Low molecular weight species of TDP-43 generated by abnormal splicing form inclusions in amyotrophic lateral sclerosis and result in motor neuron death

Xiao, Shangxi; Sanelli, Teresa; Chiang, Helen; Sun, Yulong; Chakrabartty, Avijit; Keith, Julia; Rogaeva, Ekaterina; Zinman, Lorne; Robertson, Janice

doi:10.1007/s00401-015-1412-5

Cited by 72 publications

(65 citation statements)

References 31 publications

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“…Overexpression of TDP-43 causes asymmetric interactions between TDP-43 and its nascent RNA to stall RNA polymerase II (RNA Pol II), leading to transcript degradation and maintaining the autoregulation of TDP-43 protein level (Avendano-Vazquez et al, 2012). Interestingly, TDP-35, a second splice variant of TDP-43, has been found to be expressed in the brains of ALS patients, through the use of the downstream start codon ATG Met85 (Xiao et al, 2015). Expression of TDP-35 in primary neurons causes cytoplasmic aggregation and neuronal death (Xiao et al, 2015).…”

Section: Tdp-43 and Fus: A Perspective Into Neurobiology And Nuclementioning

confidence: 99%

“…Interestingly, TDP-35, a second splice variant of TDP-43, has been found to be expressed in the brains of ALS patients, through the use of the downstream start codon ATG Met85 (Xiao et al, 2015). Expression of TDP-35 in primary neurons causes cytoplasmic aggregation and neuronal death (Xiao et al, 2015). …”

Section: Tdp-43 and Fus: A Perspective Into Neurobiology And Nuclementioning

confidence: 99%

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TDP-43/FUS in motor neuron disease: Complexity and challenges

Guerrero

Wang

Mitra

et al. 2016

Progress in Neurobiology

103

122

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Amyotrophic lateral sclerosis (ALS), a common motor neuron disease affecting two per 100,000 people worldwide, encompasses at least five distinct pathological subtypes, including, ALS-SOD1, ALS-C9orf72, ALS-TDP-43, ALS-FUS and Guam-ALS. The etiology of a major subset of ALS involves toxicity of the TAR DNA-binding protein-43 (TDP-43). A second RNA/DNA binding protein, fused in sarcoma/translocated in liposarcoma (FUS/TLS) has been subsequently associated with about 1% of ALS patients. While mutations in TDP-43 and FUS have been linked to ALS, the key contributing molecular mechanism(s) leading to cell death are still unclear. One unique feature of TDP-43 and FUS pathogenesis in ALS is their nuclear clearance and simultaneous cytoplasmic aggregation in affected motor neurons. Since the discoveries in the last decade implicating TDP-43 and FUS toxicity in ALS, a majority of studies have focused on their cytoplasmic aggregation and disruption of their RNA-binding functions. However, TDP-43 and FUS also bind to DNA, although the significance of their DNA binding in disease-affected neurons has been less investigated. A recent observation of accumulated genomic damage in TDP-43 and FUS-linked ALS and association of FUS with neuronal DNA damage repair pathways indicate a possible role of deregulated DNA binding function of TDP-43 and FUS in ALS. In this review, we discuss the different ALS disease subtypes, crosstalk of etiopathologies in disease progression, available animal models and their limitations, and recent advances in understanding the specific involvement of RNA/DNA binding proteins, TDP-43 and FUS, in motor neuron diseases.

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Section: Tdp-43 and Fus: A Perspective Into Neurobiology And Nuclementioning

confidence: 99%

Section: Tdp-43 and Fus: A Perspective Into Neurobiology And Nuclementioning

confidence: 99%

TDP-43/FUS in motor neuron disease: Complexity and challenges

Guerrero

Wang

Mitra

et al. 2016

Progress in Neurobiology

103

122

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“…One challenge may be that as TDP-43 is a self-aggregating protein, it may self-assemble and generate structures that limit access of the detection antibody when present in biofluids. In addition, TDP-43 has been shown to be subject to alternative splicing causing truncations of the N-or C-terminus, leading to splice variants linked to ALS [96]. TDP-43 has been detected as 2 distinct species via Western blot: a 45-kDa (phosphorylated form) and 28-kDa isoform [95].…”

Section: Tar Dna-binding Protein Of 43 Kdamentioning

confidence: 99%

Fluid-Based Biomarkers for Amyotrophic Lateral Sclerosis

Bowser

2017

Neurotherapeutics

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Amyotrophic lateral sclerosis (ALS) is a highly heterogeneous disease with no effective treatment. Drug development has been hampered by the lack of biomarkers that aid in early diagnosis, demonstrate target engagement, monitor disease progression, and can serve as surrogate endpoints to assess the efficacy of treatments. Fluid-based biomarkers may potentially address these issues. An ideal biomarker should exhibit high specificity and sensitivity for distinguishing ALS from control (appropriate disease mimics and other neurologic diseases) populations and monitor disease progression within individual patients. Significant progress has been made using cerebrospinal fluid, serum, and plasma in the search for ALS biomarkers, with urine and saliva biomarkers still in earlier stages of development. A few of these biomarker candidates have demonstrated use in patient stratification, predicting disease course (fast vs slow progression) and severity, or have been used in preclinical and clinical applications. However, while ALS biomarker discovery has seen tremendous advancements in the last decade, validating biomarkers and moving them towards the clinic remains more elusive. In this review, we highlight biomarkers that are moving towards clinical utility and the challenges that remain in order to implement biomarkers at all stages of the ALS drug development process.

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“…Similarly, cleavage of TDP-43 leads to generation of C-terminal fragments (25 kDa in size), which are enriched in the insoluble fraction of pathological tissue with TDP-43 truncation due to caspase-3 [38]. More recently, formation of TDP-43 truncated form was shown to be generated by abnormal splicing using an alternate translation initiation codon (ATGMet85) with this isoform being associated with pathological inclusion bodies [39]. TDP-43 acetylation switch was also demonstrated to participate in its toxicity and aggregation [40].…”

Section: Aggregation Initiation Of Amyotrophic Lateral Sclerosis-assomentioning

confidence: 97%

Deciphering spreading mechanisms in amyotrophic lateral sclerosis

Pradat

Kabashi

Desnuelle

2015

Current Opinion in Neurology

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Although ALS is clinically heterogeneous, a shared characteristic is the focal onset and the progressive extension to all body regions. Being viewed until now as just summation of the increased number of affected neurons, dispersion is now rather considered as the result of a seeded self-propagating process. A sequential regional spreading pattern is supported by the distribution of TDP-43 aggregates in ALS autopsy cases. Electrophysiology and advanced neuroimaging methods also recently provided some evidence for propagation of lesions both in the brain and spinal cord, more longitudinal studies being still needed. Lesions are supposed to spread cell-to-cell regionally or through connected neuronal pathway. At the molecular level, the prion-like spreading is an emerging mechanism hypothesis, but other machineries such as those that are in charge of dealing with misfolded proteins and secretion of deleterious peptides may be involved in the propagation of neuron loss. Deciphering the mechanisms underlying spreading of ALS symptoms is of crucial importance to better understand this neurodegenerative disease, build new and appropriate animal models and to define novel therapeutic targets.

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Low molecular weight species of TDP-43 generated by abnormal splicing form inclusions in amyotrophic lateral sclerosis and result in motor neuron death

Cited by 72 publications

References 31 publications

TDP-43/FUS in motor neuron disease: Complexity and challenges

TDP-43/FUS in motor neuron disease: Complexity and challenges

Fluid-Based Biomarkers for Amyotrophic Lateral Sclerosis

Deciphering spreading mechanisms in amyotrophic lateral sclerosis

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