Reduction of toxic RNAs in myotonic dystrophies type 1 and type 2 by the RNA helicase p68/DDX5

Jones, Karlie; Wei, Christina; Schöser, Benedikt; Meola, G.; Timchenko, Nikolai A.; Timchenko, Lubov

doi:10.1073/pnas.1422273112

Cited by 28 publications

(28 citation statements)

References 20 publications

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“…Biopsy samples from DM1 and DM2 skeletal muscles showed the reduced level of p68. Ectopic p68 reduces skeletal muscle myopathy and atrophy by lowering the pathogenic CUG or CCUG RNA(49). First, Spoon KH domain might be facilitating decay of the pathogenic SCA8 transcripts.…”

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confidence: 99%

The RNA binding KH domain of Spoonbill depletes pathogenic non-coding spinocerebellar ataxia 8 transcripts and suppresses neurodegeneration in Drosophila

Tripathi

Surabhi

Bhaskar

et al. 2016

Biochimica et Biophysica Acta (BBA) - Molecular Basis of Diseas

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Spinocerebellar ataxia 8 (SCA8) pathogenesis is a resultant of gain-of-function machinery that primarily results at the RNA level. It has been reported that expanded non-coding CTG trinucleotide repeat in the ATXN8OS transcripts leads to SCA8 coupled neurodegeneration. Targeted depletion of pathogenic SCA8 transcripts is a viable therapeutic approach. In this report we have focused on the suppression of toxic RNA gain-of-function associated with SCA8. We report suppression of SCA8 associated neurodegeneration by KH RNA binding domain of Spoonbill. KH domain suppresses pathogenic SCA8 associated phenotype in adult flies. Ectopic expression of KH domain leads to massive reduction in the number and size of SCA8 RNA foci. We show that Spoonbill interacts with toxic SCA8 transcripts via its KH domain and promotes its depletion. Till date, no attempts have been made for therapeutic intervention of SCA8 pathogenesis. Further characterization of Spoonbill KH domain may aid us in designing peptide based therapeutics for SCA8 associated neurodegeneration.

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confidence: 99%

The RNA binding KH domain of Spoonbill depletes pathogenic non-coding spinocerebellar ataxia 8 transcripts and suppresses neurodegeneration in Drosophila

Tripathi

Surabhi

Bhaskar

et al. 2016

Biochimica et Biophysica Acta (BBA) - Molecular Basis of Diseas

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“…For instance, two DM1 RNA toxic foci enhancers ( str-67 and ocrl-1 ) have been identified in Caenorhabditis elegans [93]. Nonsense-mediated decay, Staufen and DEAD-box helicase 5 (DDX5) all have an impact on toxic RNA transport and degradation [94–96]. In addition, a large ribonucleoprotein complex may transiently regulate the sense foci (Fig.…”

Section: Rna Toxicity and Foci In Dmmentioning

confidence: 99%

RNA toxicity and foci formation in microsatellite expansion diseases

Zhang

Ashizawa

2017

Current Opinion in Genetics & Development

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More than 30 incurable neurological and neuromuscular diseases are caused by simple microsatellite expansions consisted of 3–6 nucleotides. These repeats can occur in non-coding regions and often result in a dominantly inherited disease phenotype that is characteristic of a toxic RNA gain-of-function. The expanded RNA adopts unusual secondary structures, sequesters various RNA binding proteins to form insoluble nuclear foci, and causes cellular defects at a multisystem level. Nuclear foci are dynamic in size, shape and colocalization of RNA binding proteins in different expansion diseases and tissue types. This review sets to provide new insights into the disease mechanisms of RNA toxicity and foci modulation, in light of recent advancement on bi-directional transcription, antisense RNA, repeat-associated non-ATG translation and beyond.

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“…Degradation of the mutant DMPK mRNA using antisense oligonucleotides or by increase of RNA helicase p68 corrects muscle pathology in HSA LR mice (10, 12). Normalization of the activities of RNA‐binding proteins, misregulated by CUG repeats (CUGBP1 and MBNL1), was also shown to be beneficial for the reduction of DM1 muscle pathology in HSA LR mice (12).…”

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confidence: 99%

“…Two of the most-studied proteins, associated with the disruption of RNA processing in DM1, are muscleblind 1 (MBNL1) and CUGBP1 [(also known as CUGBP1 elav-like factor (CELF1)] (3)(4)(5)(6)(7). Other RNA-binding proteins are also affected in DM1, including Staufen1 and RNA helicases DDX5 and DDX6 (8)(9)(10)(11).…”

