Your search keyword '"Angelo Quattrini"' showing total 259 results

1. Circulating MAIT cells in multiple sclerosis and amyotrophic lateral sclerosis

Author

Davide De Federicis, Claudia Bassani, Rosaria Rita Chiarelli, Federico Montini, Antonino Giordano, Federica Esposito, Nilo Riva, Angelo Quattrini, Vittorio Martinelli, Massimo Filippi, and Cinthia Farina

Subjects

amyotrophic lateral sclerosis, blood, CD161, MAIT cells, progressive multiple sclerosis, Immunologic diseases. Allergy, RC581-607

Abstract

Neurological disorders, including multiple sclerosis (MS) and amyotrophic lateral sclerosis (ALS), may be associated with alterations in blood cell composition and phenotype. Here, we focused our attention on circulating mucosal-associated invariant T (MAIT) cells, a CD8+ T cell memory population expressing the invariant Vα7.2 region in the T cell receptor and high surface levels of the CD161 marker. Transcriptomics data relative to peripheral blood mononuclear cells (PBMC) highlighted downregulation of CD161 and other MAIT-associated markers in progressive MS and not relapsing remitting (RR)-MS when gene expressions relative to each disease course were compared to those from healthy controls. Multiparametric flow cytometry of freshly isolated PBMC samples from untreated RR-MS, primary or secondary progressive MS (PP- or SP-MS), ALS and age- and sex-matched healthy controls revealed specific loss of circulating CD8+ MAIT cells in PP-MS and no other MS courses or another neurological disorder such as ALS. Overall, these observations point to the existence of immunological changes in blood specific for the primary progressive course of MS that may support clinical definition of disease.

Published

2024

2. The Evolution of Technology‐Driven In Vitro Models for Neurodegenerative Diseases

Author

Eleonora De Vitis, Antonella Stanzione, Alessandro Romano, Angelo Quattrini, Giuseppe Gigli, Lorenzo Moroni, Francesca Gervaso, and Alessandro Polini

Subjects

bioinks, bioprinting, hydrogels, in vitro models, microfabrication, neurodegenerative diseases, Science

Abstract

Abstract The alteration in the neural circuits of both central and peripheral nervous systems is closely related to the onset of neurodegenerative disorders (NDDs). Despite significant research efforts, the knowledge regarding NDD pathological processes, and the development of efficacious drugs are still limited due to the inability to access and reproduce the components of the nervous system and its intricate microenvironment. 2D culture systems are too simplistic to accurately represent the more complex and dynamic situation of cells in vivo and have therefore been surpassed by 3D systems. However, both models suffer from various limitations that can be overcome by employing two innovative technologies: organ‐on‐chip and 3D printing. In this review, an overview of the advantages and shortcomings of both microfluidic platforms and extracellular matrix‐like biomaterials will be given. Then, the combination of microfluidics and hydrogels as a new synergistic approach to study neural disorders by analyzing the latest advances in 3D brain‐on‐chip for neurodegenerative research will be explored.

Published

2024

3. Neuronal models of TDP-43 proteinopathy display reduced axonal translation, increased oxidative stress, and defective exocytosis

Author

Alessandra Pisciottani, Laura Croci, Fabio Lauria, Chiara Marullo, Elisa Savino, Alessandro Ambrosi, Paola Podini, Marta Marchioretto, Filippo Casoni, Ottavio Cremona, Stefano Taverna, Angelo Quattrini, Jean-Michel Cioni, Gabriella Viero, Franca Codazzi, and G. Giacomo Consalez

Subjects

amyotrophic lateral sclerosis, TDP-43 proteinopathy, cortical neurons, axonal translation, oxidative stress, synaptic function, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Amyotrophic lateral sclerosis (ALS) is a progressive, lethal neurodegenerative disease mostly affecting people around 50–60 years of age. TDP-43, an RNA-binding protein involved in pre-mRNA splicing and controlling mRNA stability and translation, forms neuronal cytoplasmic inclusions in an overwhelming majority of ALS patients, a phenomenon referred to as TDP-43 proteinopathy. These cytoplasmic aggregates disrupt mRNA transport and localization. The axon, like dendrites, is a site of mRNA translation, permitting the local synthesis of selected proteins. This is especially relevant in upper and lower motor neurons, whose axon spans long distances, likely accentuating their susceptibility to ALS-related noxae. In this work we have generated and characterized two cellular models, consisting of virtually pure populations of primary mouse cortical neurons expressing a human TDP-43 fusion protein, wt or carrying an ALS mutation. Both forms facilitate cytoplasmic aggregate formation, unlike the corresponding native proteins, giving rise to bona fide primary culture models of TDP-43 proteinopathy. Neurons expressing TDP-43 fusion proteins exhibit a global impairment in axonal protein synthesis, an increase in oxidative stress, and defects in presynaptic function and electrical activity. These changes correlate with deregulation of axonal levels of polysome-engaged mRNAs playing relevant roles in the same processes. Our data support the emerging notion that deregulation of mRNA metabolism and of axonal mRNA transport may trigger the dying-back neuropathy that initiates motor neuron degeneration in ALS.

Published

2023

4. Neural precursor cells tune striatal connectivity through the release of IGFBPL1

Author

Erica Butti, Stefano Cattaneo, Marco Bacigaluppi, Marco Cambiaghi, Giulia Maria Scotti, Elena Brambilla, Francesca Ruffini, Giacomo Sferruzza, Maddalena Ripamonti, Fabio Simeoni, Laura Cacciaguerra, Aurora Zanghì, Angelo Quattrini, Riccardo Fesce, Paola Panina-Bordignon, Francesca Giannese, Davide Cittaro, Tanja Kuhlmann, Patrizia D’Adamo, Maria Assunta Rocca, Stefano Taverna, and Gianvito Martino

Subjects

Science

Abstract

The physiological role of endogenous neural protenitor cells of the subventricular zone in adult stage is not fully understood. Here the authors show that in mice, these cells tune neuronal activity of the striatum via insulin-like growth factor binding protein-like 1 and cognitive functions.

Published

2022

5. Restoring calcium homeostasis in Purkinje cells arrests neurodegeneration and neuroinflammation in the ARSACS mouse model

Author

Andrea Del Bondio, Fabiana Longo, Daniele De Ritis, Erica Spirito, Paola Podini, Bernard Brais, Angela Bachi, Angelo Quattrini, and Francesca Maltecca

Subjects

Cell biology, Neuroscience, Medicine

Abstract

Autosomal recessive spastic ataxia of Charlevoix-Saguenay (ARSACS) is caused by mutations in SACS gene encoding sacsin, a huge protein highly expressed in cerebellar Purkinje cells (PCs). Patients with ARSACS, as well as mouse models, display early degeneration of PCs, but the underlying mechanisms remain unexplored, with no available treatments. In this work, we demonstrated aberrant calcium (Ca2+) homeostasis and its impact on PC degeneration in ARSACS. Mechanistically, we found pathological elevation in Ca2+-evoked responses in Sacs–/– PCs as the result of defective mitochondria and ER trafficking to distal dendrites and strong downregulation of key Ca2+ buffer proteins. Alteration of cytoskeletal linkers, which we identified as specific sacsin interactors, likely account for faulty organellar trafficking in Sacs–/– cerebellum. Based on this pathogenetic cascade, we treated Sacs–/– mice with Ceftriaxone, a repurposed drug that exerts neuroprotection by limiting neuronal glutamatergic stimulation and, thus, Ca2+ fluxes into PCs. Ceftriaxone treatment significantly improved motor performances of Sacs–/– mice, at both pre- and postsymptomatic stages. We correlated this effect to restored Ca2+ homeostasis, which arrests PC degeneration and attenuates secondary neuroinflammation. These findings disclose key steps in ARSACS pathogenesis and support further optimization of Ceftriaxone in preclinical and clinical settings for the treatment of patients with ARSACS.

Published

2023

6. A novel GRN mutation in an Italian patient with non-fluent variant of primary progressive aphasia at onset: a longitudinal case report

Author

Veronica Castelnovo, Elisa Canu, Teuta Domi, Laura Pozzi, Francesca Vignaroli, Edoardo Gioele Spinelli, Alma Ghirelli, Giacomo Tondo, Cristoforo Comi, Nilo Riva, Angelo Quattrini, Paola Carrera, Massimo Filippi, and Federica Agosta

Subjects

progranulin, primary progressive aphasia, longitudinal, frontotemporal dementia, case report, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

ObjectivesWe report the clinical presentation and evolution of a case with a novel Progranulin gene (GRN) mutation and non-fluent language disturbances at onset.Materials and methodsA 60 year-old, white patient was followed due to a history of language disturbances. Eighteen months after onset, the patient underwent FDG positron emission tomography (PET), and at month 24 was hospitalized to perform neuropsychological evaluation, brain 3 T MRI, lumbar puncture for cerebrospinal fluid (CSF) analysis, and genotyping. At month 31, the patient repeated the neuropsychological evaluation and brain MRI.ResultsAt onset the patient complained prominent language production difficulties, such as effortful speech and anomia. At month 18, FDG-PET showed left fronto-temporal and striatal hypometabolism. At month 24, the neuropsychological evaluation reported prevalent speech and comprehension deficits. Brain MRI reported left fronto-opercular and striatal atrophy, and left frontal periventricular white matter hyperintensities (WMHs). Increased CSF total tau level was observed. Genotyping revealed a new GRN c.1018delC (p.H340TfsX21) mutation. The patient received a diagnosis of non-fluent variant of primary progressive aphasia (nfvPPA). At month 31, language deficits worsened, together with attention and executive functions. The patient presented also with behavioral disturbances, and a progressive atrophy in the left frontal-opercular and temporo-mesial region.Discussion and conclusionThe new GRN p.H340TfsX21 mutation resulted in a case of nfvPPA characterized by fronto-temporal and striatal alterations, typical frontal asymmetric WMHs, and a fast progression toward a widespread cognitive and behavioral impairment, which reflects a frontotemporal lobar degeneration. Our findings extend the current knowledge of the phenotypic heterogeneity among GRN mutation carriers.

