Your search keyword '"Comi, Giacomo P"' showing total 28 results

1. Clinical Phenotype of Pediatric and Adult Patients With Spinal Muscular Atrophy With Four SMN2 Copies: Are They Really All Stable?

Author

Ricci, Martina, Cicala, Gianpaolo, Capasso, Anna, Coratti, Giorgia, Fiori, Stefania, Cutrona, Costanza, D'Amico, Adele, Sansone, Valeria A., Bruno, Claudio, Messina, Sonia, Mongini, Tiziana, Coccia, Michela, Siciliano, Gabriele, Pegoraro, Elena, Masson, Riccardo, Filosto, Massimiliano, Comi, Giacomo P., Corti, Stefania, Ronchi, Dario, and Maggi, Lorenzo

Subjects

SPINAL muscular atrophy, NATURAL history, PHENOTYPES, PHENOTYPIC plasticity, ASYMPTOMATIC patients

Abstract

Objective: The aim of this study was to provide an overview of the clinical phenotypes associated with 4 SMN2 copies. Methods: Clinical phenotypes were analyzed in all the patients with 4 SMN2 copies as part of a nationwide effort including all the Italian pediatric and adult reference centers for spinal muscular atrophy (SMA). Results: The cohort includes 169 patients (102 men and 67 women) with confirmed 4 SMN2 copies (mean age at last follow‐up = 36.9 ± 19 years). Six of the 169 patients were presymptomatic, 8 were classified as type II, 145 as type III (38 type IIIA and 107 type IIIB), and 8 as type IV. The remaining 2 patients were asymptomatic adults identified because of a familial case. The cross‐sectional functional data showed a reduction of scores with increasing age. Over 35% of the type III and 25% of the type IV lost ambulation (mean age = 26.8 years ± 16.3 SD). The risk of loss of ambulation was significantly associated with SMA type (p < 0.0001), with patients with IIIB and IV less likely to lose ambulation compared to type IIIA. There was an overall gender effect with a smaller number of women and a lower risk for women to lose ambulation. This was significant in the adult (p = 0.009) but not in the pediatric cohort (p = 0.43). Interpretation: Our results expand the existing literature on natural history of 4 SMN2 copies confirming the variability of phenotypes in untreated patients, ranging from type II to type IV and an overall reduction of functional scores with increasing age. ANN NEUROL 2023;94:1126–1135 [ABSTRACT FROM AUTHOR]

Published

2023

2. Intravenous thrombolysis + endovascular thrombectomy versus thrombolysis alone in large vessel occlusion mild stroke: a propensity score matched analysis.

Author

Schwarz, Ghil, Bonato, Sara, Lanfranconi, Silvia, Matusevicius, Marius, Ghione, Isabella, Valcamonica, Gloria, Tsivgoulis, Georgios, Paiva Nunes, Ana, Mancuso, Michelangelo, Zini, Andrea, Candelaresi, Paolo, Rand, Viiu‐Marika, Comi, Giacomo P., Mazya, Michael V., and Ahmed, Niaz

Subjects

ENDOVASCULAR surgery, PROPENSITY score matching, STROKE, INTERNAL carotid artery, THROMBOLYTIC therapy, LACUNAR stroke

Abstract

Background and purpose: The best reperfusion treatment for patients with mild acute ischaemic stroke harbouring proximal anterior circulation large vessel occlusion (LVO) is unknown. The aim was to compare the safety and efficacy of intravenous thrombolysis (IVT) plus endovascular thrombectomy (EVT) versus IVT alone in LVO patients with mild symptoms. Methods: From the Safe Implementation of Treatment in Stroke–International Stroke Thrombolysis and Thrombectomy Register (SITS‐ISTR), were included: (i) consecutive acute ischaemic stroke patients, (ii) treated within 4.5 h from symptoms onset, (iii) baseline National Institutes of Health Stroke Scale (NIHSS) score ≤5 and (iv) intracranial internal carotid artery [ICA], M1 or T occlusion [defined as occlusion of ICA terminal bifurcation]. After propensity score matching, 3‐month functional outcomes (modified Rankin Scale [mRS] 0–1 and 0–2) and safety outcomes (symptomatic intracerebral haemorrhage and death) were compared (via univariable and multivariable logistic [and ordinal] regression analyses) in patients treated with IVT + EVT versus IVT alone. Results: In all, 1037 patients were included. After propensity score matching (n = 312 per group), IVT + EVT was independently associated with poor functional outcomes (adjusted odds ratio [aOR] 0.46 for mRS 0–1, 95% confidence interval [CI] 0.30–0.72, p = 0.001; aOR 0.52 for mRS 0–2, 95% CI 0.32–0.84, p = 0.007; aOR 1.61 for 1‐point shift in mRS score, 95% CI 1.12–2.32, p = 0.011), with no significant differences in safety outcomes compared to IVT alone, despite numerically higher rates of symptomatic intracerebral haemorrhage (3.3% vs. 1.1%; p = 0.082), a higher rate of any haemorrhagic transformation (17.6% vs. 7.3%; p < 0.001) and subarachnoid haemorrhage (7.9% vs. 1.5%; p = 0.002) in the IVT + EVT group. Discussion: In anterior circulation LVO patients presenting with NIHSS score ≤5, IVT + EVT (vs. IVT alone) was associated with poorer 3‐month functional outcome. Randomized controlled trials are needed to elucidate the best treatments in mild LVO patients. [ABSTRACT FROM AUTHOR]

Published

2023

3. Characterization of patients with Becker muscular dystrophy by histology, magnetic resonance imaging, function, and strength assessments.

