Your search keyword '"Luigi Vescovi A"' showing total 10 results

1. Production of CSSi013-A (9360) iPSC line from an asymptomatic subject carrying an heterozygous mutation in TDP-43 protein

Author

Angela D'Anzi, Elisa Perciballi, Giorgia Ruotolo, Daniela Ferrari, Antonietta Notaro, Ivan Lombardi, Maurizio Gelati, Katia Frezza, Laura Bernardini, Isabella Torrente, Alessandro De Luca, Vincenzo La Bella, Angelo Luigi Vescovi, Jessica Rosati, D'Anzi, Angela, Perciballi, Elisa, Ruotolo, Giorgia, Ferrari, Daniela, Notaro, Antonietta, Lombardi, Ivan, Gelati, Maurizio, Frezza, Katia, Bernardini, Laura, Torrente, Isabella, De Luca, Alessandro, La Bella, Vincenzo, Luigi Vescovi, Angelo, Rosati, Jessica, D'Anzi, A, Perciballi, E, Ruotolo, G, Ferrari, D, Notaro, A, Lombardi, I, Gelati, M, Frezza, K, Bernardini, L, Torrente, I, De Luca, A, La Bella, V, Luigi Vescovi, A, and Rosati, J

Subjects

DNA-Binding Proteins, Heterozygote, DNA-Binding Protein, Amyotrophic Lateral Sclerosis, Induced Pluripotent Stem Cells, Mutation, Humans, Cell Biology, General Medicine, Induced Pluripotent Stem Cell, Developmental Biology, Amyotrophic Lateral Sclerosi, Human

Abstract

Amyotrophic Lateral Sclerosis (ALS) is a fatal disease affecting both upper and lower motoneurons. The transactive response DNA binding protein (TARDBP) gene, encoding for TDP-43, is one of the most commonly mutated gene associated with familial cases of ALS (10%). We generated a human induced pluripotent stem cell (hiPSC) line from the fibroblasts of an asymptomatic subject carrying the TARDBP p.G376D mutation. This mutation is very rare and was described in a large Apulian family, in which all ALS affected members are carriers of the mutation. The subject here described is the first identified asymptomatic carrier of the mutation.

Published

2022

2. Corrigendum: Deepening the understanding of CNVs on chromosome 15q11–13 by using hiPSCs: An overview

Author

Angela Maria Giada Giovenale, Giorgia Ruotolo, Amata Amy Soriano, Elisa Maria Turco, Giovannina Rotundo, Alessia Casamassa, Angela D’Anzi, Angelo Luigi Vescovi, and Jessica Rosati

Subjects

Cell Biology, Developmental Biology

Published

2023

3. Deepening the understanding of CNVs on chromosome 15q11–13 by using hiPSCs: An overview

Author

Angela Maria Giada Giovenale, Giorgia Ruotolo, Amata Amy Soriano, Elisa Maria Turco, Giovannina Rotundo, Alessia Casamassa, Angela D’Anzi, Angelo Luigi Vescovi, and Jessica Rosati

Subjects

Cell Biology, Developmental Biology

Abstract

The human α7 neuronal nicotinic acetylcholine receptor gene (CHRNA7) is widely expressed in the central and peripheral nervous systems. This receptor is implicated in both brain development and adult neurogenesis thanks to its ability to mediate acetylcholine stimulus (Ach). Copy number variations (CNVs) of CHRNA7 gene have been identified in humans and are genetically linked to cognitive impairments associated with multiple disorders, including schizophrenia, bipolar disorder, epilepsy, Alzheimer’s disease, and others. Currently, α7 receptor analysis has been commonly performed in animal models due to the impossibility of direct investigation of the living human brain. But the use of model systems has shown that there are very large differences between humans and mice when researchers must study the CNVs and, in particular, the CNV of chromosome 15q13.3 where the CHRNA7 gene is present. In fact, human beings present genomic alterations as well as the presence of genes of recent origin that are not present in other model systems as well as they show a very heterogeneous symptomatology that is associated with both their genetic background and the environment where they live. To date, the induced pluripotent stem cells, obtained from patients carrying CNV in CHRNA7 gene, are a good in vitro model for studying the association of the α7 receptor to human diseases. In this review, we will outline the current state of hiPSCs technology applications in neurological diseases caused by CNVs in CHRNA7 gene. Furthermore, we will discuss some weaknesses that emerge from the overall analysis of the published articles.