Published

2023

7. Neutrophils predominate the immune signature of cerebral thrombi in COVID-19 stroke patients

Author

Angela Genchi, Aurora Semerano, Ghil Schwarz, Beatrice Dell’Acqua, Giorgia Serena Gullotta, Michela Sampaolo, Enzo Boeri, Angelo Quattrini, Francesca Sanvito, Susanna Diamanti, Andrea Bergamaschi, Stefano Grassi, Paola Podini, Pietro Panni, Caterina Michelozzi, Franco Simionato, Francesco Scomazzoni, Paolo Remida, Luca Valvassori, Andrea Falini, Carlo Ferrarese, Patrik Michel, Guillaume Saliou, Steven Hajdu, Simone Beretta, Luisa Roveri, Massimo Filippi, Davide Strambo, Gianvito Martino, and Marco Bacigaluppi

Subjects

SARS-CoV2, COVID-19, Thrombosis, Neutrophils, Ischemic stroke, Endovascular treatment, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Coronavirus disease 2019 (COVID-19) is associated with an increased risk of thrombotic events. Ischemic stroke in COVID-19 patients entails high severity and mortality rates. Here we aimed to analyze cerebral thrombi of COVID-19 patients with large vessel occlusion (LVO) acute ischemic stroke to expose molecular evidence for SARS-CoV-2 in the thrombus and to unravel any peculiar immune-thrombotic features. We conducted a systematic pathological analysis of cerebral thrombi retrieved by endovascular thrombectomy in patients with LVO stroke infected with COVID-19 (n = 7 patients) and non-covid LVO controls (n = 23). In thrombi of COVID-19 patients, the SARS-CoV-2 docking receptor ACE2 was mainly expressed in monocytes/macrophages and showed higher expression levels compared to controls. Using polymerase chain reaction and sequencing, we detected SARS-CoV-2 Clade20A, in the thrombus of one COVID-19 patient. Comparing thrombus composition of COVID-19 and control patients, we noted no overt differences in terms of red blood cells, fibrin, neutrophil extracellular traps (NETs), von Willebrand Factor (vWF), platelets and complement complex C5b-9. However, thrombi of COVID-19 patients showed increased neutrophil density (MPO+ cells) and a three-fold higher Neutrophil-to-Lymphocyte Ratio (tNLR). In the ROC analysis both neutrophils and tNLR had a good discriminative ability to differentiate thrombi of COVID-19 patients from controls. In summary, cerebral thrombi of COVID-19 patients can harbor SARS-CoV2 and are characterized by an increased neutrophil number and tNLR and higher ACE2 expression. These findings suggest neutrophils as the possible culprit in COVID-19-related thrombosis. Graphical Abstract

Published

2022

8. Clinical and pathological findings in neurolymphomatosis: Preliminary association with gene expression profiles in sural nerves

Author

Federica Cerri, Francesco Gentile, Ferdinando Clarelli, Silvia Santoro, Yuri Matteo Falzone, Giorgia Dina, Alessandro Romano, Teuta Domi, Laura Pozzi, Raffaella Fazio, Paola Podini, Melissa Sorosina, Paola Carrera, Federica Esposito, Nilo Riva, Chiara Briani, Tiziana Cavallaro, Massimo Filippi, and Angelo Quattrini

Subjects

lymphoproliferative disorders, non-hodgkin lymphoma, ribosomal proteins, neuropathy, nerve biopsy, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Although inflammation appears to play a role in neurolymphomatosis (NL), the mechanisms leading to degeneration in the peripheral nervous system are poorly understood. The purpose of this exploratory study was to identify molecular pathways underlying NL pathogenesis, combining clinical and neuropathological investigation with gene expression (GE) studies. We characterized the clinical and pathological features of eight patients with NL. We further analysed GE changes in sural nerve biopsies obtained from a subgroup of NL patients (n=3) and thirteen patients with inflammatory neuropathies as neuropathic controls. Based on the neuropathic symptoms and signs, NL patients were classified into three forms of neuropathy: chronic symmetrical sensorimotor polyneuropathy (SMPN, n=3), multiple mononeuropathy (MN, n=4) and acute motor-sensory axonal neuropathy (AMSAN, n=1). Predominantly diffuse malignant cells infiltration of epineurium was present in chronic SMPN, whereas endoneurial perivascular cells invasion was observed in MN. In contrast, diffuse endoneurium malignant cells localization occurred in AMSAN. We identified alterations in the expression of 1266 genes, with 115 up-regulated and 1151 down-regulated genes, which were mainly associated with ribosomal proteins (RP) and olfactory receptors (OR) signaling pathways, respectively. Among the top up-regulated genes were actin alpha 1 skeletal muscle (ACTA1) and desmin (DES). Similarly, in NL nerves ACTA1, DES and several RPs were highly expressed, associated with endothelial cells and pericytes abnormalities. Peripheral nerve involvement may be due to conversion towards a more aggressive phenotype, potentially explaining the poor prognosis. The candidate genes reported in this study may be a source of clinical biomarkers for NL.

Published

2022

9. Tako-Tsubo Syndrome in Amyotrophic Lateral Sclerosis: Single-Center Case Series and Brief Literature Review

Author

Giovanni Napoli, Martina Rubin, Gianni Cutillo, Paride Schito, Tommaso Russo, Angelo Quattrini, Massimo Filippi, and Nilo Riva

Subjects

motor neuron disease, autonomic system, mortality, non-invasive ventilation, PEG, NIMV, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Amyotrophic lateral sclerosis (ALS) is a neurodegenerative disease with variable phenotypic expressions which has been associated with autonomic dysfunction. The cardiovascular system seems to be affected especially in the context of bulbar involvement. We describe four new cases of Tako-Tsubo syndrome (TTS) in ALS patients with an appraisal of the literature. We present a late-stage ALS patient with prominent bulbar involvement that presented TTS during hospitalization. We then retrospectively identify three additional ALS–TTS cases reporting relevant clinical findings. TTS cardiomyopathy has been observed in different acute neurological conditions, and the co-occurrence of ALS and TTS has already been reported. Cardiovascular autonomic dysfunctions have been described in ALS, especially in the context of an advanced diseases and with bulbar involvement. Noradrenergic hyperfunction linked to sympathetic denervation and ventilatory deficits coupled in different instances with a trigger event could play a synergistic role in the development of TTS in ALS. Sympathetic hyperfunctioning and ventilatory deficits in conjunction with cardiac autonomic nerves impairment may play a role in the development of TTS in a context of ALS.

Published

2023

10. A microfabricated multi-compartment device for neuron and Schwann cell differentiation

Author

Eleonora De Vitis, Velia La Pesa, Francesca Gervaso, Alessandro Romano, Angelo Quattrini, Giuseppe Gigli, Lorenzo Moroni, and Alessandro Polini

Subjects

Medicine, Science

Abstract

Abstract Understanding the complex communication between different cell populations and their interaction with the microenvironment in the central and peripheral nervous systems is fundamental in neuroscience research. The development of appropriate in vitro approaches and tools, able to selectively analyze and/or probe specific cells and cell portions (e.g., axons and cell bodies in neurons), driving their differentiation into specific cell phenotypes, has become therefore crucial in this direction. Here we report a multi-compartment microfluidic device where up to three different cell populations can be cultured in a fluidically independent circuit. The device allows cell migration across the compartments and their differentiation. We showed that an accurate choice of the device geometrical features and cell culture parameters allows to (1) maximize cell adhesion and proliferation of neuron-like human cells (SH-SY5Y cells), (2) control the inter-compartment cell migration of neuron and Schwann cells, (3) perform long-term cell culture studies in which both SH-SY5Y cells and primary rat Schwann cells can be differentiated towards specific phenotypes. These results can lead to a plethora of in vitro co-culture studies in the neuroscience research field, where tuning and investigating cell–cell and cell–microenvironment interactions are essential.

Published

2021

11. Selective loss of microvesicles is a major issue of the differential centrifugation isolation protocols

Author

Annamaria Nigro, Annamaria Finardi, Marzia M. Ferraro, Daniela E. Manno, Angelo Quattrini, Roberto Furlan, and Alessandro Romano

Subjects

Medicine, Science

Abstract

Abstract Microvesicles (MVs) are large extracellular vesicles differing in size, cargo and composition that share a common mechanism of release from the cells through the direct outward budding of the plasma membrane. They are involved in a variety of physiological and pathological conditions and represent promising biomarkers for diseases. MV heterogeneity together with the lack of specific markers had strongly hampered the development of effective methods for MV isolation and differential centrifugation remains the most used method to purify MVs. In this study, we analysed the capacity of the differential centrifugation method to isolate MVs from cell-conditioned medium using flow cytometry and TEM/AFM microscopy. We found that the loss of MVs (general population and/or specific subpopulations) represents a major and underestimate drawback of the differential centrifugation protocol. We demonstrate that the choice of the appropriate rotor type (fixed-angle vs swinging-bucket) and the implementation of an additional washing procedure to the first low-speed centrifugation step of the protocol allow to overcome this problem increasing the total amount of isolated vesicles and avoiding the selective loss of MV subpopulations. These parameters/procedures should be routinely employed into optimized differential centrifugation protocols to ensure isolation of the high-quantity/quality MVs for the downstream analysis/applications.

Published

2021

12. Current application of neurofilaments in amyotrophic lateral sclerosis and future perspectives

Author

Yuri Matteo Falzone, Tommaso Russo, Teuta Domi, Laura Pozzi, Angelo Quattrini, Massimo Filippi, and Nilo Riva

Subjects

amyotrophic lateral sclerosis, biomarkers, motor neuron disease, neurofilament light chain, phosphorylated neurofilament heavy chain, Neurology. Diseases of the nervous system, RC346-429

Abstract

Motor neuron disease includes a heterogeneous group of relentless progressive neurological disorders defined and characterized by the degeneration of motor neurons. Amyotrophic lateral sclerosis is the most common and aggressive form of motor neuron disease with no effective treatment so far. Unfortunately, diagnostic and prognostic biomarkers are lacking in clinical practice. Neurofilaments are fundamental structural components of the axons and neurofilament light chain and phosphorylated neurofilament heavy chain can be measured in both cerebrospinal fluid and serum. Neurofilament light chain and phosphorylated neurofilament heavy chain levels are elevated in amyotrophic lateral sclerosis, reflecting the extensive damage of motor neurons and axons. Hence, neurofilaments are now increasingly recognized as the most promising candidate biomarker in amyotrophic lateral sclerosis. The potential usefulness of neurofilaments regards various aspects, including diagnosis, prognosis, patient stratification in clinical trials and evaluation of treatment response. In this review paper, we review the body of literature about neurofilaments measurement in amyotrophic lateral sclerosis. We also discuss the open issues concerning the use of neurofilaments clinical practice, as no overall guideline exists to date; finally, we address the most recent evidence and future perspectives.

Published

2021

13. NEK1 Variants in a Cohort of Italian Patients With Amyotrophic Lateral Sclerosis

Author

Nilo Riva, Laura Pozzi, Tommaso Russo, Giovanni Battista Pipitone, Paride Schito, Teuta Domi, Federica Agosta, Angelo Quattrini, Paola Carrera, and Massimo Filippi

Subjects

motor neuron disease, frontotemporal dementia, neuromuscular diseases, neurodegenerative disorders, genetics, never in mitosis a (NIMA)-related kinase 1, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

IntroductionIn the last few years, different studies highlighted a significant enrichment of NEK1 loss of function (LoF) variants in amyotrophic lateral sclerosis (ALS), and an additional role for the p.Arg261His missense variant in the disease susceptibility. Several other missense variants have been described so far, whose pathogenic relevance remains however unclear since many of them have been reported in both patients and controls. This study aimed to investigate the presence of NEK1 variants and their correlation with phenotype in a cohort of Italian patients with ALS.MethodsWe sequenced a cohort of 350 unrelated Italian patients with ALS by next-generation sequencing (NGS) and then we analyzed the clinical features of NEK1 carriers.ResultsWe detected 20 different NEK1 rare variants (four LoF and 16 missense) in 33 unrelated patients with sporadic ALS (sALS). The four LoF variants (two frameshift and two splice-site variants) were all novel. The p.Arg261His missense variant was enriched in the patients’ cohort (p < 0.001). Excluding this variant from counting, the difference in the frequency of NEK1 rare missense variants between patients and controls was not statistically significant. NEK1 carriers had a higher frequency of flail arm (FA) phenotype compared with the other patients of the cohort (29.2% vs. 6.4%). Nine NEK1 carriers (37.5%) also harbored variants in other ALS-related genes.ConclusionThis study confirms that NEK1 LoF and p.Arg261. His missense variants are associated with ALS in an Italian ALS cohort and suggests a correlation between the presence of NEK1 variants and FA phenotype.

