An MND/ALS phenotype associated with <i>C9orf72</i> repeat expansion: Abundant p62‐positive, TDP‐43‐negative inclusions in cerebral cortex, hippocampus and cerebellum but without associated cognitive decline

Troakes, Claire; Maekawa, Satomi; Wijesekera, Lokesh; Rogelj, Boris; Szabó, László; Bell, Christopher; Smith, Bradley N.; Newhouse, Stephen J.; Vance, Caroline; Johnson, Lauren; Hortobágyi, Tibor; Shatunov, Aleksey; Al‐Chalabi, Ammar; Leigh, Nigel; Shaw, Christopher E.; King, Andrew; Al‐Sarraj, Safa

doi:10.1111/j.1440-1789.2011.01286.x

Cited by 114 publications

(101 citation statements)

References 39 publications

(53 reference statements)

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“…4). This evidence supports that the abnormal accumulation of TDP-43, p62, and ubiquitin seen in patients with ALS and FTD with C9orf72 expansions (21,(38)(39)(40) is not induced by a loss of C9orf72 function mRNA and supports that ASO-mediated C9orf72 reductions should be tolerated in an adult nervous system and may be safe to use in ALS and FTD.…”

Section: Discussionsupporting

confidence: 75%

“…Abnormal aggregations of TDP-43, p62, and ubiquitin have been extensively described in the neuropathology of ALS and FTD with C9orf72 expansion (21,(38)(39)(40). After 18 wk of ASOmediated depletion of C9orf72 RNA, examination of tissue sections revealed that TDP-43 remained mainly nuclear in spinal cord, hippocampus, and cortex (Fig.…”

Section: Ggggccmentioning

confidence: 77%

“…Among these, ALS and FTD from repeat expansions in C9orf72 display a unique neuropathology signature, including aggregation of protein biomarkers, such as p62, that are deposited in cerebellar Purkinje and granule cells and in hippocampal neurons (38,39). To this specific signature, we now add the presence of nuclear RNA foci containing the hexanucleotide repeats transcribed from both sense and antisense strands.…”

Section: Discussionmentioning

confidence: 99%

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Targeted degradation of sense and antisense C9orf72 RNA foci as therapy for ALS and frontotemporal degeneration

Lagier‐Tourenne

Baughn

Rigo

et al. 2013

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

507

539

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Expanded hexanucleotide repeats in the chromosome 9 open reading frame 72 (C9orf72) gene are the most common genetic cause of ALS and frontotemporal degeneration (FTD). Here, we identify nuclear RNA foci containing the hexanucleotide expansion (GGGGCC) in patient cells, including white blood cells, fibroblasts, glia, and multiple neuronal cell types (spinal motor, cortical, hippocampal, and cerebellar neurons). RNA foci are not present in sporadic ALS, familial ALS/FTD caused by other mutations (SOD1, TDP-43, or tau), Parkinson disease, or nonneurological controls. Antisense oligonucleotides (ASOs) are identified that reduce GGGGCC-containing nuclear foci without altering overall C9orf72 RNA levels. By contrast, siRNAs fail to reduce nuclear RNA foci despite marked reduction in overall C9orf72 RNAs. Sustained ASO-mediated lowering of C9orf72 RNAs throughout the CNS of mice is demonstrated to be well tolerated, producing no behavioral or pathological features characteristic of ALS/FTD and only limited RNA expression alterations. Genome-wide RNA profiling identifies an RNA signature in fibroblasts from patients with C9orf72 expansion. ASOs targeting sense strand repeat-containing RNAs do not correct this signature, a failure that may be explained, at least in part, by discovery of abundant RNA foci with C9orf72 repeats transcribed in the antisense (GGCCCC) direction, which are not affected by sense strand-targeting ASOs. Taken together, these findings support a therapeutic approach by ASO administration to reduce hexanucleotide repeat-containing RNAs and raise the potential importance of targeting expanded RNAs transcribed in both directions.E xpanded hexanucleotide repeats in the first intron of the chromosome 9 open reading frame 72 (C9orf72) gene were recently identified (1, 2) as the most common genetic cause of ALS, frontotemporal degeneration (FTD), or concomitant ALS/ FTD (3, 4). The mechanisms by which the expanded repeats cause neurodegeneration are unknown, but leading candidate mechanisms are RNA-mediated toxicity, loss of the C9orf72 gene function (from reduced C9orf72 produced by the allele with the expansion), or a combination of the two.RNA-mediated toxicity from nucleotide repeat expansion was initially described for CUG expansion in the RNA encoded by the DMPK gene in myotonic muscular dystrophy (5). A consensus view is that RNA toxicity plays a crucial role in a variety of repeat expansion disorders (6). A hallmark of these disorders is the accumulation of expanded transcripts into nuclear RNA foci (7). RNAs harboring a long stretch of repeats are thought to fold into stable structures and sequester RNA binding proteins, which, in turn, sets off a molecular cascade leading to neurodegeneration (7). In myotonic dystrophy, sequestration and functional disruption of the muscleblind-like family of RNA binding proteins are associated with specific splicing and expression changes in affected tissues (5,(8)(9)(10)(11)(12).Sequestration of one or more RNA binding proteins into pathological RNA foci has ...

