Your search keyword '"Francesca Puglisi"' showing total 15 results

1. Chronic lymphocytic leukemia cells impair osteoblastogenesis and promote osteoclastogenesis: role of TNFα, IL-6 and IL-11 cytokines

Author

Paolo Giannoni, Cecilia Marini, Giovanna Cutrona, Serena Matis, Maria Cristina Capra, Francesca Puglisi, Paola Luzzi, Simona Pigozzi, Gabriele Gaggero, Antonino Neri, Katia Todoerti, Fortunato Morabito, Adalberto Ibatici, Maurizio Miglino, Micaela Bergamaschi, Silvia Bruno, Gian Mario Sambuceti, Jean Louis Ravetti, Manlio Ferrarini, Franco Fais, and Daniela de Totero

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Bone skeletal alterations are no longer considered a rare event in chronic lymphocytic leukemia (CLL), especially at more advanced stages of the disease. This study is aimed at elucidating the mechanisms underlying this phenomenon. Bone marrow stromal cells, induced to differentiate toward osteoblasts in osteogenic medium, appeared unable to complete their maturation upon co-culture with CLL cells, CLL-cell-derived conditioned media (CLL-cm) or CLL-sera (CLL-sr). Inhibition of osteoblast differentiation was documented by decreased levels of RUNX2 and osteocalcin mRNA expression, by increased osteopontin and DKK-1 mRNA levels, and by a marked reduction of mineralized matrix deposition. The addition of neutralizing TNFα, IL-11 or anti-IL-6R monoclonal antibodies to these cocultures resulted in restoration of bone mineralization, indicating the involvement of these cytokines. These findings were further supported by silencing TNFα, IL-11 and IL-6 in leukemic cells. We also demonstrated that the addition of CLL-cm to monocytes, previously stimulated with MCSF and RANKL, significantly amplified the formation of large, mature osteoclasts as well as their bone resorption activity. Moreover, enhanced osteoclastogenesis, induced by CLL-cm, was significantly reduced by treating cultures with the anti-TNFα monoclonal antibody infliximab. An analogous effect was observed with the use of the BTK inhibitor, ibrutinib. Interestingly, CLL cells co-cultured with mature osteoclasts were protected from apoptosis and upregulated Ki-67. These experimental results parallel the direct correlation between amounts of TNFα in CLL-sr and the degree of compact bone erosion that we previously described, further strengthening the indication of a reciprocal influence between leukemic cell expansion and bone structure derangement.

Published

2020

2. Torsin A Localization in the Mouse Cerebellar Synaptic Circuitry.

Author

Francesca Puglisi, Valentina Vanni, Giulia Ponterio, Annalisa Tassone, Giuseppe Sciamanna, Paola Bonsi, Antonio Pisani, and Georgia Mandolesi

Subjects

Medicine, Science

Abstract

Torsin A (TA) is a ubiquitous protein belonging to the superfamily of proteins called "ATPases associated with a variety of cellular activities" (AAA(+) ATPase). To date, a great deal of attention has been focused on neuronal TA since its mutant form causes early-onset (DYT1) torsion dystonia, an inherited movement disorder characterized by sustained muscle contractions and abnormal postures. Interestingly, it has been proposed that TA, by interacting with the cytoskeletal network, may contribute to the control of neurite outgrowth and/or by acting as a chaperone at synapses could affect synaptic vesicle turnover and neurotransmitter release. Accordingly, both its peculiar developmental expression in striatum and cerebellum and evidence from DYT1 knock-in mice suggest that TA may influence dendritic arborization and synaptogenesis in the brain. Therefore, to better understand TA function a detailed description of its localization at synaptic level is required. Here, we characterized by means of rigorous quantitative confocal analysis TA distribution in the mouse cerebellum at postnatal day 14 (P14), when both cerebellar synaptogenesis and TA expression peak. We observed that the protein is broadly distributed both in cerebellar cortex and in the deep cerebellar nuclei (DCN). Of note, Purkinje cells (PC) express high levels of TA also in the spines and axonal terminals. In addition, abundant expression of the protein was found in the main GABA-ergic and glutamatergic inputs of the cerebellar cortex. Finally, TA was observed also in glial cells, a cellular population little explored so far. These results extend our knowledge on TA synaptic localization providing a clue to its potential role in synaptic development.

Published

2013

3. Developmental profile of the aberrant dopamine D2 receptor response in striatal cholinergic interneurons in DYT1 dystonia.

Author

Giuseppe Sciamanna, Annalisa Tassone, Giuseppina Martella, Georgia Mandolesi, Francesca Puglisi, Dario Cuomo, Grazia Madeo, Giulia Ponterio, David George Standaert, Paola Bonsi, and Antonio Pisani

Subjects

Medicine, Science

Abstract

DYT1 dystonia, a severe form of genetically determined human dystonia, exhibits reduced penetrance among carriers and begins usually during adolescence. The reasons for such age dependence and variability remain unclear.We characterized the alterations in D2 dopamine receptor (D2R) signalling in striatal cholinergic interneurons at different ages in mice overexpressing human mutant torsinA (hMT). An abnormal excitatory response to the D2R agonist quinpirole was recorded at postnatal day 14, consisting of a membrane depolarization coupled to an increase in spiking frequency, and persisted unchanged at 3 and 9 months in hMT mice, compared to mice expressing wild-type human torsinA and non-transgenic mice. This response was blocked by the D2R antagonist sulpiride and depended upon G-proteins, as it was prevented by intrapipette GDP-β-S. Patch-clamp recordings from dissociated interneurons revealed a significant increase in the Cav2.2-mediated current fraction at all ages examined. Consistently, chelation of intracellular calcium abolished the paradoxical response to quinpirole. Finally, no gross morphological changes were observed during development.These results suggest that an imbalanced striatal dopaminergic/cholinergic signaling occurs early in DYT1 dystonia and persists along development, representing a susceptibility factor for symptom generation.