Published

2022

14. Retromer stabilization results in neuroprotection in a model of Amyotrophic Lateral Sclerosis

Author

Luca Muzio, Riccardo Sirtori, Davide Gornati, Simona Eleuteri, Andrea Fossaghi, Diego Brancaccio, Leonardo Manzoni, Linda Ottoboni, Luca De Feo, Angelo Quattrini, Eloise Mastrangelo, Luca Sorrentino, Emanuele Scalone, Giancarlo Comi, Luciana Marinelli, Nilo Riva, Mario Milani, Pierfausto Seneci, and Gianvito Martino

Subjects

Science

Abstract

ALS is a neurodegenerative disease characterized by loss of motor neurons. Here, the authors showed that reduced levels of the VSP35 subunit in the retromer complex is a conserved ALS feature and identified a new lead compound increasing retromer stability ameliorating the disease phenotype.

Published

2020

15. JAB1 deletion in oligodendrocytes causes senescence-induced inflammation and neurodegeneration in mice

Author

Cristina Rivellini, Emanuela Porrello, Giorgia Dina, Simona Mrakic-Sposta, Alessandra Vezzoli, Marco Bacigaluppi, Giorgia Serena Gullotta, Linda Chaabane, Letizia Leocani, Silvia Marenna, Emanuela Colombo, Cinthia Farina, Jia Newcombe, Klaus-Armin Nave, Ruggero Pardi, Angelo Quattrini, and Stefano C. Previtali

Subjects

Inflammation, Neuroscience, Medicine

Abstract

Oligodendrocytes are the primary target of demyelinating disorders, and progressive neurodegenerative changes may evolve in the CNS. DNA damage and oxidative stress are considered key pathogenic events, but the underlying molecular mechanisms remain unclear. Moreover, animal models do not fully recapitulate human diseases, complicating the path to effective treatments. Here we report that mice with cell-autonomous deletion of the nuclear COP9 signalosome component CSN5 (JAB1) in oligodendrocytes develop DNA damage and defective DNA repair in myelinating glial cells. Interestingly, oligodendrocytes lacking JAB1 expression underwent a senescence-like phenotype that fostered chronic inflammation and oxidative stress. These mutants developed progressive CNS demyelination, microglia inflammation, and neurodegeneration, with severe motor deficits and premature death. Notably, blocking microglia inflammation did not prevent neurodegeneration, whereas the deletion of p21CIP1 but not p16INK4a pathway ameliorated the disease. We suggest that senescence is key to sustaining neurodegeneration in demyelinating disorders and may be considered a potential therapeutic target.

Published

2022

16. Corneal and Epidermal Nerve Quantification in Chemotherapy Induced Peripheral Neuropathy

Author

Nilo Riva, Filippo Bonelli, Romina Mayra Lasagni Vitar, Marco Barbariga, Philippe Fonteyne, Ignazio Diego Lopez, Teuta Domi, Fabio Scarpa, Alfredo Ruggeri, Michele Reni, Magda Marcatti, Angelo Quattrini, Federica Agosta, Paolo Rama, and Giulio Ferrari

Subjects

corneal confocal microscopy, chemotherapy-induced neuropathy, skin biopsy, nerves, neurotoxicity, cornea, Medicine (General), R5-920

Abstract

Chemotherapy-induced neurotoxicity is an increasingly recognized clinical issue in oncology. in vivo confocal microscopy (IVCM) of corneal nerves has been successfully used to diagnose peripheral neuropathies, including diabetic neuropathy. The purpose of this study was to test if the combination of corneal nerve density and morphology assessed by IVCM is useful to monitor the neurotoxic effects of chemotherapy compared to epidermal nerve quantification. Overall, 95 adult patients with different cancer types were recruited from the oncology and hematology departments of the San Raffaele Hospital. Neurological examination, including clinical Total Neuropathy Score, and in vivo corneal confocal microscopy (IVCM), were performed before and after chemotherapy. In a group of 14 patients, skin biopsy was performed at the first and last visit. In the group of 14 patients who underwent both skin biopsy and corneal nerve imaging, clinical worsening (+69%, p = 0.0018) was paralleled by corneal nerve fiber (CNF) density reduction (−22%, p = 0.0457). Clinical Total neuropathy score significantly worsened from the first to the last visit (+62%, p < 0.0001). CNF length was not significantly reduced overall. However, CNF density/tortuosity ratio significantly decreased after therapy. Correlation analysis showed that the CNF density/tortuosity ratio was also correlated with the number of chemotherapy cycles (r = −0.04790, P = 0.0009). Our data confirm that in vivo corneal confocal microscopy is a helpful, non-invasive tool which shows promise for the diagnosis of chemotherapy-induced peripheral neuropathies. IVCM could allow a rapid, reproducible and non-invasive quantification of peripheral nerve pathology in chemotherapy-associated neuropathy.

Published

2022

17. MiR-146a in ALS: Contribution to Early Peripheral Nerve Degeneration and Relevance as Disease Biomarker

Author

Eleonora Giagnorio, Claudia Malacarne, Paola Cavalcante, Letizia Scandiffio, Marco Cattaneo, Viviana Pensato, Cinzia Gellera, Nilo Riva, Angelo Quattrini, Eleonora Dalla Bella, Giuseppe Lauria, Renato Mantegazza, Silvia Bonanno, and Stefania Marcuzzo

Subjects

amyotrophic lateral sclerosis, microRNA-146a, axon degeneration, biomarker, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Amyotrophic lateral sclerosis (ALS) is characterized by the progressive, irreversible loss of upper and lower motor neurons (UMNs, LMNs). MN axonal dysfunctions are emerging as relevant pathogenic events since the early ALS stages. However, the exact molecular mechanisms leading to MN axon degeneration in ALS still need to be clarified. MicroRNA (miRNA) dysregulation plays a critical role in the pathogenesis of neuromuscular diseases. These molecules represent promising biomarkers for these conditions since their expression in body fluids consistently reflects distinct pathophysiological states. Mir-146a has been reported to modulate the expression of the NFL gene, encoding the light chain of the neurofilament (NFL) protein, a recognized biomarker for ALS. Here, we analyzed miR-146a and Nfl expression in the sciatic nerve of G93A-SOD1 ALS mice during disease progression. The miRNA was also analyzed in the serum of affected mice and human patients, the last stratified relying on the predominant UMN or LMN clinical signs. We revealed a significant miR-146a increase and Nfl expression decrease in G93A-SOD1 peripheral nerve. In the serum of both ALS mice and human patients, the miRNA levels were reduced, discriminating UMN-predominant patients from the LMN ones. Our findings suggest a miR-146a contribution to peripheral axon impairment and its potential role as a diagnostic and prognostic biomarker for ALS.

Published

2023

18. Impaired flickering of the permeability transition pore causes SPG7 spastic paraplegia

Author

Irene Sambri, Filomena Massa, Francesca Gullo, Simone Meneghini, Laura Cassina, Michela Carraro, Giorgia Dina, Angelo Quattrini, Lorenzo Patanella, Annamaria Carissimo, Antonella Iuliano, Filippo Santorelli, Franca Codazzi, Fabio Grohovaz, Paolo Bernardi, Andrea Becchetti, and Giorgio Casari

Subjects

Hereditary spastic paraplegia, Paraplegin, SPG7, Mitochondria, Permeability transition pore, Synaptic vesicles, Medicine, Medicine (General), R5-920

Abstract

Background: Mutations of the mitochondrial protein paraplegin cause hereditary spastic paraplegia type 7 (SPG7), a so-far untreatable degenerative disease of the upper motoneuron with still undefined pathomechanism.The intermittent mitochondrial permeability transition pore (mPTP) opening, called flickering, is an essential process that operates to maintain mitochondrial homeostasis by reducing intra-matrix Ca2+ and reactive oxygen species (ROS) concentration, and is critical for efficient synaptic function. Methods: We use a fluorescence-based approach to measure mPTP flickering in living cells and biochemical and molecular biology techniques to dissect the pathogenic mechanism of SPG7. In the SPG7 animal model we evaluate the potential improvement of the motor defect, neuroinflammation and neurodegeneration by means of an mPTP inducer, the benzodiazepine Bz-423. Findings: We demonstrate that paraplegin is required for efficient transient opening of the mPTP, that is impaired in both SPG7 patients-derived fibroblasts and primary neurons from Spg7−/− mice. We show that dysregulation of mPTP opening at the pre-synaptic terminal impairs neurotransmitter release leading to ineffective synaptic transmission. Lack of paraplegin impairs mPTP flickering by a mechanism involving increased expression and activity of sirtuin3, which promotes deacetylation of cyclophilin D, thus hampering mPTP opening. Pharmacological treatment with Bz-423, which bypasses the activity of CypD, normalizes synaptic transmission and rescues the motor impairment of the SPG7 mouse model. Interpretation: mPTP targeting opens a new avenue for the potential therapy of this form of spastic paraplegia. Funding: Telethon Foundation grant (TGMGCSBX16TT); Dept. of Defense, US Army, grant W81XWH-18–1–0001

Published

2020

19. Counteracting roles of MHCI and CD8+ T cells in the peripheral and central nervous system of ALS SOD1G93A mice

Author

Giovanni Nardo, Maria Chiara Trolese, Mattia Verderio, Alessandro Mariani, Massimiliano de Paola, Nilo Riva, Giorgia Dina, Nicolò Panini, Eugenio Erba, Angelo Quattrini, and Caterina Bendotti

Subjects

Amyotrophic lateral sclerosis, SOD1G93A mice, Neuroinflammation, MHCI, CD8+ T cells, Motor neuron, Neurology. Diseases of the nervous system, RC346-429, Geriatrics, RC952-954.6

Abstract

Abstract Background The major histocompatibility complex I (MHCI) is a key molecule for the interaction of mononucleated cells with CD8+T lymphocytes. We previously showed that MHCI is upregulated in the spinal cord microglia and motor axons of transgenic SOD1G93A mice. Methods To assess the role of MHCI in the disease, we examined transgenic SOD1G93A mice crossbred with β2 microglobulin-deficient mice, which express little if any MHCI on the cell surface and are defective for CD8+ T cells. Results The lack of MHCI and CD8+ T cells in the sciatic nerve affects the motor axon stability, anticipating the muscle atrophy and the disease onset. In contrast, MHCI depletion in resident microglia and the lack of CD8+ T cell infiltration in the spinal cord protect the cervical motor neurons delaying the paralysis of forelimbs and prolonging the survival of SOD1G93A mice. Conclusions We provided straightforward evidence for a dual role of MHCI in the peripheral nervous system (PNS) compared to the CNS, pointing out regional and temporal differences in the clinical responses of ALS mice. These findings offer a possible explanation for the failure of systemic immunomodulatory treatments and suggest new potential strategies to prevent the progression of ALS.