Author

Comi, Giacomo P., Niks, Erik H., Cinnante, Claudia M., Kan, Hermien E., Vandenborne, Krista, Willcocks, Rebecca J., Velardo, Daniele, Ripolone, Michela, van Benthem, Jules J., van de Velde, Nienke M., Nava, Simone, Ambrosoli, Laura, Cazzaniga, Sara, and Bettica, Paolo U.

Abstract

Introduction/Aims: Becker muscular dystrophy (BMD) is characterized by variable disease severity and progression, prompting the identification of biomarkers for clinical trials. We used data from an ongoing phase II study to provide a comprehensive characterization of a cohort of patients with BMD, and to assess correlations between histological and magnetic resonance imaging (MRI) markers with muscle function and strength. Methods: Eligible patients were ambulatory males with BMD, aged 18 to 65 years (200 to 450 meters on 6‐minute walk test). The following data were obtained: function test results, strength, fat‐fraction quantification using chemical shift‐encoded MRI (whole thigh and quadriceps), and fibrosis and muscle fiber area (MFA) of the brachial biceps. Results: Of 70 patients screened, 51 entered the study. There was substantial heterogeneity between patients in muscle morphology (histology and MRI), with high fat replacement. Total fibrosis correlated significantly and mostly moderately with all functional endpoints, including both upper arm strength assessments (left and right elbow flexion rho −.574 and −.588, respectively [both P <.0001]), as did MRI fat fraction (whole thigh and quadriceps), for example, with four‐stair‐climb velocity −.554 and −.550, respectively (both P <.0001). Total fibrosis correlated significantly and moderately with both MRI fat fraction assessments (.500 [P =.0003] and.423 [.0024], respectively). Discussion: In this BMD cohort, micro‐ and macroscopic morphological muscle parameters correlated moderately with each other and with functional parameters, potentially supporting the use of MRI fat fraction and histology as surrogate outcome measures in patients with BMD, although additional research is required to validate this. [ABSTRACT FROM AUTHOR]

Published

2022

4. A Novel Homozygous VPS11 Variant May Cause Generalized Dystonia.

Author

Monfrini, Edoardo, Cogiamanian, Filippo, Salani, Sabrina, Straniero, Letizia, Fagiolari, Gigliola, Garbellini, Manuela, Carsana, Emma, Borellini, Linda, Biella, Fabio, Moggio, Maurizio, Bresolin, Nereo, Corti, Stefania, Duga, Stefano, Comi, Giacomo P., Aureli, Massimo, and Di Fonzo, Alessio

Subjects

DYSTONIA, CHIMERIC proteins, ENDOSOMES, AUTOPHAGY, FIBROBLASTS

Abstract

In this work, we describe the association of a novel homozygous VPS11 variant with adult‐onset generalized dystonia, providing a detailed clinical report and biological evidence of disease mechanism. Vps11 is a subunit of the homotypic fusion and protein sorting (HOPS) complex, which promotes the fusion of late endosomes and autophagosomes with the lysosome. Functional studies on mutated fibroblasts showed marked lysosomal and autophagic abnormalities, which improved after overexpression of the wild type Vps11 protein. In conclusion, a deleterious VPS11 variant, damaging the autophagic and lysosomal pathways, is the probable genetic cause of a novel form of generalized dystonia. ANN NEUROL 2021;89:834–839 [ABSTRACT FROM AUTHOR]

Published

2021

5. MYH2 myopathy, a new case expands the clinical and pathological spectrum of the recessive form.

Author

Telese, Roberta, Pagliarani, Serena, Lerario, Alberto, Ciscato, Patrizia, Fagiolari, Gigliola, Cassandrini, Denise, Grimoldi, Nadia, Conte, Giorgio, Cinnante, Claudia, Santorelli, Filippo M., Comi, Giacomo P., Sciacco, Monica, and Peverelli, Lorenzo

Subjects

NEMALINE myopathy, MUSCLE weakness, MUSCLE diseases, GENETIC mutation, RARE diseases

Abstract

Background: Hereditary myosin myopathies are a group of rare muscle disorders, caused by mutations in genes encoding for skeletal myosin heavy chains (MyHCs). MyHCIIa is encoded by MYH2 and is expressed in fast type 2A and 2B muscle fibers. MYH2 mutations are responsible for an autosomal dominant (AD) progressive myopathy, characterized by the presence of rimmed vacuoles and by a reduction in the number and size of type 2A fibers, and a recessive early onset myopathy characterized by complete loss of type 2A fibers. Recently, a patient with a homozygous mutation but presenting a dominant phenotype has been reported. Methods: The patient was examined thoroughly and two muscle biopsies were performed through the years. NGS followed by confirmation in Sanger sequencing was used to identify the genetic cause. Results: We describe the second case presenting with late‐onset ophthalmoparesis, ptosis, diffuse muscle weakness, and histopathological features typical for AD forms but with a recessive MYH2 genotype. Conclusion: This report contributes to expand the clinical and genetic spectrum of MYH2 myopathies and to increase the awareness of these very rare diseases. [ABSTRACT FROM AUTHOR]