Published

2023

4. Generation of an induced pluripotent stem cell line CSSi015-A (9553), carrying a point mutation c.2915C > T in the human calcium sensing receptor (CasR) gene

Author

Giovannina Rotundo, Elisa Maria Turco, Giorgia Ruotolo, Isabella Torrente, Ornella Candido, Gianluca Lopez, Daniela Ferrari, Caterina Caputi, Mario Mastrangelo, Francesco Pisani, Maurizio Gelati, Vito Guarnieri, Angelo Luigi Vescovi, and Jessica Rosati

Subjects

Familial Hypocalciuric Hypercalcemia, calcium-sensing receptor gene, pluripotent stem cell, Cell Biology, General Medicine, Developmental Biology

Published

2023

5. Characterization of the p.L145F and p.S135N Mutations in SOD1: Impact on the Metabolism of Fibroblasts Derived from Amyotrophic Lateral Sclerosis Patients

Author

Elisa Perciballi, Federica Bovio, Jessica Rosati, Federica Arrigoni, Angela D’Anzi, Serena Lattante, Maurizio Gelati, Fabiola De Marchi, Ivan Lombardi, Giorgia Ruotolo, Matilde Forcella, Letizia Mazzini, Sandra D’Alfonso, Lucia Corrado, Mario Sabatelli, Amelia Conte, Luca De Gioia, Sabata Martino, Angelo Luigi Vescovi, Paola Fusi, Daniela Ferrari, Perciballi, E, Bovio, F, Rosati, J, Arrigoni, F, D'Anzi, A, Lattante, S, Gelati, M, De Marchi, F, Lombardi, I, Ruotolo, G, Forcella, M, Mazzini, L, D'Alfonso, S, Corrado, L, Sabatelli, M, Conte, A, De Gioia, L, Martino, S, Vescovi, A, Fusi, P, and Ferrari, D

Subjects

amyotrophic lateral sclerosis, energetic metabolism, SOD1 expression, Physiology, ALS, p.L144F, p.S134N, SOD1 mutations, seahorse, p.L145F, p.S135N, mitochondria, Clinical Biochemistry, Cell Biology, Settore MED/03 - GENETICA MEDICA, Biochemistry, SOD1 mutation, metabolic studies, amyotrophic lateral sclerosi, Molecular Biology

Abstract

Amyotrophic lateral sclerosis (ALS) is a fatal neurodegenerative disease characterized by the loss of the upper and lower motor neurons (MNs). About 10% of patients have a family history (familial, fALS); however, most patients seem to develop the sporadic form of the disease (sALS). SOD1 (Cu/Zn superoxide dismutase-1) is the first studied gene among the ones related to ALS. Mutant SOD1 can adopt multiple misfolded conformation, lose the correct coordination of metal binding, decrease structural stability, and form aggregates. For all these reasons, it is complicated to characterize the conformational alterations of the ALS-associated mutant SOD1, and how they relate to toxicity. In this work, we performed a multilayered study on fibroblasts derived from two ALS patients, namely SOD1L145F and SOD1S135N, carrying the p.L145F and the p.S135N missense variants, respectively. The patients showed diverse symptoms and disease progression in accordance with our bioinformatic analysis, which predicted the different effects of the two mutations in terms of protein structure. Interestingly, both mutations had an effect on the fibroblast energy metabolisms. However, while the SOD1L145F fibroblasts still relied more on oxidative phosphorylation, the SOD1S135N fibroblasts showed a metabolic shift toward glycolysis. Our study suggests that SOD1 mutations might lead to alterations in the energy metabolism.