Published

2018

20. Two factor-based reprogramming of rodent and human fibroblasts into Schwann cells

Author

Pietro Giuseppe Mazzara, Luca Massimino, Marta Pellegatta, Giulia Ronchi, Alessandra Ricca, Angelo Iannielli, Serena Gea Giannelli, Marco Cursi, Cinzia Cancellieri, Alessandro Sessa, Ubaldo Del Carro, Angelo Quattrini, Stefano Geuna, Angela Gritti, Carla Taveggia, and Vania Broccoli

Subjects

Science

Abstract

Schwann cells (SCs) myelinate peripheral nerve axons and offer opportunities for the treatment of injuries and demyelinating diseases but reliable and renewable sources of these cells are hard to come by. Here the authors reprogram rat, mouse and human fibroblasts into Schwann cells using two transcription factors.

Published

2017

21. The Peripheral Nervous System in Amyotrophic Lateral Sclerosis: Opportunities for Translational Research

Author

Francesco Gentile, Stefania Scarlino, Yuri Matteo Falzone, Christian Lunetta, Lucio Tremolizzo, Angelo Quattrini, and Nilo Riva

Subjects

motor neuron disease, lower motor neuron syndrome, nerve, neuropathy, CMT, distal SMA, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Although amyotrophic lateral sclerosis (ALS) has been considered as a disorder of the motor neuron (MN) cell body, recent evidences show the non-cell-autonomous pathogenic nature of the disease. Axonal degeneration, loss of peripheral axons and destruction of nerve terminals are early events in the disease pathogenic cascade, anticipating MN degeneration, and the onset of clinical symptoms. Therefore, although ALS and peripheral axonal neuropathies should be differentiated in clinical practice, they also share damage to common molecular pathways, including axonal transport, RNA metabolism and proteostasis. Thus, an extensive evaluation of the molecular events occurring in the peripheral nervous system (PNS) could be fundamental to understand the pathogenic mechanisms of ALS, favoring the discovery of potential disease biomarkers, and new therapeutic targets.

Published

2019

22. Diet, Microbiota and Brain Health: Unraveling the Network Intersecting Metabolism and Neurodegeneration

Author

Francesco Gentile, Pietro Emiliano Doneddu, Nilo Riva, Eduardo Nobile-Orazio, and Angelo Quattrini

Subjects

dysbiosis, diet, metabolism, Alzheimer’s disease, Parkinson’s disease, amyotrophic lateral sclerosis, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Increasing evidence gives support for the idea that extra-neuronal factors may affect brain physiology and its predisposition to neurodegenerative diseases. Epidemiological and experimental studies show that nutrition and metabolic disorders such as obesity and type 2 diabetes increase the risk of Alzheimer’s and Parkinson’s diseases after midlife, while the relationship with amyotrophic lateral sclerosis is uncertain, but suggests a protective effect of features of metabolic syndrome. The microbiota has recently emerged as a novel factor engaging strong interactions with neurons and glia, deeply affecting their function and behavior in these diseases. In particular, recent evidence suggested that gut microbes are involved in the seeding of prion-like proteins and their spreading to the central nervous system. Here, we present a comprehensive review of the impact of metabolism, diet and microbiota in neurodegeneration, by affecting simultaneously several aspects of health regarding energy metabolism, immune system and neuronal function. Advancing technologies may allow researchers in the future to improve investigations in these fields, allowing the buildup of population-based preventive interventions and development of targeted therapeutics to halt progressive neurologic disability.

Published

2020

23. Development of Injectable Thermosensitive Chitosan-Based Hydrogels for Cell Encapsulation

Author

Antonella Stanzione, Alessandro Polini, Velia La Pesa, Alessandro Romano, Angelo Quattrini, Giuseppe Gigli, Lorenzo Moroni, and Francesca Gervaso

Subjects

stimuli-responsive hydrogel, natural polymers, cell encapsulation, in vitro degradation, swelling ratio, injectable hydrogel, Technology, Engineering (General). Civil engineering (General), TA1-2040, Biology (General), QH301-705.5, Physics, QC1-999, Chemistry, QD1-999

Abstract

The three-dimensional complexity of the native extracellular matrix (ECM) suggests switching from 2D to 3D culture systems for providing the cells with an architecture more similar to the physiological environment. Reproducing the three-dimensionality in vitro can guarantee beneficial effects in terms of cell growth, adhesion, proliferation, and/or their differentiation. Hydrogels have the same tailorable physico-chemical and biological characteristics as ECM materials. In this study, we propose a thermoresponsive chitosan-based hydrogel that gels thanks to the addition of organic and inorganic salt solutions (beta-glycerolphosphate and sodium hydrogen carbonate) and is suitable for cell encapsulation allowing obtaining 3D culture systems. Physico-chemical analyses showed that the hydrogel formulations jellify at physiological conditions (37 °C, pH 7.4), are stable in vitro up to three weeks, have high swelling ratios and mechanical stiffness suitable for cellular encapsulation. Moreover, preliminary biological tests underlined the pronounced biocompatibility of the system. Therefore, these chitosan-based hydrogels are proposed as valid biomaterials for cell encapsulation.

Published

2020

24. Burden of Rare Variants in ALS and Axonal Hereditary Neuropathy Genes Influence Survival in ALS: Insights from a Next Generation Sequencing Study of an Italian ALS Cohort

Author

Stefania Scarlino, Teuta Domi, Laura Pozzi, Alessandro Romano, Giovanni Battista Pipitone, Yuri Matteo Falzone, Lorena Mosca, Silvana Penco, Christian Lunetta, Valeria Sansone, Lucio Tremolizzo, Raffaella Fazio, Federica Agosta, Massimo Filippi, Paola Carrera, Nilo Riva, and Angelo Quattrini

Subjects

motor neuron disease, lower motor neuron syndrome, nerve, neuropathy, CMT, distal SMA, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Although the genetic architecture of amyotrophic lateral sclerosis (ALS) is incompletely understood, recent findings suggest a complex model of inheritance in ALS, which is consistent with a multistep pathogenetic process. Therefore, the aim of our work is to further explore the architecture of ALS using targeted next generation sequencing (NGS) analysis, enriched in motor neuron diseases (MND)-associated genes which are also implicated in axonal hereditary motor neuropathy (HMN), in order to investigate if disease expression, including the progression rate, could be influenced by the combination of multiple rare gene variants. We analyzed 29 genes in an Italian cohort of 83 patients with both familial and sporadic ALS. Overall, we detected 43 rare variants in 17 different genes and found that 43.4% of the ALS patients harbored a variant in at least one of the investigated genes. Of note, 27.9% of the variants were identified in other MND- and HMN-associated genes. Moreover, multiple gene variants were identified in 17% of the patients. The burden of rare variants is associated with reduced survival and with the time to reach King stage 4, i.e., the time to reach the need for percutaneous endoscopic gastrostomy (PEG) positioning or non-invasive mechanical ventilation (NIMV) initiation, independently of known negative prognostic factors. Our data contribute to a better understanding of the molecular basis of ALS supporting the hypothesis that rare variant burden could play a role in the multistep model of disease and could exert a negative prognostic effect. Moreover, we further extend the genetic landscape of ALS to other MND-associated genes traditionally implicated in degenerative diseases of peripheral axons, such as HMN and CMT2.

Published

2020

25. Distinct Protein Expression Networks are Activated in Microglia Cells after Stimulation with IFN-γ and IL-4

Author

Daniele Vergara, Annamaria Nigro, Alessandro Romano, Stefania De Domenico, Marina Damato, Julien Franck, Chiara Coricciati, Maxence Wistorski, Tristan Cardon, Isabelle Fournier, Angelo Quattrini, Michel Salzet, Roberto Furlan, and Michele Maffia

Subjects

microglia plasticity, microglia, IFN-γ, IL-4, mass spectrometry, proteomics, Cytology, QH573-671

Abstract

Microglia cells are the primary immune population of the central nervous system with a role in the regulation of several physiological and pathological conditions. Upon appropriate stimulation, microglia cells can be polarized in a pro-inflammatory M1-like or anti-inflammatory M2-like status. Biological processes and pathways engaged in microglia polarization are starting to be elucidated. To help clarify this, we used a liquid chromatography-mass spectrometry (LC-MS/MS) label free approach to characterize the proteomic profile of human microglia cell line (CHME-5) stimulated with gamma-interferon (IFN-γ) and interleukin-4 (IL-4) to induce a M1 or M2 phenotype, respectively. Outside the classical M1/M2 polarization markers, the M1 status appears to center around the activation of a classical inflammatory response and through the activation of multiple signaling pathways. M2 polarization resulted in a different pattern of protein modulation related to RNA and cellular metabolic processes. Together, our findings provide information regarding the protein changes specific to M1 and M2 activation states, and potentially link the polarization of microglia cells to the acquisition of a specific proteomic profile.

Published

2019

26. Lab-on-Chip for Exosomes and Microvesicles Detection and Characterization

Author

Maria Serena Chiriacò, Monica Bianco, Annamaria Nigro, Elisabetta Primiceri, Francesco Ferrara, Alessandro Romano, Angelo Quattrini, Roberto Furlan, Valentina Arima, and Giuseppe Maruccio

Subjects

lab-on-chip, microfabrication, microfluidics, biosensors, extracellular vesicles, exosomes, Chemical technology, TP1-1185

Abstract

Interest in extracellular vesicles and in particular microvesicles and exosomes, which are constitutively produced by cells, is on the rise for their huge potential as biomarkers in a high number of disorders and pathologies as they are considered as carriers of information among cells, as well as being responsible for the spreading of diseases. Current methods of analysis of microvesicles and exosomes do not fulfill the requirements for their in-depth investigation and the complete exploitation of their diagnostic and prognostic value. Lab-on-chip methods have the potential and capabilities to bridge this gap and the technology is mature enough to provide all the necessary steps for a completely automated analysis of extracellular vesicles in body fluids. In this paper we provide an overview of the biological role of extracellular vesicles, standard biochemical methods of analysis and their limits, and a survey of lab-on-chip methods that are able to meet the needs of a deeper exploitation of these biological entities to drive their use in common clinical practice.

Published

2018

27. Monoclonal Antibodies Conjugated with Superparamagnetic Iron Oxide Particles Allow Magnetic Resonance Imaging Detection of Lymphocytes in the Mouse Brain

Author

Alessandro Luchetti, Davide Milani, Francesca Ruffini, Rossella Galli, Andrea Falini, Angelo Quattrini, Giuseppe Scotti, Giancarlo Comi, Gianvito Martino, Roberto Furlan, and Letterio S. Politi

Subjects

Biology (General), QH301-705.5, Medical technology, R855-855.5

Abstract

We investigated the potential of antibody-vectorialized superparamagnetic iron oxide (SPIO) particles as cellular specific magnetic resonance contrast agents to image lymphocyte populations within the central nervous system (CNS), with the final goal of obtaining a reliable tool for noninvasively detecting and tracking specific cellular populations in vivo. We used superparamagnetic particles bound to a monoclonal antibody. The particle is the contrast agent, by means of its T 2 * relaxation properties; the antibody is the targeting vector, responsible for homing the particle to target a surface antigen. To investigate the efficiency of particle vectorialization by these antibodies, we compared two types of antibody-vectorialized CD3-specific particles in vivo. We successfully employed vectorialized SPIO particles to image B220 + cells in a murine model of B-cell lymphoma. Likewise, we were able to identify CD3 + infiltrates in a murine model of multiple sclerosis. The specificity of the technique was confirmed by immunohistochemistry and electron microscopy of corresponding sections. Our findings suggest that indirect binding of the antibody to a streptavidinated particle allows for enhanced particle vectorialization compared to covalent binding of the antibody to the particle.

