Your search keyword '"Anna Bagliani"' showing total 2 results

1. SETBP1 accumulation induces P53 inhibition and genotoxic stress in neural progenitors underlying neurodegeneration in Schinzel-Giedion syndrome

Author

Angelo Ianielli, Mattia Zaghi, Chiara Di Resta, Federica Banfi, Edoardo Bellini, Mirko Luoni, Luca Massimino, Rocco Piazza, Alicia Rubio, Alessandro Sessa, Anna Bagliani, Vania Broccoli, Giulia Fagnocchi, Cinzia Cancellieri, Maurizio Ferrari, Luca Mologni, Camilla Maffezzini, Banfi, F, Rubio, A, Zaghi, M, Massimino, L, Fagnocchi, G, Bellini, E, Luoni, M, Cancellieri, C, Bagliani, A, Di Resta, C, Maffezzini, C, Ianielli, A, Ferrari, M, Piazza, R, Mologni, L, Broccoli, V, Sessa, A, Banfi, F., Rubio, A., Zaghi, M., Massimino, L., Fagnocchi, G., Bellini, E., Luoni, M., Cancellieri, C., Bagliani, A., Di Resta, C., Maffezzini, C., Ianielli, A., Ferrari, M., Piazza, R., Mologni, L., Broccoli, V., and Sessa, A.

Subjects

Organoid, 0301 basic medicine, General Physics and Astronomy, Craniofacial Abnormalities, 0302 clinical medicine, Neural Stem Cells, Neurological models, Neural Stem Cell, Cells, Cultured, Nuclear Protein, Multidisciplinary, Neurodegenerative diseases, Neurodegeneration, Nuclear Proteins, Phenotype, Organoids, Heredodegenerative Disorders, Nervous System, Hand Deformities, Congenital, Human, Cell death, Programmed cell death, DNA damage, Science, Nails, Malformed, Biology, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, stomatognathic system, Intellectual Disability, medicine, Humans, Abnormalities, Multiple, Progenitor cell, Disease model, Craniofacial Abnormalitie, Schinzel–Giedion syndrome, SETBP1 Gene, General Chemistry, medicine.disease, 030104 developmental biology, Apoptosis, Mutation, Diseases of the nervous system, Tumor Suppressor Protein p53, Carrier Protein, Carrier Proteins, Neuroscience, 030217 neurology & neurosurgery, DNA Damage

Abstract

The investigation of genetic forms of juvenile neurodegeneration could shed light on the causative mechanisms of neuronal loss. Schinzel-Giedion syndrome (SGS) is a fatal developmental syndrome caused by mutations in the SETBP1 gene, inducing the accumulation of its protein product. SGS features multi-organ involvement with severe intellectual and physical deficits due, at least in part, to early neurodegeneration. Here we introduce a human SGS model that displays disease-relevant phenotypes. We show that SGS neural progenitors exhibit aberrant proliferation, deregulation of oncogenes and suppressors, unresolved DNA damage, and resistance to apoptosis. Mechanistically, we demonstrate that high SETBP1 levels inhibit P53 function through the stabilization of SET, which in turn hinders P53 acetylation. We find that the inheritance of unresolved DNA damage in SGS neurons triggers the neurodegenerative process that can be alleviated either by PARP-1 inhibition or by NAD + supplementation. These results implicate that neuronal death in SGS originates from developmental alterations mainly in safeguarding cell identity and homeostasis., Schinzel-Giedion syndrome (SGS) is a fatal developmental syndrome characterized by severe intellectual and physical deficits due, at least in part, to early neurodegeneration. Here the authors introduce a human SGS model that displays disease-relevant phenotypes to demonstrate that neuronal death in SGS originates from developmental alterations mainly in safeguarding cell identity and homeostasis.

Published

2021

2. TBL1XR1 Ensures Balanced Neural Development Through NCOR Complex-Mediated Regulation of the MAPK Pathway

Author

Giuseppina Mastrototaro, Mattia Zaghi, Luca Massimino, Matteo Moneta, Neda Mohammadi, Federica Banfi, Edoardo Bellini, Marzia Indrigo, Giulia Fagnocchi, Anna Bagliani, Stefano Taverna, Maria Rohm, Stephan Herzig, and Alessandro Sessa

Subjects

MAPK/ERK pathway, neurodevelopmental disorders, Point mutation, Wnt signaling pathway, Repressor, brain development, Context (language use), Cell Biology, Biology, MAPK cascade, MAPK, Mapk, Ncor, Tbl1xr1, Brain Development, Neurodevelopmental Disorders, Cell biology, Cell and Developmental Biology, lcsh:Biology (General), Nuclear receptor, NCOR, TBL1XR1, lcsh:QH301-705.5, Neural development, Original Research, Developmental Biology

Abstract

TBL1XR1 gene is associated with multiple developmental disorders presenting several neurological aspects. The relative protein is involved in the modulation of important cellular pathways and master regulators of transcriptional output, including nuclear receptor repressors, Wnt signaling, and MECP2 protein. However, TBL1XR1 mutations (including complete loss of its functions) have not been experimentally studied in a neurological context, leaving a knowledge gap in the mechanisms at the basis of the diseases. Here, we show that Tbl1xr1 knock-out mice exhibit behavioral and neuronal abnormalities. Either the absence of TBL1XR1 or its point mutations interfering with stability/regulation of NCOR complex induced decreased proliferation and increased differentiation in neural progenitors. We suggest that this developmental unbalance is due to a failure in the regulation of the MAPK cascade. Taken together, our results broaden the molecular and functional aftermath of TBL1XR1 deficiency associated with human disorders.

Published

2021