Published

2022

6. Retinoic acid-induced 1 gene haploinsufficiency alters lipid metabolism and causes autophagy defects in Smith-Magenis syndrome

Author

Elisa Maria Turco, Angela Maria Giada Giovenale, Laura Sireno, Martina Mazzoni, Alessandra Cammareri, Caterina Marchioretti, Laura Goracci, Alessandra Di Veroli, Elena Marchesan, Daniel D’Andrea, Antonella Falconieri, Barbara Torres, Laura Bernardini, Maria Chiara Magnifico, Alessio Paone, Serena Rinaldo, Matteo Della Monica, Stefano D’Arrigo, Diana Postorivo, Anna Maria Nardone, Giuseppe Zampino, Roberta Onesimo, Chiara Leoni, Federico Caicci, Domenico Raimondo, Elena Binda, Laura Trobiani, Antonella De Jaco, Ada Maria Tata, Daniela Ferrari, Francesca Cutruzzolà, Gianluigi Mazzoccoli, Elena Ziviani, Maria Pennuto, Angelo Luigi Vescovi, Jessica Rosati, Turco, E, Giovenale, A, Sireno, L, Mazzoni, M, Cammareri, A, Marchioretti, C, Goracci, L, Di Veroli, A, Marchesan, E, D'Andrea, D, Falconieri, A, Torres, B, Bernardini, L, Magnifico, M, Paone, A, Rinaldo, S, Della Monica, M, D'Arrigo, S, Postorivo, D, Nardone, A, Zampino, G, Onesimo, R, Leoni, C, Caicci, F, Raimondo, D, Binda, E, Trobiani, L, De Jaco, A, Tata, A, Ferrari, D, Cutruzzola, F, Mazzoccoli, G, Ziviani, E, Pennuto, M, Vescovi, A, and Rosati, J

Subjects

Cancer Research, Haploinsufficiency genetic, Immunology, Autophagy genetic, Smith-Magenis Syndrome diagnosi, Tretinoin, Haploinsufficiency, Trans-Activators metabolism, Tretinoin pharmacology, Cellular and Molecular Neuroscience, Transcription Factors metabolism, Autophagy, Humans, RAI1, IPCSc, SMS, autophagy, IPCSc, Cell Biology, Lipid, Lipid Metabolism, Lipids, Smith-Magenis Syndrome pathology, Tretinoin metabolism, Lipid Metabolism genetic, Phenotype, SMS, Smith-Magenis Syndrome genetic, Trans-Activators, RAI1, Smith-Magenis Syndrome, Transcription Factors, Human

Abstract

Smith-Magenis syndrome (SMS) is a neurodevelopmental disorder characterized by cognitive and behavioral symptoms, obesity, and sleep disturbance, and no therapy has been developed to alleviate its symptoms or delay disease onset. SMS occurs due to haploinsufficiency of the retinoic acid-induced-1 (RAI1) gene caused by either chromosomal deletion (SMS-del) or RAI1 missense/nonsense mutation. The molecular mechanisms underlying SMS are unknown. Here, we generated and characterized primary cells derived from four SMS patients (two with SMS-del and two carrying RAI1 point mutations) and four control subjects to investigate the pathogenetic processes underlying SMS. By combining transcriptomic and lipidomic analyses, we found altered expression of lipid and lysosomal genes, deregulation of lipid metabolism, accumulation of lipid droplets, and blocked autophagic flux. We also found that SMS cells exhibited increased cell death associated with the mitochondrial pathology and the production of reactive oxygen species. Treatment with N-acetylcysteine reduced cell death and lipid accumulation, which suggests a causative link between metabolic dyshomeostasis and cell viability. Our results highlight the pathological processes in human SMS cells involving lipid metabolism, autophagy defects and mitochondrial dysfunction and suggest new potential therapeutic targets for patient treatment.

