Chemotherapeutic deletion of CTG repeats in lymphoblast cells from DM1 patients

Hashem, Vera I.; Pytlos, Malgorzata J.; Klysik, Elzbieta; Tsuji, Kuniko; Khajav, Merhdad; Ashizawa, Tetsuo; Sinden, Richard R.

doi:10.1093/nar/gkh976

Cited by 54 publications

(43 citation statements)

References 86 publications

(141 reference statements)

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“…Experimental therapy was performed by using lymphoblast cells of DM1 patients and CTG repeat expansion can be reduced by chemotherapeutic agents; ethylmethanesulfonate, mitomycin C, mitoxantrone, doxorubicin (31). This may be eventually applicable to 17 neurological intractable diseases including spinocerebellar degeneration in addition to DM1.…”

Section: F) Treatment For Severe Constipation In Myotonic Dystrophymentioning

confidence: 99%

New Classification and Treatment for Myotonic Disorders

Kurihara

2005

Intern. Med.

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Myotonia is repetitive firing of muscle action potentials causing prolonged muscle contractions even after mechanical stimulations to the muscles have ceased. Most common myotonic disorder is myotonic dystrophy which is now termed DM1, myotonic dystrophy type 1. In Japan, proximal myotonic myopathy, which is now called DM2 has not been reported. Both DM1 and DM2 have Cl channel abnormality which causes myotonia. Less commonly we encounter Thomsen's disease, and autosomal recessive generalized myotonia (Becker type) which also have a Cl channel abnormality. There are other myotonic disorders related to Na channelopathy which include three disorders: paramyotonia congenita, adynamia episodica hereditaria, and myotonia fluctuans. Myotonia has been treated by various Na channel blockers, mexiletine, phenytoin, and carbamazepine, but they were originally developed for cardiac arrhythmia, or seizure disorders and they have undesirable side effects, weakness. Comprehensive treatment includes myotonia control without reducing the strength, and care for systemic manifestations of DM1.

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Section: F) Treatment For Severe Constipation In Myotonic Dystrophymentioning

confidence: 99%

New Classification and Treatment for Myotonic Disorders

Kurihara

2005

Intern. Med.

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“…Chemotherapeutic drugs that are used to treat cancer can also attack DNA and result in DNA damage including bulky DNA adducts and interstrand cross-link (ICL) (26,32). Some DNA lesions are highly mutagenic and cause mutations in the genome, thereby altering genetic information that is passed from parent cells to daughter cells.…”

Section: Figure I1 Deamination Of Cytosine (C) and 5-methylcytosine mentioning

confidence: 99%

“…Trinucleotide repeat deletions can be induced in human lymphoblasts (32), bacterial cells (26) and mouse sperm (175), by DNA-damaging agents including ethyl methanesulfonate, mitomycin C, ethylnitrosourea, ultraviolet radiation, cisplatin and ionizing radiation (32,175,176). Because the DNA-damaging agents can induce alkylating DNA damage, DNA strand breaks, DNA cross-links that are usually subjected to BER and nucleotide excision repair, it suggests that BER and NER are actively involved in mediating TNR deletion.…”

Section: Overviewmentioning

confidence: 99%

“…Twenty nanograms of the repaired DNA was used for subsequent DNA fragment analysis. All substrates were 32 Pradiolabeled at the 5'-end of the strand that contained a deoxyuridine or a THF residue.…”

Section: In Vitro Ber In Mouse Embryonic Fibroblast Cell Extractsmentioning

confidence: 99%

“…Substrates were 32 P-labeled at the 3'-or 5'-end of the strand with an 8-oxoG or a THF residue, the upstream primer and downstream primer.…”

Section: In Vitro Ber Reconstituted With Purified Enzymesmentioning

confidence: 99%

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Oxidative DNA Damage Modulates Trinucleotide Repeat Instability Via DNA Base Excision Repair

Xu¹

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Identification of Trinucleotide Repeat Ligands with a FRET Melting Assay

et al. 2008

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DNA hairpin structures formed within a repeated tract might be a causative factor for triplet expansion observed in several debilitating diseases. We have designed and used a fluorescence resonance energy transfer (FRET) melting assay to screen for ligands that bind specifically to the CNG triplet repeats. Using this assay, we screened a panel of 33 chemicals that were previously designed to bind DNA or RNA secondary structures. Remarkably, we found that macrocyclic compounds, such as acridine dimers and trimers, exhibit interesting affinities and specificities for this motif.

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Chemotherapeutic deletion of CTG repeats in lymphoblast cells from DM1 patients

Cited by 54 publications

References 86 publications

New Classification and Treatment for Myotonic Disorders

New Classification and Treatment for Myotonic Disorders

Oxidative DNA Damage Modulates Trinucleotide Repeat Instability Via DNA Base Excision Repair

Identification of Trinucleotide Repeat Ligands with a FRET Melting Assay

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