Published

2020

6. Genetic modifiers of respiratory function in Duchenne muscular dystrophy.

Author

Bello, Luca, D'Angelo, Grazia, Villa, Matteo, Fusto, Aurora, Vianello, Sara, Merlo, Beatrice, Sabbatini, Daniele, Barp, Andrea, Gandossini, Sandra, Magri, Francesca, Comi, Giacomo P., Pedemonte, Marina, Tacchetti, Paola, Lanzillotta, Valentina, Trucco, Federica, D'Amico, Adele, Bertini, Enrico, Astrea, Guja, Politano, Luisa, and Masson, Riccardo

Subjects

DUCHENNE muscular dystrophy, GENERALIZED estimating equations, EXPERIMENTAL design, RESPIRATORY insufficiency, SKELETAL muscle, EXPIRATORY flow, NEMALINE myopathy

Abstract

Objective: Respiratory insufficiency is a major complication of Duchenne muscular dystrophy (DMD). Its progression shows considerable interindividual variability, which has been less thoroughly characterized and understood than in skeletal muscle. We collected pulmonary function testing (PFT) data from a large retrospective cohort followed at Centers collaborating in the Italian DMD Network. Furthermore, we analyzed PFT associations with different DMD mutation types, and with genetic variants in SPP1, LTBP4, CD40, and ACTN3, known to modify skeletal muscle weakness in DMD. Genetic association findings were independently validated in the Cooperative International Neuromuscular Research Group Duchenne Natural History Study (CINRG‐DNHS). Methods and Results: Generalized estimating equation analysis of 1852 PFTs from 327 Italian DMD patients, over an average follow‐up time of 4.5 years, estimated that forced vital capacity (FVC) declined yearly by −4.2%, forced expiratory volume in 1 sec by −5.0%, and peak expiratory flow (PEF) by −2.9%. Glucocorticoid (GC) treatment was associated with higher values of all PFT measures (approximately + 15% across disease stages). Mutations situated 3' of DMD intron 44, thus predicted to alter the expression of short dystrophin isoforms, were associated with lower (approximately −6%) PFT values, a finding independently validated in the CINRG‐DNHS. Deletions amenable to skipping of exon 51 and 53 were independently associated with worse PFT outcomes. A meta‐analysis of the two cohorts identified detrimental effects of SPP1 rs28357094 and CD40 rs1883832 minor alleles on both FVC and PEF. Interpretation: These findings support GC efficacy in delaying respiratory insufficiency, and will be useful for the design and interpretation of clinical trials focused on respiratory endpoints in DMD. [ABSTRACT FROM AUTHOR]

Published

2020

7. Dystonia‐ataxia syndrome with permanent torsional nystagmus caused by ECHS1 deficiency.

Author

Ronchi, Dario, Monfrini, Edoardo, Bonato, Sara, Mancinelli, Veronica, Cinnante, Claudia, Salani, Sabrina, Bordoni, Andreina, Ciscato, Patrizia, Fortunato, Francesco, Villa, Marianna, Di Fonzo, Alessio, Corti, Stefania, Bresolin, Nereo, and Comi, Giacomo P.

Subjects

HEARING disorders, NYSTAGMUS, BASAL ganglia, SYNDROMES, AMINO acids, CEREBELLUM degeneration

Abstract

Biallelic mutations in ECHS1, encoding the mitochondrial enoyl‐CoA hydratase, have been associated with mitochondrial encephalopathies with basal ganglia involvement. Here, we describe a novel clinical presentation consisting of dystonia‐ataxia syndrome with hearing loss and a peculiar torsional nystagmus observed in two adult siblings. The presence of a 0.9‐ppm peak at MR spectroscopy analysis suggested the accumulation of branched‐chain amino acids. Exome sequencing in index probands identified two ECHS1 mutations, one of which was novel (p.V82L). ECHS1 protein levels and residual activities were reduced in patients' fibroblasts. This paper expands the phenotypic spectrum observed in patients with impaired valine catabolism. [ABSTRACT FROM AUTHOR]

Published

2020

8. MicroRNAs as regulators of cell death mechanisms in amyotrophic lateral sclerosis.

Author

Gagliardi, Delia, Comi, Giacomo P., Bresolin, Nereo, and Corti, Stefania

Subjects

MICRORNA, AMYOTROPHIC lateral sclerosis, APOPTOSIS, NECROSIS, MOTOR neurons, GENETIC regulation, NEURODEGENERATION, THERAPEUTICS research

Abstract

Amyotrophic lateral sclerosis (ALS) is a progressive neurodegenerative disorder affecting upper and lower motor neurons (MNs), resulting in paralysis and precocious death from respiratory failure. Although the causes of ALS are incompletely understood, the role of alterations in RNA metabolism seems central. MicroRNAs (miRNAs) are noncoding RNAs implicated in the regulation of gene expression of many relevant physiological processes, including cell death. The recent model of programmed cell death (PCD) encompasses different mechanisms, from apoptosis to regulated necrosis (RN), in particular necroptosis. Both apoptosis and necroptosis play a significant role in the progressive death of MNs in ALS. In this review, we present key research related to miRNAs that modulate apoptosis and RN pathways in ALS. We also discuss whether these miRNAs represent potential targets for therapeutic development in patients. [ABSTRACT FROM AUTHOR]

Published

2019

9. The analysis of myotonia congenita mutations discloses functional clusters of amino acids within the CBS2 domain and the C‐terminal peptide of the ClC‐1 channel.

