The
            <i>C9orf72</i>
            GGGGCC Repeat Is Translated into Aggregating Dipeptide-Repeat Proteins in FTLD/ALS

Mori, Kohji; Weng, Shih-Ming; Arzberger, Thomas; May, Stephanie; Rentzsch, Kristin; Kremmer, Elisabeth; Schmid, Bettina; Kretzschmar, Hans A.; Cruts, Marc; Broeckhoven, Christine Van; Haass, Christian; Edbauer, Dieter

doi:10.1126/science.1232927

Cited by 1,115 publications

(1,265 citation statements)

References 22 publications

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“…Abnormal proteins in the CNS of individuals with ALS causative mutations may provide specific biomarkers in gene-targeted therapy. Repeat expansions in C9ORF72, called dipeptide repeat proteins, in patients with ALS are presumably generated by non-ATG translation, serve as a critical component of p62 positive inclusions found in the cerebellum and hippocampus, and can also be identified in CSF [44][45][46]. The specificity of dipeptide repeat proteins for these patients confers an opportunity for use in trials and could even be a therapeutic target [47].…”

Section: Toward Novel Outcome Measures and Biomarkers In Als Trialsmentioning

confidence: 99%

Clinical Trial Designs in Amyotrophic Lateral Sclerosis: Does One Design Fit All?

2015

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The last 2 decades have seen a surge in the number of amyotrophic lateral sclerosis (ALS) clinical trials with the hope of finding successful treatments. Clinical trialists aim to repurpose existing drugs and test novel compounds to target potential ALS disease pathophysiology. Recent technological advancements have led to the discovery of new causative genetic agents and modes of delivering potential therapy, calling for increasingly sophisticated trial design. The standard ALS clinical trial design may be modified depending on study needs: type of therapy; route of therapy delivery; phase of therapy development; applicable subpopulation; market availability of therapy; and utility of telemedicine. Novel biomarkers of diagnostic, predictive, prognostic, and pharmacodynamic value are undergoing development and validation for use in clinical trials. Design modifications build on the traditional clinical trial design and may be employed in either the learning or confirming trial phase. Novel designs aim to minimize patient risk, study duration, and sample size, while improving efficiency and promoting statistical power to herald an exciting era for clinical research in ALS.

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Section: Toward Novel Outcome Measures and Biomarkers In Als Trialsmentioning

confidence: 99%

Clinical Trial Designs in Amyotrophic Lateral Sclerosis: Does One Design Fit All?

2015

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“…The C9orf72 hexanucleotide G 4 C 2 repeat is located within the first intron of the locus, in a noncoding region, and yet is translated into polypeptides through a unique pathway known as repeat-associated non-AUG dependent (RAN) translation [130][131][132][133] (Fig. 1).…”

Section: Alternative Rna-based Mechanismsmentioning

confidence: 99%

Linking RNA Dysfunction and Neurodegeneration in Amyotrophic Lateral Sclerosis

Barmada

2015

Neurotherapeutics

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The degeneration of motor neurons in amyotrophic lateral sclerosis (ALS) inevitably causes paralysis and death within a matter of years. Mounting genetic and functional evidence suggest that abnormalities in RNA processing and metabolism underlie motor neuron loss in sporadic and familial ALS. Abnormal localization and aggregation of essential RNA-binding proteins are fundamental pathological features of sporadic ALS, and mutations in genes encoding RNA processing enzymes cause familial disease. Also, expansion mutations occurring in the noncoding region of C9orf72-the most common cause of inherited ALS-result in nuclear RNA foci, underscoring the link between abnormal RNA metabolism and neurodegeneration in ALS. This review summarizes the current understanding of RNA dysfunction in ALS, and builds upon this knowledge base to identify converging mechanisms of neurodegeneration in ALS. Potential targets for therapy development are highlighted, with particular emphasis on early and conserved pathways that lead to motor neuron loss in ALS.

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“…One needs to remain open to the idea that expanded repeats so much longer than 30 GGGGCCs either might not sequester RNA-binding proteins and/or trigger another mechanism such as gene silencing at the C9ORF72 locus or translation of a toxic peptide. In this regard, it is worth noting that two groups recently reported immunostaining for GGGGCC repeat encoded insoluble peptides in the brains of patients who succumbed to C9ORF72 disease (9,10). Whether these peptides actually contribute to C9ORF72 remains to be shown.…”

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confidence: 99%

Toxic RNA as a driver of disease in a common form of ALS and dementia

Orr

2013

Proc. Natl. Acad. Sci. U.S.A.

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The C9orf72 GGGGCC Repeat Is Translated into Aggregating Dipeptide-Repeat Proteins in FTLD/ALS

Cited by 1,115 publications

References 22 publications

Clinical Trial Designs in Amyotrophic Lateral Sclerosis: Does One Design Fit All?

Clinical Trial Designs in Amyotrophic Lateral Sclerosis: Does One Design Fit All?

Linking RNA Dysfunction and Neurodegeneration in Amyotrophic Lateral Sclerosis

Toxic RNA as a driver of disease in a common form of ALS and dementia

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