ALS-derived fibroblasts exhibit reduced proliferation rate, cytoplasmic TDP-43 aggregation and a higher susceptibility to DNA damage

ALS-derived fibroblasts exhibit reduced proliferation rate, cytoplasmic TDP-43 aggregation and a higher susceptibility to DNA damage

Background Dermic fibroblasts have been proposed as a potential genetic-ALS cellular model. This study aimed to explore whether dermic fibroblasts from patients with sporadic-ALS (sALS) recapitulate alterations typical of ALS motor neurons and exhibit abnormal DNA-damage response. Methods Dermic fib...

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Veröffentlicht in:Journal of neurology 2020-05, Vol.267 (5), p.1291-1299
Hauptverfasser: Riancho, Javier, Castanedo-Vázquez, David, Gil-Bea, Francisco, Tapia, Olga, Arozamena, Jana, Durán-Vían, Carlos, Sedano, María José, Berciano, Maria Teresa, Lopez de Munain, Adolfo, Lafarga, Miguel
Format: Artikel
Sprache:eng
Schlagworte:
Aged
Amyotrophic lateral sclerosis
Amyotrophic Lateral Sclerosis - metabolism
Brain architecture
Cell Proliferation - physiology
Cell size
Cells, Cultured
Clinical Neurology
Cytology
Cytoplasm - metabolism
Deoxyribonucleic acid
DNA
DNA damage
DNA Damage - physiology
DNA repair
DNA-Binding Proteins - metabolism
Female
Fibroblasts
Fibroblasts - metabolism
Humans
Immunofluorescence
Life Sciences & Biomedicine
Male
Medicine
Medicine & Public Health
Middle Aged
Motor neurons
Neurology
Neuroradiology
Neurosciences
Neurosciences & Neurology
Nucleoli
Original Communication
Protein Aggregation, Pathological - metabolism
Radiation
Science & Technology
Skin - cytology
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Zusammenfassung:Background Dermic fibroblasts have been proposed as a potential genetic-ALS cellular model. This study aimed to explore whether dermic fibroblasts from patients with sporadic-ALS (sALS) recapitulate alterations typical of ALS motor neurons and exhibit abnormal DNA-damage response. Methods Dermic fibroblasts were obtained from eight sALS patients and four control subjects. Cellular characterization included proliferation rate analysis, cytoarchitecture studies and confocal immunofluorescence assessment for TDP-43. Additionally, basal and irradiation-induced DNA damage was evaluated by confocal immunofluorescence and biochemical techniques. Results sALS-fibroblasts showed decreased proliferation rates compared to controls. Additionally, whereas control fibroblasts exhibited the expected normal spindle-shaped morphology, ALS fibroblasts were thinner, with reduced cell size and enlarged nucleoli, with frequent cytoplasmic TDP-43aggregates. Also, baseline signs of DNA damage were evidenced more frequently in ALS-derived fibroblasts (11 versus 4% in control-fibroblasts). Assays for evaluating the irradiation-induced DNA damage demonstrated that DNA repair was defective in ALS-fibroblasts, accumulating more than double of γH2AX-positive DNA damage foci than controls. Very intriguingly, the proportion of fibroblasts particularly vulnerable to irradiation (with more than 15 DNA damage foci per nucleus) was seven times higher in ALS-derived fibroblasts than in controls. Conclusions Dermic-derived ALS fibroblasts recapitulate relevant cellular features of sALS and show a higher susceptibility to DNA damage and defective DNA repair responses. Altogether, these results support that dermic fibroblasts may represent a convenient and accessible ALS cellular model to study pathogenetic mechanisms, particularly those related to DNA damage response, as well as the eventual response to disease-modifying therapies.
ISSN:0340-5354
1432-1459
DOI:10.1007/s00415-020-09704-8