RNA-Mediated Neurodegeneration Caused by the Fragile X Premutation rCGG Repeats in Drosophila

Jin, Peng; Zarnescu, Daniela C.; Zhang, Fuping; Pearson, Christopher E.; Lucchesi, John C.; Moses, Kevin; Warren, Stephen T.

doi:10.1016/s0896-6273(03)00533-6

Cited by 334 publications

(372 citation statements)

References 34 publications

Supporting

Mentioning

353

Contrasting

Unclassified

Order By: Relevance

“…1B). These results are in accord with the observations made for shorter model transcripts (CNG) 16 and (CNG) 17 containing the artificial G-C clamp at the base of their hairpin stem (20). For comparison the model transcripts having not-clamped repeats were shown to have freedom of alignment and formed several alternative "slipped" structures each containing 4-nucleotide terminal loop (20).…”

Section: Pure Expanded Cag Repeats Form a Stable Hairpin Structure Wsupporting

confidence: 88%

“…This clamp forces the repeats to a single alignment, and the 7-nucleotide loop is formed in the transcript containing an even number of repeats whereas the 4-nucleotide loop is present in those having an odd repeat number. This pattern of the stem structure and loop sizes follows those observed for shorter (CAG) 16 and (CAG) 17 repeat tracts containing an artificial G-C clamp (20). Thus, it may be concluded from the above that both the uninterrupted normal repeats as well as expanded repeats present in mutation carriers form the same type of regular hairpin structure (Fig.…”

Section: Structures Of the Sca1 Transcripts Are The Same In Cellularsupporting

confidence: 72%

“…2C). Only at the temperature of 70°C and higher the structure formed by the helices H4 and 14 12-1-1-1-14 ⌬ ϭ Ϫ2 29 (CAG) 16 CAUCAGCAU (CAG) 10 16-1-1-1-10 ⌬ ϭ ϩ6 (CAG) 12 CAU (CAG) 16 12-1-16 ⌬ ϭ Ϫ4 30 (CAG) 12 CAUCAGCAU (CAG) 15 12-1-1-1-15 ⌬ ϭ Ϫ3 (CAG) 13 CAUCAGCAU (CAG) 14 13-1-1-1-14 ⌬ ϭ Ϫ1 31 (CAG) 11 CAUCAGCAUCAGCAU (CAG) 15 11-1-1-1-1-1-15 ⌬ ϭ Ϫ4 32 (CAG) 14 CAUCAGCAU (CAG) 15 14-1-1-1-15 ⌬ ϭ Ϫ1 (CAG) 12 CAUCAGCAU (CAG) 17 12- H3 was melted and all internucleotide bonds of that region showed similar reactivity. The structures formed by the repeats containing asymmetrically located interruptions are somewhat different (Fig.…”

Section: Cag Repeats Containing Either One or Two Cau Interruptions Umentioning

confidence: 99%

See 2 more Smart Citations

Imperfect CAG Repeats Form Diverse Structures in SCA1 Transcripts

Sobczak

Krzyżosiak

2004

Journal of Biological Chemistry

View full text Add to dashboard Cite

The expanded CAG repeat in the coding sequence of the spinocerebellar ataxia type 1 (SCA1) gene is responsible for SCA1, one of the hereditary human neurodegenerative diseases. In the normal SCA1 alleles usually 1-3 CAT triplets break the continuity of the CAG repeat tracts. Here we show what is the structural role of the CAU interruptions in the SCA1 transcripts. Depending on their number and localization within the repeat tract the interruptions either enlarge the terminal loop of the hairpin formed by the repeats, nucleate the internal loops in its stem structure, or force the repeats to fold into two smaller hairpins. Thus, the interruptions destabilize the CAG repeat hairpin, which is likely to decrease its ability to participate in the putative RNA pathogenesis mechanism driven by the long CAG repeat hairpins.