Published

2022

7. Generation and characterization of CSSi016-A (9938) human pluripotent stem cell line carrying two biallelic variants in MTMR5/SBF1 gene resulting in a case of severe CMT4B3

Author

Elisa, Maria Turco, Angela, Maria Giada Giovenale, Giovannina, Rotundo, Martina, Mazzoni, Paola, Zanfardino, Katia, Frezza, Isabella, Torrente, Rose, Mary Carletti, Devid, Damiani, Filippo M, Santorelli, Angelo, Luigi Vescovi, Vittoria, Petruzzella, and Jessica, Rosati

Subjects

Pluripotent Stem Cells, Intracellular Signaling Peptides and Proteins, Humans, Cell Biology, General Medicine, Child, Developmental Biology

Abstract

Charcot-Marie-Tooth type 4B3 (CMT4B3) is a rare subtype of hereditary neuropathy associated with variants in the MTMR5/SBF1 gene. Herein, we report the generation and characterization of a hiPSC line from a 12-year-old Italian girl with early onset severe polyneuropathy with motor and axonal involvement, harboring biallelic variants in the MTMR5/SBF1 gene. Fibroblasts were reprogrammed using non-integrating episomal plasmids, and iPSCs successfully passed the stemness and pluripotency tests. Patient-specific hiPSCs were produced to obtain a disease model for the study of this rare condition.

Published

2022

8. Generation of an induced pluripotent stem cells line, CSSi014-A 9407, carrying the variant c.479C>T in the human iduronate 2-sulfatase (hIDS) gene

Author

Alessia Casamassa, Alessandra Zanetti, Daniela Ferrari, Ivan Lombardi, Gaia Galluzzi, Francesca D'Avanzo, Gabriella Cipressa, Alessia Bertozzi, Isabella Torrente, Angelo Luigi Vescovi, Rosella Tomanin, Jessica Rosati, Casamassa, A, Zanetti, A, Ferrari, D, Lombardi, I, Galluzzi, G, D'Avanzo, F, Cipressa, G, Bertozzi, A, Torrente, I, Vescovi, A, Tomanin, R, and Rosati, J

Subjects

Phenotype, Glycosaminoglycan, Iduronic Acid, Induced Pluripotent Stem Cells, Humans, Iduronate Sulfatase, Cell Biology, General Medicine, Induced Pluripotent Stem Cell, Human, Glycosaminoglycans, Mucopolysaccharidosis II, Developmental Biology

Abstract

Mucopolysaccharidosis type II (Hunter Syndrome) is a rare X-linked inherited lysosomal storage disorder presenting a wide genetic heterogeneity. It is due to pathogenic variants in the IDS gene, causing the deficit of the lysosomal hydrolase iduronate 2-sulfatase, degrading the glycosaminoglycans (GAGs) heparan- and dermatan-sulfate. Based on the presence/absence of neurocognitive signs, commonly two forms are recognized, the severe and the attenuate ones. Here we describe a line of induced pluripotent stem cells, generated from dermal fibroblasts, carrying the mutation c.479C>T, and obtained from a patient showing an attenuated phenotype. The line will be useful to study the disease neuropathogenesis.

Published

2022

9. Generation of an induced pluripotent stem cell line, CSSi011-A (6534), from an Amyotrophic lateral sclerosis patient with heterozygous L145F mutation in SOD1 gene

Author

Marina Goldoni, Sandra D'Alfonso, Fabiola De Marchi, Letizia Mazzini, Elisa Perciballi, Daniela Ferrari, Angela D'Anzi, Alice Di Pierro, Maurizio Gelati, Angelo Luigi Vescovi, Filomena Altieri, Jessica Rosati, Laura Bernardini, D'Anzi, A, Altieri, F, Perciballi, E, Ferrari, D, Bernardini, L, Goldoni, M, Mazzini, L, De Marchi, F, Di Pierro, A, D'Alfonso, S, Gelati, M, Vescovi, A, and Rosati, J

Subjects

0301 basic medicine, Somatic cell, SOD1, Biology, medicine.disease_cause, hiPSC, familial ALS, 03 medical and health sciences, 0302 clinical medicine, medicine, Missense mutation, Amyotrophic lateral sclerosis, Induced pluripotent stem cell, Gene, lcsh:QH301-705.5, Mutation, nutritional and metabolic diseases, Cell Biology, General Medicine, Motor neuron, medicine.disease, nervous system diseases, 030104 developmental biology, medicine.anatomical_structure, nervous system, lcsh:Biology (General), CSSi011-A, ALS, human induced pluripotent stem cell, Cancer research, 030217 neurology & neurosurgery, Developmental Biology