Published

2012

28. Urokinase plasminogen receptor and the fibrinolytic complex play a role in nerve repair after nerve crush in mice, and in human neuropathies.

Author

Cristina Rivellini, Giorgia Dina, Emanuela Porrello, Federica Cerri, Marina Scarlato, Teuta Domi, Daniela Ungaro, Ubaldo Del Carro, Alessandra Bolino, Angelo Quattrini, Giancarlo Comi, and Stefano C Previtali

Subjects

Medicine, Science

Abstract

Remodeling of extracellular matrix (ECM) is a critical step in peripheral nerve regeneration. In fact, in human neuropathies, endoneurial ECM enriched in fibrin and vitronectin associates with poor regeneration and worse clinical prognosis. Accordingly in animal models, modification of the fibrinolytic complex activity has profound effects on nerve regeneration: high fibrinolytic activity and low levels of fibrin correlate with better nerve regeneration. The urokinase plasminogen receptor (uPAR) is a major component of the fibrinolytic complex, and binding to urokinase plasminogen activator (uPA) promotes fibrinolysis and cell movement. uPAR is expressed in peripheral nerves, however, little is known on its potential function on nerve development and regeneration. Thus, we investigated uPAR null mice and observed that uPAR is dispensable for nerve development, whereas, loss of uPAR affects nerve regeneration. uPAR null mice showed reduced nerve repair after sciatic nerve crush. This was a consequence of reduced fibrinolytic activity and increased deposition of endoneurial fibrin and vitronectin. Exogenous fibrinolysis in uPAR null mice rescued nerve repair after sciatic nerve crush. Finally, we measured the fibrinolytic activity in sural nerve biopsies from patients with peripheral neuropathies. We showed that neuropathies with defective regeneration had reduced fibrinolytic activity. On the contrary, neuropathies with signs of active regeneration displayed higher fibrinolytic activity. Overall, our results suggest that enforced fibrinolysis may facilitate regeneration and outcome of peripheral neuropathies.

Published

2012

29. Genetic interaction between MTMR2 and FIG4 phospholipid phosphatases involved in Charcot-Marie-Tooth neuropathies.

Author

Ilaria Vaccari, Giorgia Dina, Hélène Tronchère, Emily Kaufman, Gaëtan Chicanne, Federica Cerri, Lawrence Wrabetz, Bernard Payrastre, Angelo Quattrini, Lois S Weisman, Miriam H Meisler, and Alessandra Bolino

Subjects

Genetics, QH426-470

Abstract

We previously reported that autosomal recessive demyelinating Charcot-Marie-Tooth (CMT) type 4B1 neuropathy with myelin outfoldings is caused by loss of MTMR2 (Myotubularin-related 2) in humans, and we created a faithful mouse model of the disease. MTMR2 dephosphorylates both PtdIns3P and PtdIns(3,5)P(2), thereby regulating membrane trafficking. However, the function of MTMR2 and the role of the MTMR2 phospholipid phosphatase activity in vivo in the nerve still remain to be assessed. Mutations in FIG4 are associated with CMT4J neuropathy characterized by both axonal and myelin damage in peripheral nerve. Loss of Fig4 function in the plt (pale tremor) mouse produces spongiform degeneration of the brain and peripheral neuropathy. Since FIG4 has a role in generation of PtdIns(3,5)P(2) and MTMR2 catalyzes its dephosphorylation, these two phosphatases might be expected to have opposite effects in the control of PtdIns(3,5)P(2) homeostasis and their mutations might have compensatory effects in vivo. To explore the role of the MTMR2 phospholipid phosphatase activity in vivo, we generated and characterized the Mtmr2/Fig4 double null mutant mice. Here we provide strong evidence that Mtmr2 and Fig4 functionally interact in both Schwann cells and neurons, and we reveal for the first time a role of Mtmr2 in neurons in vivo. Our results also suggest that imbalance of PtdIns(3,5)P(2) is at the basis of altered longitudinal myelin growth and of myelin outfolding formation. Reduction of Fig4 by null heterozygosity and downregulation of PIKfyve both rescue Mtmr2-null myelin outfoldings in vivo and in vitro.

Published

2011

30. Two neuronal models of TDP-43 proteinopathy display reduced axonal translation, increased oxidative stress, and defective exocytosis

Author

Alessandra Pisciottani, Laura Croci, Fabio Lauria, Chiara Marullo, Elisa Savino, Alessandro Ambrosi, Paola Podini, Marta Marchioretto, Filippo Casoni, Ottavio Cremona, Stefano Taverna, Angelo Quattrini, Jean-Michel Cioni, Gabriella Viero, Franca Codazzi, and G. Giacomo Consalez

Abstract

Amyotrophic lateral sclerosis (ALS) is a progressive, lethal neurodegenerative disease mostly affecting people around 50-60 years of age. TDP-43, a ubiquitously expressed RNA-binding protein involved in pre-mRNA splicing and controlling mRNA stability and translation, forms neuronal cytoplasmic inclusions in an overwhelming majority of ALS patients, of both sporadic and familial origin, a phenomenon referred to as TDP-43 proteinopathy. These cytoplasmic aggregates disrupt the subcellular transport and localization of mRNA. The axon, like dendrites, is a site of mRNA translation, permitting the local synthesis of selected proteins, both constitutively and in response to stimuli reaching the axon and presynaptic terminal. This is especially relevant in upper and lower motor neurons, whose axon spans long distances, likely accentuating their susceptibility to ALS-related noxae. In this work we have generated and characterized two models of TDP-43 proteinopathy, consisting of virtually pure populations of mouse cortical neurons expressing a human TDP-43 fusion protein, wt or mutant, which accumulates as cytoplasmic aggregates. Neurons expressing human TDP-43 exhibit a global impairment in axonal protein synthesis, an increase in oxidative stress, and defects in presynaptic function and electrical activity. These changes correlate with deregulation in the axonal levels of polysome-engaged mRNAs playing relevant roles in those processes. Our data support the emerging notion that deregulation of mRNA metabolism and of axonal mRNA transport may trigger the dying-back neuropathy that initiates motor neuron degeneration in ALS.

Published

2023

31. Clinical Features and Biomarkers to Differentiate Primary and Amyotrophic Lateral Sclerosis in Patients With an Upper Motor Neuron Syndrome

Author

Paride Schito, Tommaso Russo, Teuta Domi, Alessandra Mandelli, Laura Pozzi, Ubaldo Del Carro, Paola Carrera, Federica Agosta, Angelo Quattrini, Roberto Furlan, Massimo Filippi, and Nilo Riva

Subjects

Neurology (clinical)

Abstract

Background:Differentiation between primary (PLS) and amyotrophic lateral sclerosis (ALS) entails relevant consequences for prognosis and management but is mostly unreliable at early stages. The objectives of the study are: i) to determine the features at onset that could help to differentiate between PLS and ALS; ii) to evaluate the diagnostic performance of an integrated serum biomarker panel; iii) to identify the prognostic factors for patients presenting with an upper motor neuron (UMN)-syndrome.Methods:We selected and retrospectively analyzed the clinical data of patients presenting with UMN-syndrome. At the first evaluation, when available, serum biomarkers were measured using ultrasensitive single molecule array.Results:Study population included 55 PLS and 50 ALS patients. PLS patients presented a longer time to first neurological evaluation (PLS: 35.0 months, IQR: 17.0-38.0; ALS: 12.5 months, IQR: 7.0-21.3; pC9orf72expansion. NfL resulted an independent predictor of final diagnosis (OR: 1.01, 95%CI: 1.00-1.02; p=0.04) and an independent prognostic factor (HR: 1.01, 95%CI: 1.00-1.01; pConclusions:NfL might help to differentiate PLS from ALS patients and to predict prognosis in patients with an UMN-syndrome.

Published

2023

32. Integrated evaluation of a panel of neurochemical biomarkers to optimize diagnosis and prognosis in amyotrophic lateral sclerosis

Author

Yuri Matteo Falzone, Teuta Domi, Alessandra Mandelli, Laura Pozzi, Paride Schito, Tommaso Russo, Alessandra Barbieri, Raffaella Fazio, Maria Antonietta Volontè, Giuseppe Magnani, Ubaldo Del Carro, Paola Carrera, Andrea Malaspina, Federica Agosta, Angelo Quattrini, Roberto Furlan, Massimo Filippi, Nilo Riva, Falzone, Y. M., Domi, T., Mandelli, A., Pozzi, L., Schito, P., Russo, T., Barbieri, A., Fazio, R., Volonte, M. A., Magnani, G., Del Carro, U., Carrera, P., Malaspina, A., Agosta, F., Quattrini, A., Furlan, R., Filippi, M., and Riva, N.

Subjects

Cohort Studies, neurofilament proteins, Neurology, Neurofilament Proteins, Frontotemporal Dementia, glial fibrillary acidic protein, Amyotrophic Lateral Sclerosis, Humans, UCHL1 protein, Neurology (clinical), Prognosis, frontotemporal dementia, Biomarkers

Abstract

Background and purpose: This study was undertaken to determine the diagnostic and prognostic value of a panel of serum biomarkers and to correlate their concentrations with several clinical parameters in a large cohort of patients with amyotrophic lateral sclerosis (ALS). Methods: One hundred forty-three consecutive patients with ALS and a control cohort consisting of 70 patients with other neurodegenerative disorders (DEG), 70 patients with ALS mimic disorders (ALSmd), and 45healthy controls (HC) were included. Serum neurofilament light chain (NfL), ubiquitin carboxyl-terminal hydrolase isozyme L1 (UCHL1), glial fibrillary acidic protein (GFAP), and total tau protein levels were measured using ultrasensitive single molecule array. Results: NfL correlated with disease progression rate (p&nbsp

Published

2022

33. Phosphorylated TDP-43 aggregates in peripheral motor nerves of patients with amyotrophic lateral sclerosis

Author

Nilo Riva, Francesco Gentile, Federica Cerri, Francesca Gallia, Paola Podini, Giorgia Dina, Yuri Matteo Falzone, Raffaella Fazio, Christian Lunetta, Andrea Calvo, Giancarlo Logroscino, Giuseppe Lauria, Massimo Corbo, Sandro Iannaccone, Adriano Chiò, Alberto Lazzerini, Eduardo Nobile-Orazio, Massimo Filippi, Angelo Quattrini, Riva, Nilo, Gentile, Francesco, Cerri, Federica, Gallia, Francesca, Podini, Paola, Dina, Giorgia, Falzone, Yuri Matteo, Fazio, Raffaella, Lunetta, Christian, Calvo, Andrea, Logroscino, Giancarlo, Lauria, Giuseppe, Corbo, Massimo, Iannaccone, Sandro, Chiò, Adriano, Lazzerini, Alberto, Nobile-Orazio, Eduardo, Filippi, Massimo, and Quattrini, Angelo