show abstract

Section: Pure Expanded Cag Repeats Form a Stable Hairpin Structure Wsupporting

confidence: 88%

Section: Structures Of the Sca1 Transcripts Are The Same In Cellularsupporting

confidence: 72%

Section: Cag Repeats Containing Either One or Two Cau Interruptions Umentioning

confidence: 99%

See 1 more Smart Citation

Imperfect CAG Repeats Form Diverse Structures in SCA1 Transcripts

Sobczak

Krzyżosiak

2004

Journal of Biological Chemistry

View full text Add to dashboard Cite

show abstract

“…In support of this hypothesis and the unified model for RNA pathogenesis in TREDs, there are recent results showing RNAmediated neurodegeneration caused by the FMR1 permutation [55]. The hairpin structure formed by the CGG repeats in the FMR1 transcript [38,56] together with its 5-10-fold increased level [57] likely to activate RNA pathogenesis in permutation carriers [55].…”

Section: Unified Model Of Rna-mediated Pathogenesis In Tredsmentioning

confidence: 69%

“…The hairpin structure formed by the CGG repeats in the FMR1 transcript [38,56] together with its 5-10-fold increased level [57] likely to activate RNA pathogenesis in permutation carriers [55]. The resulting syndromes, tremor-ataxia and premature ovarian failure, differ significantly in their clinical features from the fragile X syndrome developed in full mutation carriers [57].…”

Section: Unified Model Of Rna-mediated Pathogenesis In Tredsmentioning

confidence: 99%

Repetitive sequences that shape the human transcriptome

Jasinska¹,

Krzyżosiak²

2004

FEBS Letters

View full text Add to dashboard Cite

Only a small portion of the total RNA transcribed in human cells becomes mature mRNA and constitutes the human transcriptome, which is context-dependent and varies with development, physiology and pathology. A small fraction of different repetitive sequences, which make up more than half of the human genome, is retained in mature transcripts and shapes their function. Among them are short interspersed elements (SINEs), of which Alu sequences are most frequent, and simple sequence repeats, which come in many varieties. In this review, we have focused on the structural and functional role of Alu elements and trinucleotide repeats in transcripts.

show abstract

Fragile X–Associated Tremor/Ataxia Syndrome

Amiri

Hagerman

Hagerman³

2008

Arch Neurol

View full text Add to dashboard Cite

ragile X-associated tremor/ataxia syndrome (FXTAS) is a late-adult-onset neurodegenerative disorder affecting primarily male (and occasionally female) carriers of a premutation expansion (55-200 CGG repeats) of the fragile X mental retardation 1 gene (FMR1). FXTAS is principally characterized as a movement disorder with progressive intention tremor and gait ataxia, with more variable associated features of parkinsonism, dysautonomia, peripheral neuropathy, and dementia. The pathogenic basis of FXTAS is overexpression of the "toxic" expanded CGG repeat FMR1 RNA, which leads to neural cell dysregulation, formation of intranuclear inclusions in neurons and astrocytes, and disruption of the nuclear lamin architecture. By contrast, larger CGG repeat expansions (Ͼ200 CGG repeats, full mutation) generally result in FMR1 silencing and absence of FMR1 RNA and protein (FMRP). The lack of FMRP is the pathogenic basis of the developmental disorder fragile X syndrome, the leading heritable form of mental impairment. Thus, the same gene presents 2 opposing faces: a neurodegenerative syndrome (FXTAS) in older adults, caused by excess gene activity and production of a toxic RNA, and a childhood-onset disorder (fragile X syndrome), caused by absence of gene activity. This review will focus on FXTAS, the aging face of the fragile X gene.

show abstract

RNA-Mediated Neurodegeneration Caused by the Fragile X Premutation rCGG Repeats in Drosophila

Cited by 334 publications

References 34 publications

Imperfect CAG Repeats Form Diverse Structures in SCA1 Transcripts

Imperfect CAG Repeats Form Diverse Structures in SCA1 Transcripts

Repetitive sequences that shape the human transcriptome

Fragile X–Associated Tremor/Ataxia Syndrome

Contact Info

Product

Resources

About