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Section: Discussionsupporting

confidence: 75%

Section: Ggggccmentioning

confidence: 77%

Section: Discussionmentioning

confidence: 99%

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Targeted degradation of sense and antisense C9orf72 RNA foci as therapy for ALS and frontotemporal degeneration

Lagier‐Tourenne

Baughn

Rigo

et al. 2013

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

507

539

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“…30 Consistent with our results, a recent study found mild to moderate p62 and TDP-43 staining in the thalamus of 4 C9ϩ carriers with MND. 31 Thalamic atrophy has been described in FTLD-TDP type A, 5,32 but not in type B, which is typically associated with FTD-MND. Although most FTD-MND cases show FTLD-TDP type B histology, an unexpected feature of C9ORF72 pathology is the frequency of FTLD-TDP type A.…”

Section: Demographicsmentioning

confidence: 99%

Frontotemporal dementia due to C9ORF72 mutations

et al. 2012

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Objective: To describe the phenotype of patients with C9FTD/ALS (C9ORF72) hexanucleotide repeat expansion. Methods:A total of 648 patients with frontotemporal dementia (FTD)-related clinical diagnoses and Alzheimer disease (AD) dementia were tested for C9ORF72 expansion and 31 carried expanded repeats (C9ϩ Results: All C9ϩ patients displayed clinical syndromes of bvFTD, ALS, or FTD-MND. At first evaluation, C9ϩ bvFTD patients had more delusions and greater impairment of working memory, but milder eating dysregulation compared to bvFTD noncarriers. C9ϩFTD-MND patients had a trend for longer survival and had an earlier age at onset than FTD-MND noncarriers. Voxel-based morphometry demonstrated more thalamic atrophy in FTD and FTD-MND carriers than in noncarriers. Conclusions: GLOSSARYAD ϭ Alzheimer disease; ALS ϭ amyotrophic lateral sclerosis; bvFTD ϭ behavioral variant frontotemporal dementia; CBS ϭ corticobasal syndrome; CDR-SB ϭ Clinical Dementia Rating Scale sum of boxes; FTD ϭ frontotemporal dementia; FWE ϭ familywise error; glm ϭ generalized linear model; lvPPA ϭ logopenic variant primary progressive aphasia; MND ϭ motor neuron disease; nfvPPA ϭ nonfluent variant primary progressive aphasia; NPI ϭ Neuropsychiatric Inventory; PSP ϭ progressive supranuclear palsy; svPPA ϭ semantic variant primary progressive aphasia; UCSF ϭ University of California, San Francisco; VBM ϭ voxel-based morphometry.Frontotemporal dementia (FTD) is a common dementia syndrome among patients presenting before 65 years of age with prevalence equal to Alzheimer disease (AD) dementia.1,2 FTD often overlaps with amyotrophic lateral sclerosis (ALS), with symptoms of FTD occurring in 15%-41% of patients with ALS and features of ALS occurring in 15% of FTD.3,4 Many patients with FTD and ALS exhibit autosomal dominant family histories (FTD 10% 5 ; ALS 5%-10% 6 ; FTD-motor neuron disease [MND] 37% 7 ) and a number of large familial cohorts have been linked to a chromosome 9p region. [7][8][9][10][11][12] Recently, a noncoding expanded hexanucleotide repeat in chromosome 9 open reading frame 72 (C9ORF72) was identified as the cause of chromosome 9p-associated FTD and ALS. 13,14 This mutation is the most common genetic cause of familial and sporadic behavioral variant FTD (bvFTD) and ALS.In one study, the C9ORF72 (C9FTD/ALS) expansion accounted for 11.7% of familial FTD, 22.5% of familial ALS, and 4% of sporadic ALS.13 Previous family studies of chromosome 9p-linked families 7,8,10 suggested that some features may distinguish this mutation from sporadic