Author

Altamura, Concetta, Lucchiari, Sabrina, Sahbani, Dalila, Ulzi, Gianna, Comi, Giacomo P., D'Ambrosio, Paola, Petillo, Roberta, Politano, Luisa, Vercelli, Liliana, Mongini, Tiziana, Dotti, Maria Teresa, Cardani, Rosanna, Meola, Giovanni, Lo Monaco, Mauro, Matthews, Emma, Hanna, Michael G., Carratù, Maria Rosaria, Conte, Diana, Imbrici, Paola, and Desaphy, Jean‐François

Abstract

Abstract: Myotonia congenita (MC) is a skeletal‐muscle hyperexcitability disorder caused by loss‐of‐function mutations in the ClC‐1 chloride channel. Mutations are scattered over the entire sequence of the channel protein, with more than 30 mutations located in the poorly characterized cytosolic C‐terminal domain. In this study, we characterized, through patch clamp, seven ClC‐1 mutations identified in patients affected by MC of various severities and located in the C‐terminal region. The p.Val829Met, p.Thr832Ile, p.Val851Met, p.Gly859Val, and p.Leu861Pro mutations reside in the CBS2 domain, while p.Pro883Thr and p.Val947Glu are in the C‐terminal peptide. We showed that the functional properties of mutant channels correlated with the clinical phenotypes of affected individuals. In addition, we defined clusters of ClC‐1 mutations within CBS2 and C‐terminal peptide subdomains that share the same functional defect: mutations between 829 and 835 residues and in residue 883 induced an alteration of voltage dependence, mutations between 851 and 859 residues, and in residue 947 induced a reduction of chloride currents, whereas mutations on 861 residue showed no obvious change in ClC‐1 function. This study improves our understanding of the mechanisms underlying MC, sheds light on the role of the C‐terminal region in ClC‐1 function, and provides information to develop new antimyotonic drugs. [ABSTRACT FROM AUTHOR]

Published

2018

10. Purkinje cell COX deficiency and mtDNA depletion in an animal model of spinocerebellar ataxia type 1.

Author

Ripolone, Michela, Lucchini, Valeria, Ronchi, Dario, Fagiolari, Gigliola, Bordoni, Andreina, Fortunato, Francesco, Mondello, Stefania, Bonato, Sara, Meregalli, Mirella, Torrente, Yvan, Corti, Stefania, Comi, Giacomo P., Moggio, Maurizio, and Sciacco, Monica

Published

2018

11. Ataluren treatment of patients with nonsense mutation dystrophinopathy.

Author

Bushby, Katharine, Finkel, Richard, Wong, Brenda, Barohn, Richard, Campbell, Craig, Comi, Giacomo P., Connolly, Anne M., Day, John W., Flanigan, Kevin M., Goemans, Nathalie, Jones, Kristi J., Mercuri, Eugenio, Quinlivan, Ros, Renfroe, James B., Russman, Barry, Ryan, Monique M., Tulinius, Mar, Voit, Thomas, Moore, Steven A., and Lee Sweeney, H.

Abstract

ABSTRACT Introduction: Dystrophinopathy is a rare, severe muscle disorder, and nonsense mutations are found in 13% of cases. Ataluren was developed to enable ribosomal readthrough of premature stop codons in nonsense mutation (nm) genetic disorders. Methods: Randomized, double-blind, placebo-controlled study; males ≥5 years with nm-dystrophinopathy received study drug orally 3 times daily, ataluren 10, 10, 20 mg/kg ( N = 57); ataluren 20, 20, 40 mg/kg ( N = 60); or placebo ( N = 57) for 48 weeks. The primary endpoint was change in 6-Minute Walk Distance (6MWD) at Week 48. Results: Ataluren was generally well tolerated. The primary endpoint favored ataluren 10, 10, 20 mg/kg versus placebo; the week 48 6MWD Δ = 31.3 meters, post hoc P = 0.056. Secondary endpoints (timed function tests) showed meaningful differences between ataluren 10, 10, 20 mg/kg, and placebo. Conclusions: As the first investigational new drug targeting the underlying cause of nm-dystrophinopathy, ataluren offers promise as a treatment for this orphan genetic disorder with high unmet medical need. Muscle Nerve 50: 477-487, 2014 [ABSTRACT FROM AUTHOR]

Published

2014

12. Myoclonus in mitochondrial disorders.

Author

Mancuso, Michelangelo, Orsucci, Daniele, Angelini, Corrado, Bertini, Enrico, Catteruccia, Michela, Pegoraro, Elena, Carelli, Valerio, Valentino, Maria L., Comi, Giacomo P., Minetti, Carlo, Bruno, Claudio, Moggio, Maurizio, Ienco, Elena Caldarazzo, Mongini, Tiziana, Vercelli, Liliana, Primiano, Guido, Servidei, Serenella, Tonin, Paola, Scarpelli, Mauro, and Toscano, Antonio