Abstract

Among the known causative genes of familial ALS, SOD1 mutation is one of the most common. It encodes for the ubiquitous detoxifying copper/zinc binding SOD1 enzyme, whose mutations selectively cause motor neuron death, although the mechanisms are not as yet clear. What is known is that mutant-mediated toxicity is not caused by loss of its detoxifying activity but by a gain-of-function. In order to better understand the pathogenic mechanisms of SOD1 mutation, a human induced pluripotent stem cell (hiPSC) line was generated from the somatic cells of a female patient carrying a missense variation in SOD1 (L145F).

Published

2020

10. The adult human subventricular zone

Author

Eleonora Aronica, Sophia F A M de Sonnaville, Tasmin Deering, Dick F. Swaab, Lidia De Filippis, Annemiek van Berkel, Rainer Glass, Vanessa Donega, Elly M. Hol, Martina Moeton, Pierre Robe, Jinte Middeldorp, Wilma D.J. van de Berg, Jacqueline A. Sluijs, Angelo Luigi Vescovi, Simone A. van den Berge, Miriam E van Strien, Netherlands Institute for Neuroscience (NIN), Anatomy and neurosciences, de Sonnaville, S, van Strien, M, Middeldorp, J, Sluijs, J, van den Berge, S, Moeton, M, Donega, V, van Berkel, A, Deering, T, De Filippis, L, Vescovi, A, Aronica, E, Glass, R, van de Berg, W, Swaab, D, Robe, P, and Hol, E

Subjects

0301 basic medicine, Glial nodule, Subventricular zone, Biology, cerebrospinal fluid, 03 medical and health sciences, glial nodules, 0302 clinical medicine, Cerebrospinal fluid, Neurosphere, medicine, human, Progenitor cell, neural stem cells, AcademicSubjects/SCI01870, Neurogenesis, General Engineering, subventricular zone, Neural stem cell, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Original Article, AcademicSubjects/MED00310, Stem cell, Ependyma, 030217 neurology & neurosurgery

Abstract

Neurogenesis continues throughout adulthood in specialized regions of the brain. One of these regions is the subventricular zone. During brain development, neurogenesis is regulated by a complex interplay of intrinsic and extrinsic cues that control stem-cell survival, renewal and cell lineage specification. Cerebrospinal fluid (CSF) is an integral part of the neurogenic niche in development as it is in direct contact with radial glial cells, and it is important in regulating proliferation and migration. Yet, the effect of CSF on neural stem cells in the subventricular zone of the adult human brain is unknown. We hypothesized a persistent stimulating effect of ventricular CSF on neural stem cells in adulthood, based on the literature, describing bulging accumulations of subventricular cells where CSF is in direct contact with the subventricular zone. Here, we show by immunohistochemistry on post-mortem adult human subventricular zone sections that neural stem cells are in close contact with CSF via protrusions through both intact and incomplete ependymal layers. We are the first to systematically quantify subventricular glial nodules denuded of ependyma and consisting of proliferating neural stem and progenitor cells, and showed that they are present from foetal age until adulthood. Neurosphere, cell motility and differentiation assays as well as analyses of RNA expression were used to assess the effects of CSF of adult humans on primary neural stem cells and a human immortalized neural stem cell line. We show that human ventricular CSF increases proliferation and decreases motility of neural stem cells. Our results also indicate that adult CSF pushes neural stem cells from a relative quiescent to a more active state and promotes neuronal over astrocytic lineage differentiation. Thus, CSF continues to stimulate neural stem cells throughout aging., De Sonnaville et al. demonstrate that subventricular glial nodules in the human subventricular zone—denuded of ependyma—consist of accumulating proliferating neural stem and progenitor cells, corroborating in vitro findings that adult cerebrospinal fluid retains the capacity to stimulate proliferation, influence motility and promote differentiation of neural stem cells., Graphical Abstract Graphical Abstract

Published

2020