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“…30 TDP-43 inclusions are also prominent in cases linked to chromosome 9p 31 but HREM-specific pathology includes abundant cytoplasmic and intranuclear p62-positive inclusions in the hippocampus and cerebellum that are TDP-43-negative. 32,33 Precisely, how the HREM causes TDP-43 mislocalisation and neurodegeneration is not currently known. Evidence that the HREM reduces levels of C9ORF72 transcripts implicates a loss of function, however, probes detecting the HREM transcript identified RNA foci within the nuclei of neurons in the frontal cortex and spinal cord.…”

Section: Human_reference : Gcgcgctaggggccggggccggggcc---------------mentioning

confidence: 99%

The C9ORF72 expansion mutation is a common cause of ALS+/−FTD in Europe and has a single founder

et al. 2012

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A massive hexanucleotide repeat expansion mutation (HREM) in C9ORF72 has recently been linked to amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD). Here we describe the frequency, origin and stability of this mutation in ALS þ / ÀFTD from five European cohorts (total n ¼ 1347). Single-nucleotide polymorphisms defining the risk haplotype in linked kindreds were genotyped in cases (n ¼ 434) and controls (n ¼ 856). Haplotypes were analysed using PLINK and aged using DMLE þ . In a London clinic cohort, the HREM was the most common mutation in familial ALS þ / ÀFTD: C9ORF72 29/112 (26%), SOD1 27/112 (24%), TARDBP 1/112 (1%) and FUS 4/112 (4%) and detected in 13/216 (6%) of unselected sporadic ALS cases but was rare in controls (3/856, 0.3%). HREM prevalence was high for familial ALS þ / ÀFTD throughout Europe: Belgium 19/22 (86%), Sweden 30/41 (73%), the Netherlands 10/27 (37%) and Italy 4/20 (20%). The HREM did not affect the age at onset or survival of ALS patients. Haplotype analysis identified a common founder in all 137 HREM carriers that arose around 6300 years ago. The haplotype from which the HREM arose is intrinsically unstable with an increased number of repeats (average 8, compared with 2 for controls, Po10 À8 ). We conclude that the HREM has a single founder and is the most common mutation in familial and sporadic ALS in Europe.

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An MND/ALS phenotype associated with C9orf72 repeat expansion: Abundant p62‐positive, TDP‐43‐negative inclusions in cerebral cortex, hippocampus and cerebellum but without associated cognitive decline

Cited by 114 publications

References 39 publications

Targeted degradation of sense and antisense C9orf72 RNA foci as therapy for ALS and frontotemporal degeneration

Targeted degradation of sense and antisense C9orf72 RNA foci as therapy for ALS and frontotemporal degeneration

Frontotemporal dementia due to C9ORF72 mutations

The C9ORF72 expansion mutation is a common cause of ALS+/−FTD in Europe and has a single founder

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