Abstract

ABSTRACT Myoclonus is a possible manifestation of mitochondrial disorders, and its presence is considered, in association with epilepsy and the ragged red fibers, pivotal for the syndromic diagnosis of MERRF (myoclonic epilepsy with ragged red fibers). However, its prevalence in mitochondrial diseases is not known. The aims of this study are the evaluation of the prevalence of myoclonus in a big cohort of mitochondrial patients and the clinical characterization of these subjects. Based on the database of the 'Nation-wide Italian Collaborative Network of Mitochondrial Diseases,' we reviewed the clinical and molecular data of mitochondrial patients with myoclonus among their clinical features. Myoclonus is a rather uncommon clinical feature of mitochondrial diseases (3.6% of 1,086 patients registered in our database). It is not strictly linked to a specific genotype or phenotype, and only 1 of 3 patients with MERRF harbors the 8344A>G mutation (frequently labeled as 'the MERRF mutation'). Finally, myoclonus is not inextricably linked to epilepsy in MERRF patients, but more to cerebellar ataxia. In a myoclonic patient, evidences of mitochondrial dysfunction must be investigated, even though myoclonus is not a common sign of mitochondriopathy. Clinical, histological, and biochemical data may predict the finding of a mitochondrial or nuclear DNA mutation. Finally, this study reinforces the notion that myoclonus is not inextricably linked to epilepsy in MERRF patients, and therefore the term 'myoclonic epilepsy' seems inadequate and potentially misleading. © 2014 International Parkinson and Movement Disorder Society [ABSTRACT FROM AUTHOR]

Published

2014

13. Molecular, genetic and stem cell-mediated therapeutic strategies for spinal muscular atrophy ( SMA).

Author

Zanetta, Chiara, Riboldi, Giulietta, Nizzardo, Monica, Simone, Chiara, Faravelli, Irene, Bresolin, Nereo, Comi, Giacomo P., and Corti, Stefania

Subjects

STEM cells, THERAPEUTICS, SPINAL muscular atrophy, MOTOR neuron diseases, MORTALITY, CLINICAL trials, GENETIC mutation

Abstract

Spinal muscular atrophy ( SMA) is an autosomal recessive motor neuron disease. It is the first genetic cause of infant mortality. It is caused by mutations in the survival motor neuron 1 ( SMN1) gene, leading to the reduction of SMN protein. The most striking component is the loss of alpha motor neurons in the ventral horn of the spinal cord, resulting in progressive paralysis and eventually premature death. There is no current treatment other than supportive care, although the past decade has seen a striking advancement in understanding of both SMA genetics and molecular mechanisms. A variety of disease modifying interventions are rapidly bridging the translational gap from the laboratory to clinical trials. In this review, we would like to outline the most interesting therapeutic strategies that are currently developing, which are represented by molecular, gene and stem cell-mediated approaches for the treatment of SMA. [ABSTRACT FROM AUTHOR]

Published

2014

14. Long-Standing Balancing Selection in the THBS 4 Gene: Influence on Sex-Specific Brain Expression and Gray Matter Volumes in Alzheimer Disease.

Author

Cagliani, Rachele, Guerini, Franca R., Rubio‐Acero, Raquel, Baglio, Francesca, Forni, Diego, Agliardi, Cristina, Griffanti, Ludovica, Fumagalli, Matteo, Pozzoli, Uberto, Riva, Stefania, Calabrese, Elena, Sikora, Martin, Casals, Ferran, Comi, Giacomo P., Bresolin, Nereo, Cáceres, Mario, Clerici, Mario, and Sironi, Manuela

Abstract

ABSTRACT The THBS4 gene encodes a glycoprotein involved in inflammatory responses and synaptogenesis. THBS4 is expressed at higher levels in the brain of humans compared with nonhuman primates, and the protein accumulates in β-amyloid plaques. We analyzed THBS4 genetic variability in humans and show that two haplotypes (hap1 and hap2) are maintained by balancing selection and modulate THBS4 expression in lymphocytes. Indeed, the balancing selection region covers a predicted transcriptional enhancer. In humans, but not in macaques and chimpanzees, THBS4 brain expression increases with age, and variants in the balancing selection region interact with sex in influencing THBS4 expression ( pinteraction = 0.038), with hap1 homozygous females showing lowest expression. In Alzheimer disease ( AD) patients, significant interactions between sex and THBS4 genotype were detected for peripheral gray matter ( pinteraction = 0.014) and total gray matter ( pinteraction = 0.012) volumes. Similarly to the gene expression results, the interaction is mainly mediated by hap1 homozygous AD females, who show reduced volumes. Thus, the balancing selection target in THBS4 is likely represented by one or more variants that regulate tissue-specific and sex-specific gene expression. The selection signature associated with THBS4 might not be related to AD pathogenesis, but rather to inflammatory responses. [ABSTRACT FROM AUTHOR]

Published

2013

15. Mitochondrial Fusion Proteins and Human Diseases.

Author

Ranieri, Michela, Brajkovic, Simona, Riboldi, Giulietta, Ronchi, Dario, Rizzo, Federica, Bresolin, Nereo, Corti, Stefania, and Comi, Giacomo P.