Subjects

DNA-Binding Proteins, Motor Neurons, neuropathology, aggregates, motor neuron disease, motor neuropathy, peripheral nervous system, Humans, Peripheral Nervous System, Retrospective Studies, Amyotrophic Lateral Sclerosis, Neurology (clinical)

Abstract

Phosphorylated TDP-43 (pTDP-43) aggregates in the cytoplasm of motor neurons and neuroglia in the brain are one of the pathological hallmarks of amyotrophic lateral sclerosis. Although the axons exceed the total volume of motor neuron soma by several orders of magnitude, systematic studies investigating the presence and distribution of pTDP-43 aggregates within motor nerves are still lacking. The aim of this study is to define the TDP-43/pTDP-43 pathology in diagnostic motor nerve biopsies performed on a large cohort of patients presenting with a lower motor neuron syndrome and to assess whether this might be a discriminating tissue biomarker for amyotrophic lateral sclerosis and non-amyotrophic lateral sclerosis cases. We retrospectively evaluated 102 lower motor neuron syndrome patients referred to our centre for a diagnostic motor nerve biopsy. Histopathological criteria of motor neuron disease and motor neuropathy were applied by two independent evaluators, who were blind to clinical data. TDP-43 and pTDP-43 were evaluated by immunohistochemistry, and results compared to final clinical diagnosis. We detected significant differences between amyotrophic lateral sclerosis and non-amyotrophic lateral sclerosis cases in pTDP-43 expression in myelinated fibres: axonal accumulation was detected in 98.2% of patients with amyotrophic lateral sclerosis versus 30.4% of non-amyotrophic lateral sclerosis samples (P < 0.0001), while concomitant positive staining in Schwan cell cytoplasm was found in 70.2% of patients with amyotrophic lateral sclerosis versus 17.4% of patients who did not have amyotrophic lateral sclerosis (P < 0.001). Importantly, we were also able to detect pTDP-43 aggregates in amyotrophic lateral sclerosis cases displaying normal features at standard histopathological analysis. Our findings demonstrated that a specific pTDP-43 signature is present in the peripheral nervous system of patients with amyotrophic lateral sclerosis, and could be exploited as a specific, accessible tissue biomarker. The detection of pTDP-43 aggregates within motor nerves of living patients with amyotrophic lateral sclerosis, occurring before axonal degeneration, suggests that this is an early event that may contribute to amyotrophic lateral sclerosis pathogenesis.

Published

2022

34. Reply to the Letter to the Editor in response to 'Integrated evaluation of a panel of neurochemical biomarkers to optimize diagnosis and prognosis in amyotrophic lateral sclerosis'

Author

Nilo Riva and Angelo Quattrini

Subjects

Neurology, Amyotrophic Lateral Sclerosis, Humans, Neurology (clinical), Prognosis, Biomarkers

Published

2022

35. Loss of function <scp>MPZ</scp> mutation causes milder <scp>CMT1B</scp> neuropathy

Author

Raffaella Fazio, Paige Howard, Tiffany Grider, Michael E. Shy, Stefano C. Previtali, Marina Scarlato, Angelo Quattrini, Alexa Bacha, and Shawna M. E. Feely

Subjects

medicine.medical_specialty, Nonsense-mediated decay, medicine.disease_cause, Mice, 03 medical and health sciences, Myelin, 0302 clinical medicine, Sensory ataxia, Charcot-Marie-Tooth Disease, Mutant protein, Internal medicine, medicine, Animals, Humans, Myelin Sheath, Loss function, Mutation, business.industry, General Neuroscience, Myelin protein zero, Electrophysiological Phenomena, Endocrinology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Neurology (clinical), medicine.symptom, Haploinsufficiency, business, Myelin P0 Protein, 030217 neurology & neurosurgery

Abstract

Mutations in Myelin Protein Zero (MPZ) cause CMT1B, the second leading cause of CMT1. Many of the >200 mutations cause neuropathy through a toxic gain of function by the mutant protein such as ER retention, activation of the Unfolded Protein Response (UPR) or disruption of myelin compaction. While there is extensive literature on the loss of function consequences of MPZ in heterozygous Mpz +/- null mice, there is little known of the consequences of MPZ haploinsufficiency in humans. We identified six patients from different families with p.Tyr68Ter or p.Asp104fs heterozygous mutations of MPZ that are predicted to cause a premature termination and nonsense mediated decay of the mutant allele. Five patients were evaluated in Milan and one in Iowa City; all should be haploinsufficient for MPZ. Patients were evaluated clinically and by electrophysiology. Sensory ataxia dominated the clinical presentation with only mild weakness present in five of the six patients. Symptoms presented in adulthood in all patients and only one individual had a CMTNSv2 >5. Deep tendon reflexes were absent in all patients. Patients with likely MPZ loss of function due to mutations that cause haplodeficiency in MPZ have a mild, predominantly large fiber sensory neuropathy that serves as a human equivalent to the neuropathy observed in heterozygous Mpz null mice. Successful therapeutic approaches in treating Mpz deficient mice may be candidates for trials in these and similar patients.

Published

2021

36. ADAM17 Regulates p75(NTR)-Mediated Fibrinolysis and Nerve Remyelination

Author

Marta Pellegatta, Paolo Canevazzi, Maria Grazia Forese, Paola Podini, Serena Valenzano, Ubaldo Del Carro, Angelo Quattrini, and Carla Taveggia

Subjects

Fibrin, Mice, Remyelination, General Neuroscience, Disintegrins, Fibrinolysis, Tissue Plasminogen Activator, Animals, ADAM17 Protein, Wallerian Degeneration, Receptor, Nerve Growth Factor, Research Articles

Abstract

We previously reported that a-disintegrin and metalloproteinase (ADAM)17 is a key protease regulating myelin formation. We now describe a role for ADAM17 during the Wallerian degeneration (WD) process. Unexpectedly, we observed that glial ADAM17, by regulating p75NTRprocessing, cell autonomously promotes remyelination, while neuronal ADAM17 is dispensable. Accordingly, p75NTRabnormally accumulates specifically when ADAM17 is maximally expressed leading to a downregulation of tissue plasminogen activator (tPA) expression, excessive fibrin accumulation over time, and delayed remyelination. Mutant mice also present impaired macrophage recruitment and defective nerve conduction velocity (NCV). Thus, ADAM17 expressed in Schwann cells, controls the whole WD process, and its absence hampers effective nerve repair. Collectively, we describe a previously uncharacterized role for glial ADAM17 during nerve regeneration. Based on the results of our study, we posit that, unlike development, glial ADAM17 promotes remyelination through the regulation of p75NTR-mediated fibrinolysis.SIGNIFICANCE STATEMENTThe α-secretase a-disintegrin and metalloproteinase (ADAM)17, although relevant for developmental PNS myelination, has never been investigated in Wallerian degeneration (WD). We now unravel a new mechanism of action for this protease and show that ADAM17 cleaves p75NTR, regulates fibrin clearance, and eventually fine-tunes remyelination. The results presented in this study provide important insights into the complex regulation of remyelination following nerve injury, identifying in ADAM17 and p75NTRa new signaling axis implicated in these events. Modulation of this pathway could have important implications in promoting nerve remyelination, an often-inefficient process, with the aim of restoring a functional axo-glial unit.

Published

2022

37. X-ray phase contrast tomography for the investigation of amyotrophic lateral sclerosis

Author

Alberto Mittone, Giuseppe Gigli, Lorenzo Massimi, Laura Maugeri, Michela Fratini, Andrea Fossaghi, Alessia Cedola, Nilo Riva, Ginevra Begani Provinciali, Francesco Gentile, Fabrizio Bardelli, Nicola Pieroni, Alberto Bravin, Angelo Quattrini, Inna Bukreeva, Francesca Palermo, Provinciali, G, Pieroni, N, Bukreeva, I, Fratini, M, Massimi, L, Maugeri, L, Palermo, F, Bardelli, F, Mittone, A, Bravin, A, Gigli, G, Gentile, F, Fossaghi, A, Riva, N, Quattrini, A, Cedola, A, Laboratoire d'optique appliquée (LOA), and École Nationale Supérieure de Techniques Avancées (ENSTA Paris)-École polytechnique (X)-Centre National de la Recherche Scientifique (CNRS)

Subjects

Nuclear and High Energy Physics, [PHYS.PHYS.PHYS-BIO-PH]Physics [physics]/Physics [physics]/Biological Physics [physics.bio-ph], FIS/07 - FISICA APPLICATA (A BENI CULTURALI, AMBIENTALI, BIOLOGIA E MEDICINA), Mice, Transgenic, Neuropathology, Disease, Signal-To-Noise Ratio, Sensitivity and Specificity, Mice, 03 medical and health sciences, Imaging, Three-Dimensional, 0302 clinical medicine, Neuroimaging, medicine, Animals, Therapy efficacy, Amyotrophic lateral sclerosis, Instrumentation, ComputingMilieux_MISCELLANEOUS, 030304 developmental biology, [PHYS.PHYS.PHYS-OPTICS]Physics [physics]/Physics [physics]/Optics [physics.optics], 0303 health sciences, Phase contrast tomography, Radiation, Amyotrophic Lateral Sclerosis, Progressive neurodegenerative disorder, Spinal cord, medicine.disease, Research Papers, Disease Models, Animal, medicine.anatomical_structure, Spinal Cord, ALS, X-ray phase contrast tomography, Tomography, X-Ray Computed, spinal cord, Neuroscience, 030217 neurology & neurosurgery

Abstract

Ex vivo X-ray phase contrast tomography of amyotrophic lateral sclerosis of a SOD1G93A mouse model is presented. Quantification of neuronal and vascular alteration in the central nervous system is described., Amyotrophic lateral sclerosis (ALS) is a progressive neurodegenerative disorder affecting motor neurons. Pre-clinical studies drive the development of animal models that well mimic ALS disorder and enable both the dissection of disease processes and an early assessment of therapy efficacy. A comprehensive knowledge of neuronal and vascular lesions in the brain and spinal cord is an essential factor to understand the development of the disease. Spatial resolution and bidimensional imaging are important drawbacks limiting current neuroimaging tools, while neuropathology relies on protocols that may alter tissue chemistry and structure. In contrast, recent ex vivo studies in mice demonstrated that X-ray phase-contrast tomography enables study of the 3D distribution of both vasculature and neuronal networks, without sample sectioning or use of staining. Here we present our findings on ex vivo SOD1G93A ALS mice spinal cord at a micrometric scale. An unprecedented direct quantification of neuro-vascular alterations at different stages of the disease is shown.

