is the commonest cause of autosomal recessive cerebellar ataxias. Currently, there is no available treatment to alter the disease trajectory, with devastating consequences for affected individuals. Inter- and Intrafamily phenotypic variability suggest the existence of genetic modifiers, which may become targets amendable to treatment. Recent studies have demonstrated the importance of DNA repair pathways in modifying spinocerebellar ataxia with CAG repeat expansions. In this review, we discuss the mechanisms in which DNA repair pathways, epigenetics and other genetic factors may act as modifiers in cerebellar ataxias due to trinucleotide repeat expansions.

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Trinucleotide repeat instability during double-strand break repair: from mechanisms to gene therapy

2018

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Trinucleotide repeats are a particular class of microsatellites whose large expansions are responsible for at least two dozen human neurological and developmental disorders. Slippage of the two complementary DNA strands during replication, homologous recombination or DNA repair is generally accepted as a mechanism leading to repeat length changes, creating expansions and contractions of the repeat tract. The present review focuses on recent developments on double-strand break repair involving trinucleotide repeat tracts. Experimental evidences in model organisms show that gene conversion and break-induced replication may lead to large repeat tract expansions, while frequent contractions occur either by single-strand annealing between repeat ends or by gene conversion, triggering near-complete contraction of the repeat tract. In the second part of this review, different therapeutic approaches using highly specific single- or double-strand endonucleases targeted to trinucleotide repeat loci are compared. Relative efficacies and specificities of these nucleases will be discussed, as well as their potential strengths and weaknesses for possible future gene therapy of these dramatic disorders.

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Precarious maintenance of simple DNA repeats in eukaryotes

Cited by 32 publications

References 124 publications

Nanopore sequencing of complex genomic rearrangements in yeast reveals mechanisms of repeat-mediated double-strand break repair

Nanopore sequencing of complex genomic rearrangements in yeast reveals mechanisms of repeat-mediated double-strand break repair

DNA repair in trinucleotide repeat ataxias

Trinucleotide repeat instability during double-strand break repair: from mechanisms to gene therapy

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