Abstract

Mitochondria are highly dynamic, complex organelles that continuously alter their shape, ranging between two opposite processes, fission and fusion, in response to several stimuli and the metabolic demands of the cell. Alterations inmitochondrial dynamics due tomutations in proteins involved in the fusion-fission machinery represent an important pathogenic mechanism of human diseases. The most relevant proteins involved in the mitochondrial fusion process are three GTPase dynamin-like proteins: mitofusin 1 (MFN1) and 2 (MFN2), located in the outermitochondrial membrane, and optic atrophy protein 1 (OPA1), in the inner membrane. An expanding number of degenerative disorders are associated with mutations in the genes encoding MFN2 and OPA1, including Charcot-Marie-Tooth disease type 2A and autosomal dominant optic atrophy. While these disorders can still be considered rare, defective mitochondrial dynamics seem to play a significant role in the molecular and cellular pathogenesis of more common neurodegenerative diseases, for example, Alzheimer's and Parkinson's diseases. This review provides an overview of the basic molecular mechanisms involved in mitochondrial fusion and focuses on the alteration in mitochondrial DNA amount resulting from impairment of mitochondrial dynamics. We also review the literature describing the main disorders associated with the disruption of mitochondrial fusion. [ABSTRACT FROM AUTHOR]

Published

2013

16. Generation of skeletal muscle cells from embryonic and induced pluripotent stem cells as an in vitro model and for therapy of muscular dystrophies.

Author

Salani, Sabrina, Donadoni, Chiara, Rizzo, Federica, Bresolin, Nereo, Comi, Giacomo P., and Corti, Stefania

Subjects

SKELETAL muscle, MYOBLASTS, EMBRYONIC stem cells, INDUCED pluripotent stem cells, MUSCULAR dystrophy treatment, CELL differentiation, MUSCLE regeneration

Abstract

Introduction, Transdifferentiation of somatic cells in skeletal myoblasts, Myogenic cell induction from ESCs The first method: generation of MMPs from ESCs and their differentiation into myogenic cells Isolation of MMPs, Differentiation into skeletal myoblasts, , The second method: EB generation and differentiation into skeletal muscle Formation of EBs, Differentiation of EBs into skeletal myoblasts, , , Protocols for myogenic cell induction from iPSCs, Mouse and human-pluripotent derived myocytes as an in vitro model of MDs, Therapeutic development based on ESC- or iPSC-derived cells, Conclusion, Muscular dystrophies (MDs) are a heterogeneous group of inherited disorders characterized by progressive muscle wasting and weakness likely associated with exhaustion of muscle regeneration potential. At present, no cures or efficacious treatments are available for these diseases, but cell transplantation could be a potential therapeutic strategy. Transplantation of myoblasts using satellite cells or other myogenic cell populations has been attempted to promote muscle regeneration, based on the hypothesis that the donor cells repopulate the muscle and contribute to its regeneration. Embryonic stem cells (ESCs) and more recently induced pluripotent stem cells (iPSCs) could generate an unlimited source of differentiated cell types, including myogenic cells. Here we review the literature regarding the generation of myogenic cells considering the main techniques employed to date to elicit efficient differentiation of human and murine ESCs or iPSCs into skeletal muscle. We also critically analyse the possibility of using these cellular populations as an alternative source of myogenic cells for cell therapy of MDs. [ABSTRACT FROM AUTHOR]

Published

2012

17. New motor outcome function measures in evaluation of Late-Onset Pompe disease before and after enzyme replacement therapy.

Author

Angelini, Corrado, Semplicini, Claudio, Ravaglia, Sabrina, Moggio, Maurizio, Comi, Giacomo P., Musumeci, Olimpia, Pegoraro, Elena, Tonin, Paola, Filosto, Massimiliano, Servidei, Serenella, Morandi, Lucia, Crescimanno, Grazia, Marrosu, Giovanni, Siciliano, Gabriele, Mongini, Tiziana, and Toscano, ANTONIO

Abstract

Introduction: The clinical course of late-onset Pompe disease is heterogeneous, and new clinical outcome measures are needed to evaluate enzyme replacement therapy (ERT). Methods: We correlated the 6-Minute Walk Test (6MWT), Walton and Gardner-Medwin (WGM) score, and GSGC (Gait, Stairs, Gower, Chair) scores in 40 patients. Results: At baseline, the GSGC score correlated with both WGM ( P < 0.001, n = 33) and 6MWT ( P < 0.001, n = 26). After 1 year of ERT, we observed a significant change in gait, stairs and chair performance on the GSGC scale. The 6MWT significantly increased from 319 to 371 meters in 32 patients, and the WGM score was reduced. Conclusions: GSGC is a group of functional tests that requires only a few minutes to perform, therefore, this score might be a good indicator to be used in future studies. Muscle Nerve 45: 831-834, 2012 [ABSTRACT FROM AUTHOR]

Published

2012

18. Mutations of mitochondrial DNA polymerase γA are a frequent cause of autosomal dominant or recessive progressive external ophthalmoplegia.

