Aggregation-prone c9FTD/ALS poly(GA) RAN-translated proteins cause neurotoxicity by inducing ER stress

Zhang, Yong Jie; Jansen-West, Karen; Xu, Ya; Gendron, Tania F.; Bieniek, Kevin F.; Lin, Wen Lang; Sasaguri, Hiroki; Caulfield, Thomas R.; Hubbard, Jaime; Daughrity, Lillian M.; Chew, Jeannie; Belzil, Véronique V.; Prudencio, Mercedes; Stankowski, Jeannette N.; Castanedes‐Casey, Monica; Whitelaw, Ena C.; Ash, Peter E.A.; DeTure, Michael; Rademakers, Rosa; Boylan, Kevin B.; Dickson, Dennis W.; Petrucelli, Leonard

doi:10.1007/s00401-014-1336-5

Cited by 293 publications

(365 citation statements)

References 78 publications

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“…Expanded repeats also undergo abnormal repeat associated non-ATG (RAN) translation (Zu et al, 2011). In patients, these proteins form stellate cytoplasmic inclusions in degenerate and non-degenerate brain regions Mackenzie et al, 2013;Mann et al, 2013;Mori et al, 2013b;Zu et al, 2013) and some have been shown to disrupt cellular function and cause toxicity when overexpressed in model systems (Kwon et al, 2014;Mizielinska et al, 2014;Wen et al, 2014;Zhang et al, 2014). Due to the number and complexity of these potential mechanisms, it remains unclear which among them contributes most to disease pathogenesis in patients.…”

Section: Introductionmentioning

confidence: 99%

Timing and significance of pathological features inC9orf72expansion-associated frontotemporal dementia

Vatsavayai

Yoon

Gardner

et al. 2016

Brain

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143

128

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) for a scientific commentary on this article.A GGGGCC repeat expansion in C9orf72 leads to frontotemporal dementia and/or amyotrophic lateral sclerosis. Diverse pathological features have been identified, and their disease relevance remains much debated. Here, we describe two illuminating patients with frontotemporal dementia due to the C9orf72 repeat expansion. Case 1 was a 65-year-old female with behavioural variant frontotemporal dementia accompanied by focal degeneration in subgenual anterior cingulate cortex, amygdala, and medial pulvinar thalamus. At autopsy, widespread RNA foci and dipeptide repeat protein inclusions were observed, but TDP-43 pathology was nearly absent, even in degenerating brain regions. Case 2 was a 74-year-old female with atypical frontotemporal dementia-motor neuron disease who underwent temporal lobe resection for epilepsy 5 years prior to her first frontotemporal dementia symptoms. Archival surgical resection tissue contained RNA foci, dipeptide repeat protein inclusions, and loss of nuclear TDP-43 but no TDP-43 inclusions despite florid TDP-43 inclusions at autopsy 8 years after first symptoms. These findings suggest that C9orf72-specific phenomena may impact brain structure and function and emerge before first symptoms and TDP-43 aggregation. Keywords: frontotemporal dementia; protein aggregation; TDP-43 Abbreviations: ALS = amyotrophic lateral sclerosis; FTD = frontotemporal dementia; mPULV = medial pulvinar nucleus of the thalamus; NCI = neuronal cytoplasmic inclusion

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Section: Introductionmentioning

confidence: 99%

Timing and significance of pathological features inC9orf72expansion-associated frontotemporal dementia

Vatsavayai

Yoon

Gardner

et al. 2016

Brain

Self Cite

143

128

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“…Similarly, gene expression analysis of ALS brain tissue from patients carrying C9orf72 mutations, the most relevant genetic alteration in ALS, mutations shows major alteration in ER stress-related genes in cerebellum [116]. In agreement with this, expression of RAN peptides derived from C9orf72 mutation in cell culture also triggers abnormal levels of ER stress [117].…”

Section: Amyotrophic Lateral Sclerosismentioning

confidence: 80%

ER stress in neurodegenerative disease: from disease mechanisms to therapeutic interventions

Cabral‐Miranda

Hetz

2017

Endoplasmic Reticulum Stress in Diseases

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The conception that protein aggregates composed by misfolded proteins underlies the occurrence of several neurodegenerative diseases suggests that this phenomenon may have a common origin, ultimately driven by disruption of proteostasis control. The unfolded protein response (UPR) embodies a major element of the proteostasis network, which is engaged by endoplasmic reticulum (ER) stress. Chronic ER stress may operate as a possible mechanism of neurodegeneration, contributing to synaptic alterations, neuroinflammation and neuronal loss. In this review we discuss most recent findings relating ER stress and the development of distinct neurodegenerative diseases, and the possible strategies for disease intervention.

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“…Indeed, biochemical data suggested that as many as 50% of the proteasome complexes in the neuron become highly entangled within poly(GA) ribbons. Removal of proteasomes from their normal location in cells through this sequestration mechanism might explain the reduced proteasomal activity in cells harbouring these aggregates 4,8 . Complexes called ribosomes, which mediate protein production and are comparable in size to proteasomes, were largely excluded from poly(GA) ribbons, suggesting that poly(GA) aggregates are actively recruited or retained by proteasomes.…”

Section: Years Agomentioning

confidence: 99%

50 & 100 Years Ago

2018

Nature

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Aggregation-prone c9FTD/ALS poly(GA) RAN-translated proteins cause neurotoxicity by inducing ER stress

Cited by 293 publications

References 78 publications

Timing and significance of pathological features inC9orf72expansion-associated frontotemporal dementia

Timing and significance of pathological features inC9orf72expansion-associated frontotemporal dementia

ER stress in neurodegenerative disease: from disease mechanisms to therapeutic interventions

50 & 100 Years Ago

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