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confidence: 99%

“…ABBREVIATIONS: BIO, 6-bromoindirubin-39-oxime; CDK4, cyclin Ddependent kinase 4; CDM1, congenital myotonic dystrophy type 1; Col, collagen; CUGBP1/CELF1, CUG-binding protein/CUGBP1 elav-like factor 1; DCX, doublecortin; DDX, DEAD-box; DM1, myotonic dystrophy type 1; DMPK, dystrophia myotonica protein kinase; ECM, extracellular matrix; eIF2, eukaryotic initiation factor 2; ES, embryonic stem cell; GSK3b, glycogen synthase kinase 3b; het, heterozygous; hom, homozygous; HSA LR , human skeletal actin mRNA, containing long repeats; IF, immunofluorescence; IP, immunoprecipitation; KO, knockout; LEF1, lymphoid enhancer binding factor 1; MBNL1, muscleblind 1 protein; MSC, myogenic satellite cell; p-, phosphorylated; Pax7, paired box 7 factor; Ppp1r14d, protein phosphatase 1 regulatory inhibitor subunit 14D; RBM45, RNA-binding motif 45 protein; RRM, RNA recognition motif; RUNX2, runt-related transcription factor 2; TCF7, T cell specific transcription factor 7; TDZD-8, 4-benzyl-2-methyl-1,2,4thiadiazolidine-3,5-dione; unp, unphosphorylated; WT, wild type Degradation of the mutant DMPK mRNA using antisense oligonucleotides or by increase of RNA helicase p68 corrects muscle pathology in HSA LR mice (10,12). Normalization of the activities of RNA-binding proteins, misregulated by CUG repeats (CUGBP1 and MBNL1), was also shown to be beneficial for the reduction of DM1 muscle pathology in HSA LR mice (12).…”

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confidence: 99%

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Correction of GSK3ß at young age prevents muscle pathology in mice with myotonic dystrophy type 1

et al. 2018

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Myotonic dystrophy type 1 (DM1) is a progressive neuromuscular disease caused by expanded CUG repeats, which misregulate RNA metabolism through several RNA-binding proteins, including CUG-binding protein/CUGBP1 elav-like factor 1 (CUGBP1/CELF1) and muscleblind 1 protein. Mutant CUG repeats elevate CUGBP1 and alter CUGBP1 activity via a glycogen synthase kinase 3β (GSK3β)-cyclin D3-cyclin D-dependent kinase 4 (CDK4) signaling pathway. Inhibition of GSK3β corrects abnormal activity of CUGBP1 in DM1 mice [human skeletal actin mRNA, containing long repeats ( HSA) model]. Here, we show that the inhibition of GSK3β in young HSA mice prevents development of DM1 muscle pathology. Skeletal muscle in 1-yr-old HSA mice, treated at 1.5 mo for 6 wk with the inhibitors of GSK3, exhibits high fiber density, corrected atrophy, normal fiber size, with reduced central nuclei and normalized grip strength. Because CUG-GSK3β-cyclin D3-CDK4 converts the active form of CUGBP1 into a form of translational repressor, we examined the contribution of CUGBP1 in myogenesis using Celf1 knockout mice. We found that a loss of CUGBP1 disrupts myogenesis, affecting genes that regulate differentiation and the extracellular matrix. Proteins of those pathways are also misregulated in young HSA mice and in muscle biopsies of patients with congenital DM1. These findings suggest that the correction of GSK3β-CUGBP1 pathway in young HSA mice might have a positive effect on the myogenesis over time.-Wei, C., Stock, L., Valanejad, L., Zalewski, Z. A., Karns, R., Puymirat, J., Nelson, D., Witte, D., Woodgett, J., Timchenko, N. A., Timchenko, L. Correction of GSK3β at young age prevents muscle pathology in mice with myotonic dystrophy type 1.

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Reduction of toxic RNAs in myotonic dystrophies type 1 and type 2 by the RNA helicase p68/DDX5

Cited by 28 publications

References 20 publications

The RNA binding KH domain of Spoonbill depletes pathogenic non-coding spinocerebellar ataxia 8 transcripts and suppresses neurodegeneration in Drosophila

The RNA binding KH domain of Spoonbill depletes pathogenic non-coding spinocerebellar ataxia 8 transcripts and suppresses neurodegeneration in Drosophila

RNA toxicity and foci formation in microsatellite expansion diseases

Correction of GSK3ß at young age prevents muscle pathology in mice with myotonic dystrophy type 1

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