Author

Lamantea, Eleonora, Tiranti, Valeria, Bordoni, Andreina, Toscano, Antonio, Bono, Francesco, Servidei, Serena, Papadimitriou, Alex, Spelbrink, Hans, Silvestri, Laura, Casari, Giorgio, Comi, Giacomo P., and Zeviani, Massimo

Published

2002

19. β-enolase deficiency, a new metabolic myopathy of distal glycolysis.

Author

Comi, Giacomo P., Fortunato, Francesco, Lucchiari, Sabrina, Bordoni, Andreina, Prelle, Alessandro, Jann, Stefano, Keller, Angélica, Ciscato, Patrizia, Galbiati, Sara, Chiveri, Luca, Torrente, Yvan, Scarlato, Guglielmo, and Bresolin, Nereo

Published

2001

20. Cytochrome c oxidase subunit I microdeletion in a patient with motor neuron disease.

Author

Comi, Giacomo P., Bordoni, Andreina, Salani, Sabrina, Franceschina, Liliana, Sciacco, Monica, Prelle, Alessandro, Fortunato, Francesco, Zeviani, Massimo, Napoli, Laura, Bresolin, Nereo, Moggio, Maurizio, Ausenda, Carlo D., Taanman, Jan-Willem, Scarlato, Guglielmo, Comi, G P, Bordoni, A, Salani, S, Franceschina, L, Sciacco, M, and Prelle, A

Published

1998

21. Spinal muscular atrophy with respiratory distress type 1: Clinical phenotypes, molecular pathogenesis and therapeutic insights.

Author

Saladini, Matteo, Nizzardo, Monica, Govoni, Alessandra, Taiana, Michela, Bresolin, Nereo, Comi, Giacomo P., and Corti, Stefania

Subjects

SPINAL muscular atrophy, PATHOLOGY, MUSCULAR atrophy, NEUROMUSCULAR diseases, MOTOR neuron diseases, MACHINE translating, MUSCLE strength, NEUROMUSCULAR transmission

Abstract

Spinal muscular atrophy with respiratory distress type 1 (SMARD1) is a rare autosomal recessive neuromuscular disorder caused by mutations in the IGHMBP2 gene, which encodes immunoglobulin μ‐binding protein 2, leading to progressive spinal motor neuron degeneration. We review the data available in the literature about SMARD1. The vast majority of patients show an onset of typical symptoms in the first year of life. The main clinical features are distal muscular atrophy and diaphragmatic palsy, for which permanent supportive ventilation is required. No effective treatment is available yet, but novel therapeutic approaches, such as gene therapy, have shown encouraging results in preclinical settings and thus represent possible methods for treating SMARD1. Significant advancements in the understanding of both the SMARD1 clinical spectrum and its molecular mechanisms have allowed the rapid translation of preclinical therapeutic strategies to human patients to improve the poor prognosis of this devastating disease. [ABSTRACT FROM AUTHOR]

Published

2020

22. A region in the dystrophin gene major hot spot harbors a cluster of deletion breakpoints and generates double-strand breaks in yeast.

Author

Sironi, Manuela, Pozzoli, Uberto, Comi, Giacomo P., Riva, Stefania, Bordoni, Andreina, Bresolin, Nereo, and Nag, Dilip K.

Subjects

MOLECULES, DYSTROPHIN genes, INTRONS, DOUBLE-stranded RNA, MEIOSIS

Abstract

This article presents a study on the molecular events that lead to deletion formation in the dystrophin gene major hot spot. The study found that a region in intron 47 has the abilty to induce double-strand breaks (DSB) during meiosis. It is suggested that DSB is not associated with secondary structure. Conclusions and significance of the study are presented.

Published

2006

23. Multipotentiality, homing properties, and pyramidal neurogenesis of CNS-derived LeX(ssea-1)+/CXCR4+ stem cells.

Author

Corti, Stefania, Locatelli, Federica, Papadimitriou, Dimitra, Donadoni, Chiara, Del Bo, Roberto, Fortunato, Francesco, Strazzer, Sandra, Salani, Sabrina, Bresolin, Nereo, and Comi, Giacomo P.

Subjects

NEURAL stem cells, ANTIGENS, CENTRAL nervous system, NEURONS, CELL transplantation

Abstract

Presents an isolation and characterization of a primitive neural stem cell population double positive for LewisX (LeX) and CXCR4 (CX) antigens that possesses central nervous system-homing potential and extensive neuronal-repopulating capacity in vivo. Ability of LeCX cells to acquire multiple neural and non-neural phenotypes; Intracerebroventricular transplantation of LeCX cells; Systemic transplantation of LeCX cells.