Published

2020

38. Primary Lateral Sclerosis Presenting With Focal Onset Spreading Through Contiguous Neuroanatomic Regions

Author

Paride Schito, Edoardo Gioele Spinelli, Antonio Malvaso, Tommaso Russo, Yuri Matteo Falzone, Federica Agosta, Angelo Quattrini, Massimo Filippi, Nilo Riva, Schito, Paride, Spinelli, Edoardo Gioele, Malvaso, Antonio, Russo, Tommaso, Falzone, Yuri Matteo, Agosta, Federica, Quattrini, Angelo, Filippi, Massimo, and Riva, Nilo

Subjects

Motor Neurons, Amyotrophic Lateral Sclerosis, Humans, Neurology (clinical)

Published

2022

39. Neurofilament light chain as a biological marker for amyotrophic lateral sclerosis: a meta-analysis study

Author

Giacomo Sferruzza, Luca Bosco, Yuri Matteo Falzone, Tommaso Russo, Teuta Domi, Angelo Quattrini, Massimo Filippi, Nilo Riva, Sferruzza, Giacomo, Bosco, Luca, Falzone, Yuri Matteo, Russo, Tommaso, Domi, Teuta, Quattrini, Angelo, Filippi, Massimo, and Riva, Nilo

Subjects

neurofilament light chain, Neurology, Neurofilament Proteins, Amyotrophic Lateral Sclerosis, Intermediate Filaments, motor neuron disease, Humans, biomarkers, Enzyme-Linked Immunosorbent Assay, Neurology (clinical), ALS, Biomarkers

Abstract

Aim: The aim of the present metanalysis is to evaluate blood and CSF Neurofilament light chain (NfL) concentrations in ALS patients, compared to healthy controls, ALS mimic disorders (ALSmd) and other neurological diseases (OND), and to evaluate their diagnostic yield against ALSmd. Methods: Search engines were systematically investigated for relevant studies. A random effect model was applied to estimate the pooled standard mean difference in NfL levels between ALS and controls and a bivariate mixed-effects model was applied to estimate their diagnostic accuracy on blood and CSF. Results and conclusions: NfL CSF levels were higher in ALS compared with all other control groups. On blood, NfL levels were significantly higher in ALS patients compared with healthy controls and ALSmd. In a subgroup analysis, the use of SIMOA yielded to a better differentiation between ALS and controls on blood, compared with ELISA. Studies performed on CSF (AUC = 0.90) yielded to better diagnostic performances compared with those conducted on blood (AUC = 0.78). Further prospective investigations are needed to determine a diagnostic cutoff, exploitable in clinical practice.

Published

2022

40. Normal structure and pathological features in peripheral neuropathies

Author

Angelo Quattrini, Ahmet Hoke, Federica Cerri, Aysel Fisgin, and Nilo Riva

Subjects

Pathology, medicine.medical_specialty, business.industry, General Neuroscience, Peripheral Nervous System Diseases, Axons, Peripheral, Myelin, medicine.anatomical_structure, nervous system, Interstitial space, medicine, Humans, Peripheral Nerves, Neurology (clinical), Peripheral Nerve Disorders, Axon, Remyelination, Differential diagnosis, business, Pathological, Myelin Sheath

Abstract

Normal nerve architecture is basic to a complete understanding of nerve pathology. Here, normal components of the nerve are illustrated, including myelinated and non-myelinated nerve fibres, stromal elements, and vascular components. These are relevant because the differential diagnosis of neuropathy depends on the pathological processes affecting axon, myelin, interstitial space, and blood vessels. Thus, we present a description of the general pathological characteristics for the diagnosis of peripheral nerve disorders.

Published

2021

41. Thermosensitive chitosan-based hydrogels supporting motor neuron-like NSC-34 cell differentiation

Author

Antonella, Stanzione, Alessandro, Polini, Velia, La Pesa, Angelo, Quattrini, Alessandro, Romano, Giuseppe, Gigli, Lorenzo, Moroni, and Francesca, Gervaso

Subjects

Motor Neurons, Chitosan, Temperature, Cell Differentiation, Hydrogels

Abstract

Motor neuron diseases are neurodegenerative diseases that predominantly affect the neuromuscular system. To date, there are no valid therapeutic treatments for such diseases, and the classical experimental models fail in faithfully reproducing the pathological mechanisms behind them. In this regard, the use of three-dimensional (3D) culture systems, which more closely reproduce the native

Published

2021

42. Neurovascular signals in amyotrophic lateral sclerosis

Author

Valentina Arima, Giuseppe Gigli, Stefano Sorrentino, Angelo Quattrini, Lorenzo Moroni, Pamela Mozetic, Alessandro Romano, Alessandro Polini, Sorrentino, Stefano, Polini, Alessandro, Arima, Valentina, Romano, Alessandro, Quattrini, Angelo, Gigli, Giuseppe, Mozetic, Pamela, and Moroni, Lorenzo

Subjects

BLOOD-BRAIN-BARRIER, business.industry, PERICYTES, MATRIX-METALLOPROTEINASE-9, Amyotrophic Lateral Sclerosis, Biomedical Engineering, TIGHT JUNCTIONS, Bioengineering, medicine.disease, Neurovascular bundle, SERUM, Pathogenesis, CELLS, medicine, Humans, SPINAL-CORD, Amyotrophic lateral sclerosis, business, MATRIX, Neuroscience, Signalling pathways, Homeostasis, Biotechnology, Human

Abstract

The neurovascular system (NVS) is a complex anatomic-functional unit that synergically works to maintain organs/tissues homeostasis of the entire body. NVS alterations have recently emerged as a common distinct feature in the pathogenesis of several neurodegenerative diseases, including amyotrophic lateral sclerosis (ALS). Despite their undeniable involvement, neurovascular signalling pathways remain still far unknown in ALS. This review underlines the importance of endothelial, mural, and fibroblast cells as novel targets for ALS investigation and identifies in the interplay between neuronal and vascular systems the way to disclose novel molecular mechanisms behind the pathogenesis of ALS.

Published

2021

43. Chip-Based Chiral 3D Metamaterial with Functional Core-Shell Architecture for Femtomolar Biodetection

Author

Giuseppe Gigli, Alessandro Romano, Yali Sun, Adriana Passaseo, Elisabetta Primiceri, Mariachiara Manoccio, Dmitry Zuev, Angelo Leo, Massimo Cuscunà, Vittorianna Tasco, Marco Esposito, Giuseppe Maruccio, and Angelo Quattrini

Subjects

Physics, Core shell architecture, Metamaterial, Nanotechnology, Chip

Abstract

Advanced sensing tools capable to detect extremely low concentrations of circulating biomarkers can open unexplored routes towards early diagnostics of diseases and their progression monitoring. Plasmonic sensors are an emerging technology enabling different optical effects that can be used as molecular tracking solutions. Here we demonstrate the sensing capabilities of a chip-based metamaterial, combining the 3D chiral geometry with an optically functional core-shell architecture. The sensor can be easily handled and exhibits reliability and stability during the whole functionalization and analytical procedure thanks to the on-chip format. The system shows a linear shift of circular dichroism spectrum upon interaction with different concentrations of TAR DNA-binding protein TDP-43, a clinically relevant biomarker for neurodegenerative disease screening. The measurements were performed in spiked solution as well as in human serum, with concentrations from 1pM down to 10fM, a range not accessible with commonly used immunological assays and that can thus open new perspectives for disease knowledge and early diagnostics.

Published

2021

44. Dysregulated copper transport in multiple sclerosis may cause demyelination via astrocytes

Author

Daniela Triolo, Vittorio Martinelli, Emanuela Colombo, Claudia Bassani, Jia Newcombe, Carla Taveggia, Evelien Fredrickx, Marco Di Dario, Giancarlo Comi, Francesco Bedogni, Isabella Fermo, Cinthia Farina, Angelo Quattrini, and Giorgia Dina

Subjects

Encephalomyelitis, Autoimmune, Experimental, Multiple Sclerosis, Tropomyosin receptor kinase B, Ligands, Cicatrix, Cuprizone, Transactivation, medicine, Animals, Humans, Receptor, trkB, Nerve Growth Factors, Myelin Sheath, Neuroinflammation, Inflammation, Mice, Knockout, Multidisciplinary, biology, Chemistry, musculoskeletal, neural, and ocular physiology, Multiple sclerosis, Membrane Transport Proteins, Biological Transport, medicine.disease, White Matter, Oligodendrocyte, Up-Regulation, Cell biology, Disease Models, Animal, medicine.anatomical_structure, nervous system, Astrocytes, Chronic Disease, Neurotrophin binding, Commentary, biology.protein, Copper, Neurotrophin, Astrocyte

Abstract

Demyelination is a key pathogenic feature of multiple sclerosis (MS). Here, we evaluated the astrocyte contribution to myelin loss and focused on the neurotrophin receptor TrkB, whose up-regulation on the astrocyte finely demarcated chronic demyelinated areas in MS and was paralleled by neurotrophin loss. Mice lacking astrocyte TrkB were resistant to demyelination induced by autoimmune or toxic insults, demonstrating that TrkB signaling in astrocytes fostered oligodendrocyte damage. In vitro and ex vivo approaches highlighted that astrocyte TrkB supported scar formation and glia proliferation even in the absence of neurotrophin binding, indicating TrkB transactivation in response to inflammatory or toxic mediators. Notably, our neuropathological studies demonstrated copper dysregulation in MS and model lesions and TrkB-dependent expression of copper transporter (CTR1) on glia cells during neuroinflammation. In vitro experiments evidenced that TrkB was critical for the generation of glial intracellular calcium flux and CTR1 up-regulation induced by stimuli distinct from neurotrophins. These events led to copper uptake and release by the astrocyte, and in turn resulted in oligodendrocyte loss. Collectively, these data demonstrate a pathogenic demyelination mechanism via the astrocyte release of copper and open up the possibility of restoring copper homeostasis in the white matter as a therapeutic target in MS.

Published

2021

45. Prostaglandin D2 synthase modulates macrophage activity and accumulation in injured peripheral nerves

Author

Cristina Rivellini, Giorgia Serena Gullotta, Marco Bacigaluppi, Carla Taveggia, Maria Grazia Forese, Angelo Quattrini, Marta Pellegatta, Paola Podini, Paolo Canevazzi, and Stefano C. Previtali

Subjects

Male, 0301 basic medicine, Wallerian degeneration, Schwann cell, Prostaglandin, Mice, 03 medical and health sciences, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Myelin, 0302 clinical medicine, Peripheral Nerve Injuries, medicine, Animals, Remyelination, biology, Prostaglandin D2 synthase, Macrophage Activation, medicine.disease, Lipocalins, Nerve Regeneration, Cell biology, Intramolecular Oxidoreductases, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, nervous system, Neurology, chemistry, Peripheral nervous system, Peripheral nerve injury, biology.protein, Female, Sciatic Neuropathy, 030217 neurology & neurosurgery

Abstract

We have previously reported that prostaglandin D2 Synthase (L-PGDS) participates in peripheral nervous system (PNS) myelination during development. We now describe the role of L-PGDS in the resolution of PNS injury, similarly to other members of the prostaglandin synthase family, which are important for Wallerian degeneration (WD) and axonal regeneration. Our analyses show that L-PGDS expression is modulated after injury in both sciatic nerves and dorsal root ganglia neurons, indicating that it might play a role in the WD process. Accordingly, our data reveals that L-PGDS regulates macrophages phagocytic activity through a non-cell autonomous mechanism, allowing myelin debris clearance and favoring axonal regeneration and remyelination. In addition, L-PGDS also appear to control macrophages accumulation in injured nerves, possibly by regulating the blood-nerve barrier permeability and SOX2 expression levels in Schwann cells. Collectively, our results suggest that L-PGDS has multiple functions during nerve regeneration and remyelination. Based on the results of this study, we posit that L-PGDS acts as an anti-inflammatory agent in the late phases of WD, and cooperates in the resolution of the inflammatory response. Thus, pharmacological activation of the L-PGDS pathway might prove beneficial in resolving peripheral nerve injury.