Published

2005

24. Intra-aortic injection of myoblasts in mdx mice: genetic and technetium-99m cell labeling and biodistribution.

Author

Bresolin, Nereo, Ausenda, Carlo D., Casati, Rosangela, Torrente, Yvan, DeLiso, Alberto, D'Angelo, Maria Grazia, Benti, Riccardo, Moggio, Maurizio, Baldessari, Sonia, Comi, Giacomo P., Colombo, Fabio, Gerundini, Paolo, Scarlato, Guglielmo, Bresolin, N, Ausenda, C D, Casati, R, Torrente, Y, DeLiso, A, D'Angelo, M G, and Benti, R

Published

1997

25. In vivo biolistic technique in control and mdx dystrophic mice.

Author

Ausenda, Carlo D., Bresolin, Nereo, De Liso, Alberto, D'Angelo, M. Grazia, Moggio, Maurizio, Del Bo, Roberto, Gallanti, Andrea, Comi, Giacomo P., Torrente, Yvan, Bordoni, Andreina, Scarlato, Guglielmo, Ausenda, C D, Bresolin, N, De Liso, A, D'Angelo, M G, Moggio, M, Del Bo, R, Gallanti, A, Comi, G P, and Torrente, Y

Published

1996

26. McArdle disease: the mutation spectrum of PYGM in a large Italian cohort.

Author

Bruno, Claudio, Cassandrini, Denise, Martinuzzi, Andrea, Toscano, Antonio, Moggio, Maurizio, Morandi, Lucia, Servidei, Serena, Mongini, Tiziana, Angelini, Corrado, Musumeci, Olimpia, Comi, Giacomo P., Lamperti, Costanza, Filosto, Massimiliano, Zara, Federico, and Minetti, Carlo

Abstract

Deficiency of the muscle isozyme of glycogen phosphorylase is causative of McArdle disease or Glycogen storage disease type V (GSD-V), the most common autosomal recessive disorder of glycogen metabolism. The typical clinical presentation is characterized by exercise intolerance with cramps, and recurrent myoglobinuria. To date, 46 mutations in the PYGM gene have been detected in GSD-V patients. We report the mutational spectrum in 68 Italian patients. We identified 30 different mutations in the PYGM gene, including 19 mutations that have not been reported previously. The novel mutations include: eight missense mutations (c.475G>A, p.G159R; c.689C>G, p.P230R; c.1094C>T, p.A365E; c.1151C>A, p.A384D; c.1182C>T, p.R428C; c.1471C>T, p.R491C; c.2444A>C, p.D815A; c.2477G>C, p.W826S), two nonsense mutations (c.1475G>A, p.W492X; c.1627A>T, p.K543X), five splice site mutations (c.855 +1G>C; c.1092 +1G>A; c. 1093-1G>T; c.1239 +1G>A; c.2380 +1G>A), and four deletions (c.715_717delGTC, p.V239del; c.304delA, p.N102DfsX4; c.1970_2177del, p.V657_G726; c.2113_2114delGG, p.G705RfsX16). Whereas we confirmed lack of direct correlation between the clinical phenotype and the genotype, we also found that the so-called 'common mutation' (p.R50X) accounted for about 43% of alleles in our cohort and that no population-related mutations are clearly identified in Italian patients. © 2006 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2006

27. Mutation finding in patients with dysferlin deficiency and role of the dysferlin interacting proteins annexin A1 and A2 in muscular dystrophies.

Author

Cagliani, Rachele, Magri, Francesca, Toscano, Antonio, Merlini, Luciano, Fortunato, Francesco, Lamperti, Costanza, Rodolico, Carmelo, Prelle, Alessandro, Sironi, Manuela, Aguennouz, Mohammed, Ciscato, Patrizia, Uncini, Antonino, Moggio, Maurizio, Bresolin, Nereo, and Comi, Giacomo P.

Abstract

Mutations in the DYSF gene underlie two main muscle diseases: Limb Girdle Muscular Dystrophy (LGMD) 2B and Miyoshi myopathy (MM). Dysferlin is involved in muscle membrane-repair and is thought to interact with other dysferlin molecules and annexins A1 and A2 at the sarcolemma. We performed genotype/phenotype correlations in a large cohort of dysferlinopathic patients and explored the possible role of annexins as modifier factors in LGMD-2B and MM. In particular, clinical examination, expression of sarcolemmal proteins and genetic analysis were performed on 27 dysferlinopathic subjects. Expression of A1 and A2 annexins was investigated in LGMD-2B/MM subjects and in patients with other muscle disorders. We identified 24 different DYSF mutations, 10 of them being novel. We observed no clear correlation between mutation type and clinical phenotype, but MM patients were found to display muscle symptoms significantly earlier in life than LGMD subjects. Remarkably, dysferlinopathic patients and subjects suffering from other muscular disorders expressed higher levels of both annexins compared to controls; a significant correlation was observed between annexin expression levels and clinical severity scores. Also, annexin amounts paralleled the degree of muscle histopathologic changes. In conclusion, our data indicate that the pathogenesis of different inherited and acquired muscle disorders involves annexin overexpression, probably because these proteins actively participate in the plasmalemma repair process. The positive correlation between annexin A1 and A2 and clinical severity, as well as muscle histopathology, suggests that their level may be a prognostic indicator of disease. © 2005 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2005

28. A collection of 33 novel human mtDNA homoplasmic variants.

Author

Crimi, Marco, Sciacco, Monica, Galbiati, Sara, Bordoni, Andreina, Malferrari, Giulia, Bo, Roberto Del, Biunno, Ida, Bresolin, Nereo, and Comi, Giacomo P.

Published

2002