Published

2019

46. Limitations in daily activities and general perception of quality of life: Long term follow‐up in patients with anti‐myelin‐glycoprotein antibody polyneuropathy

Author

Giancarlo Comi, Angelo Quattrini, Marta Campagnolo, Alessandro Salvalaggio, Raffaella Fazio, Mariangela Bianco, Yuri Matteo Falzone, Federica Cerri, Marta Ruiz, Eduardo Nobile-Orazio, Francesca Castellani, Mario Ermani, Chiara Briani, Fabio Giannini, Nilo Riva, and Daniele Martinelli

Subjects

Adult, Male, medicine.medical_specialty, peripheral neuropathy, Visual analogue scale, Disability and Health (ICF), International Classification of Functioning, Disability Evaluation, Polyneuropathies, 03 medical and health sciences, quality of life (QoL), 0302 clinical medicine, International Classification of Functioning, Disability and Health, Quality of life, Statistical significance, Internal medicine, Activities of Daily Living, follow-up, 80 and over, medicine, Humans, Immunologic Factors, anti-MAG antibodies, Aged, Aged, 80 and over, Myelin glycoprotein, business.industry, General Neuroscience, International Classification of Functioning, Disability and Health (ICF), Middle Aged, medicine.disease, Myelin-Associated Glycoprotein, Treatment Outcome, Peripheral neuropathy, 030220 oncology & carcinogenesis, Cohort, Quality of Life, Female, Rituximab, Neurology (clinical), business, Polyneuropathy, 030217 neurology & neurosurgery

Abstract

In this study, we assessed the modifications over time of daily activities and quality of life (QoL) in 32 subjects with anti-myelin-glycoprotein (MAG) antibody neuropathy. A widespread panel including clinical scores and patient-reported questionnaires, in compliance of the terms by the International Classification of Functioning, Disability, and Health (ICF) of the World Health Organization (WHO), was employed at enrollment (T0) and at follow-up evaluation (T1) after a mean interval of 15.4 ± 5.7 months. The Sensory Modality Sum score (SMS) at four limbs showed a significant worsening over time (mean score 27.2 ± 3.9 at T0 vs 25.7 ± 3 at T1 at upper limbs, P = .03; 20.5 ± 4.8 at T0 vs 18.6 ± 5.9 at T1 at lower limbs, P = .04). The Visual Analogue Scale (VAS) for pain significantly worsened at upper limbs at T1 (mean values 0.84 ± 1.95 at T0 vs 1.78 ± 2.6 at T1, P = .03). All the other tests did not show significant differences between T0 and T1. In the subgroup who underwent rituximab (15/32 treated before T0, 3/32 patients treated between T0 and T1 with median interval of 1 year), no significant differences were observed between T0 and T1. Despite the quite long follow-up, statistical significance was not achieved either for the limited number of patients or for the lack of sensitive outcome measures. In our cohort, the significant worsening of the SMS and VAS after a median of 14 months can be considered as a reliable expression of the natural history of the disease, and suggest that these scales might represent possible outcome measures in anti-MAG antibody neuropathy.

Published

2019

47. Neural Stem Cells of the Subventricular Zone Contribute to Neuroprotection of the Corpus Callosum after Cuprizone-Induced Demyelination

Author

Linda Chaabane, Elena Brambilla, Marco Bacigaluppi, Erica Butti, Gianvito Martino, Carolina Montonati, Giulia Berera, Francesca Ruffini, Angelo Quattrini, Butti, E., Bacigaluppi, M., Chaabane, L., Ruffini, F., Brambilla, E., Berera, G., Montonati, C., Quattrini, A., and Martino, G.

Subjects

0301 basic medicine, Axonal loss, Subventricular zone, Ablation, Biology, Neuroprotection, Corpus Callosum, Multiple sclerosis, Cuprizone, Mice, 03 medical and health sciences, 0302 clinical medicine, Neural Stem Cells, Cell Movement, Lateral Ventricles, Precursor cell, medicine, Transgenic mice, Animals, Remyelination, Demyelinating Disorder, Research Articles, Myelin Sheath, Neural stem cells, Sub ventricular zone, General Neuroscience, medicine.disease, Neural stem cell, Mice, Inbred C57BL, Oligodendroglia, 030104 developmental biology, medicine.anatomical_structure, nervous system, Female, Neuroscience, 030217 neurology & neurosurgery, Demyelinating Diseases

Abstract

Myelin loss occurring in demyelinating diseases, including multiple sclerosis, is the leading cause of long-lasting neurological disability in adults. While endogenous remyelination, driven by resident oligodendrocyte precursor cells (OPCs), might partially compensate myelin loss in the early phases of demyelinating disorders, this spontaneous reparative potential fails at later stages. To investigate the cellular mechanisms sustaining endogenous remyelination in demyelinating disorders, we focused our attention on endogenous neural precursor cells (eNPCs) located within the subventricular zone (SVZ) since this latter area is considered one of the primary sources of new OPCs in the adult forebrain. First, we fate mapped SVZ-eNPCs in cuprizone-induced demyelination and found that SVZ endogenous neural stem/precursor cells are recruited during the remyelination phase to the corpus callosum (CC) and are capable of forming new oligodendrocytes. When we ablated SVZ-derived eNPCs during cuprizone-induced demyelination in female mice, the animals displayed reduced numbers of oligodendrocytes within the lesioned CC. Although this reduction in oligodendrocytes did not impact the ensuing remyelination, eNPC-ablated mice experienced increased axonal loss. Our results indicate that, in toxic models of demyelination, SVZ-derived eNPCs contribute to support axonal survival. SIGNIFICANCE STATEMENT One of the significant challenges in MS research is to understand the detrimental mechanisms leading to the failure of CNS tissue regeneration during disease progression. One possible explanation is the inability of recruited oligodendrocyte precursor cells (OPCs) to complete remyelination and to sustain axonal survival. The contribution of endogenous neural precursor cells (eNPCs) located in the subventricular zone (SVZ) to generate new OPCs in the lesion site has been debated. Using transgenic mice to fate map and to selectively kill SVZ-derived eNPCs in the cuprizone demyelination model, we observed migration of SVZ-eNPCs after injury and their contribution to oligodendrogenesis and axonal survival. We found that eNPCs are dispensable for remyelination but protect partially from increased axonal loss.

Published

2019

48. Nerve pathology in animal models of neuropathies

Author

Alessandra Bolino, Angelo Quattrini, Maurizio D'Antonio, Valentina Alda Carozzi, Guido Cavaletti, Carozzi, V, Bolino, A, D'Antonio, M, Quattrini, A, and Cavaletti, G

Subjects

Charcot-Marie-Tooth, Pathology, medicine.medical_specialty, medicine.diagnostic_test, experimental autoimmune neuriti, Nerve pathology, business.industry, General Neuroscience, Neuritis, medicine.disease, Peripheral, inherited peripheral neuropathie, Peripheral neuropathy, Chemotherapy-induced peripheral neuropathy, Charcot-Marie-Tooth Disease, Biopsy, Models, Animal, medicine, Animals, Humans, Neurology (clinical), business, Axonal degeneration, Pathological, chemotherapy-induced peripheral neuropathy

Abstract

To understand the pathology of axonal degeneration and demyelination in peripheral neuropathy, histological investigations in different animal models that mimic some aspects of human peripheral neuropathy are needed. Thus, in the following section of this special issue, the main pathological features of experimental autoimmune neuritis, animal models of chemotherapy-induced peripheral neuropath and of human inherited peripheral neuropathies (IPNs) will be illustrated. When possible, micrographs from animal models and selected human biopsy will be shown side by side.

Published

2021

49. Hemiplegic-type ALS shows a strong correlation between upper, lower motor neuron degeneration and pTDP-43 pathology

Author

Nilo Riva and Angelo Quattrini

Subjects

Pathology, medicine.medical_specialty, business.industry, Genetic heterogeneity, Amyotrophic Lateral Sclerosis, Hemiplegia, Neuropathology, medicine.disease, DNA-Binding Proteins, 03 medical and health sciences, Psychiatry and Mental health, 0302 clinical medicine, Disease spreading, Motor system, Nerve Degeneration, Motor neuron degeneration, Lower motor neuron degeneration, Medicine, Humans, Surgery, Neurology (clinical), Amyotrophic lateral sclerosis, business, 030217 neurology & neurosurgery

Abstract

Several lines of evidence shoe that motor neuron degeneration starts as a focal process in amyotrophic lateral sclerosis (ALS), subsequently spreading through the complex anatomy of the motor system. ALS may present with considerable phenotypic heterogeneity, reflecting the varied degree of involvement of both motor and extramotor areas.1 Even though, historically, clinicpathological studies have provided an unevaluable contribution to the identification of ALS as a nosological entity, to unravel the central pathogenetic role of the phosphorylated 43 kDa transactive response DNA-binding protein (pTDP-43) as well as to conceptualise disease spreading, few reports have been focused on ALS restricted phenotypes so far. Sainouchi et al present an intriguing clinicopathological study of two cases of hemiplegic ALS. Both patients presented at onset with upper …

Published

2021

50. Selective loss of microvesicles is a major issue of the differential centrifugation isolation protocols

Author

Alessandro Romano, Annamaria Finardi, Daniela Manno, Annamaria Nigro, Angelo Quattrini, Marzia M. Ferraro, Roberto Furlan, Nigro, A., Finardi, A., Ferraro, M. M., Manno, D. E., Quattrini, A., Furlan, R., and Romano, A.

Subjects

Differential centrifugation, Cell biology, education.field_of_study, Multidisciplinary, medicine.diagnostic_test, Chemistry, Science, Vesicle, Biological techniques, Population, Isolation (microbiology), Extracellular vesicles, Article, Microvesicles, Flow cytometry, TEM/AFM microscopy, extracellular vesicles, Biophysics, medicine, Medicine, Centrifugation, education

Abstract

Microvesicles (MVs) are large extracellular vesicles differing in size, cargo and composition that share a common mechanism of release from the cells through the direct outward budding of the plasma membrane. They are involved in a variety of physiological and pathological conditions and represent promising biomarkers for diseases. MV heterogeneity together with the lack of specific markers had strongly hampered the development of effective methods for MV isolation and differential centrifugation remains the most used method to purify MVs. In this study, we analysed the capacity of the differential centrifugation method to isolate MVs from cell-conditioned medium using flow cytometry and TEM/AFM microscopy. We found that the loss of MVs (general population and/or specific subpopulations) represents a major and underestimate drawback of the differential centrifugation protocol. We demonstrate that the choice of the appropriate rotor type (fixed-angle vs swinging-bucket) and the implementation of an additional washing procedure to the first low-speed centrifugation step of the protocol allow to overcome this problem increasing the total amount of isolated vesicles and avoiding the selective loss of MV subpopulations. These parameters/procedures should be routinely employed into optimized differential centrifugation protocols to ensure isolation of the high-quantity/quality MVs for the downstream analysis/applications.

Published

2021