Published

2011

4. 'Green-reduced' graphene oxide induces in vitro an enhanced biomimetic mineralization of polycaprolactone electrospun meshes

Author

Silvia Scaglione, Alessandra Marrella, Paolo Giannoni, Giacomo Tedeschi, Alberto Lagazzo, Rodolfo Quarto, Fabrizio Barberis, Francesca Puglisi, and Francesca Sbrana

Subjects

Materials science, Polyesters, Nanofibers, Oxide, Bioengineering, 02 engineering and technology, 010402 general chemistry, 01 natural sciences, Bone and Bones, law.invention, Biomaterials, Extracellular matrix, Mice, chemistry.chemical_compound, Calcification, Physiologic, Biomimetic Materials, Osteogenesis, law, Ultimate tensile strength, Animals, mineralization, Reduced graphene oxide, bone tissue engineering, Cell adhesion, electrospinning, roughness, Osteoblasts, Tissue Engineering, Graphene, technology, industry, and agriculture, Cell Differentiation, Fibroblasts, 021001 nanoscience & nanotechnology, Ascorbic acid, Reduced graphene oxide, PCL, electrospinning, roughness, mineralization, bone tissue engineering, Electrospinning, 0104 chemical sciences, Chemical engineering, chemistry, PCL, Mechanics of Materials, Polycaprolactone, NIH 3T3 Cells, Graphite, 0210 nano-technology, Oxidation-Reduction

Abstract

A novel green method for graphene oxide (GO) reduction via ascorbic acid has been adopted to realize bio-friendly reduced graphene oxide (RGO)/polycaprolactone (PCL) nanofibrous meshes, as substrates for bone tissue engineering applications. PCL fibrous mats enriched with either RGO or GO (0.25 wt%) were fabricated to recapitulate the fibrillar structure of the bone extracellular matrix (ECM) and the effects of RGO incorporation on the structural proprieties, biomechanics and bioactivity of the nano-composites meshes were evaluated. RGO/PCL fibrous meshes displayed superior mechanical properties (i.e. Young's Modulus and ultimate tensile strength) besides supporting noticeably improved cell adhesion, spreading and proliferation of fibroblasts and osteoblast-like cell lines. Furthermore, RGO-based electrospun substrates enhanced in vitro calcium deposition in the ECM produced by osteoblast-like cells, which was paralleled, in human mesenchymal stem cells grown onto the same substrates, by an increased expression of the osteogenic markers mandatory for mineralization. In this respect, the capability of graphene-based materials to adsorb osteogenic factors cooperates synergically with the rougher surface of RGO/PCL-based materials, evidenced by AFM analysis, to ignite mineralization of the neodeposited matrix and to promote the osteogenic commitment of the cultured cell in the surrounding microenvironment.

Published

2018

5. Chronic lymphocytic leukemia cells impair osteoblastogenesis and promote osteoclastogenesis: role of TNF?, IL-6 and IL-11 cytokines

Author

Cecilia Marini, Maria Cristina Capra, Fortunato Morabito, Paolo Giannoni, Simona Pigozzi, Daniela de Totero, Giovanna Cutrona, Francesca Puglisi, Adalberto Ibatici, Manlio Ferrarini, Katia Todoerti, Silvia Bruno, Paola Luzzi, Micaela Bergamaschi, Serena Matis, Maurizio Miglino, Gian Mario Sambuceti, Jean Louis Ravetti, Gabriele Gaggero, Antonino Neri, and Franco Fais

Subjects

Stromal cell, Chronic lymphocytic leukemia, Osteoclasts, Article, Bone resorption, Osteogenesis, immune system diseases, hemic and lymphatic diseases, medicine, Humans, Chronic Lymphocytic Leukemia, Osteopontin, osteoblastogenesis, Cells, Cultured, osteoclastogenesis, Osteoblasts, biology, Interleukin-6, Tumor Necrosis Factor-alpha, Chemistry, Bone Marrow Microenvironment, Mesenchymal Stem Cells, Cell Differentiation, Osteoblast, Hematology, Interleukin-11, medicine.disease, Leukemia, Lymphocytic, Chronic, B-Cell, medicine.anatomical_structure, RANKL, Cancer research, biology.protein, Osteocalcin, Cytokines, Bone marrow

Abstract

Bone skeletal alterations are no longer considered a rare event in chronic lymphocytic leukemia (CLL), especially at more advanced stages of the disease. This study is aimed at elucidating the mechanisms underlying this phenomenon. Bone marrow stromal cells, induced to differentiate toward osteoblasts in osteogenic medium, appeared unable to complete their maturation upon co-culture with CLL cells, CLL-cell-derived conditioned media (CLL-cm) or CLL-sera (CLL-sr). Inhibition of osteoblast differentiation was documented by decreased levels of RUNX2 and osteocalcin mRNA expression, by increased osteopontin and DKK-1 mRNA levels, and by a marked reduction of mineralized matrix deposition. The addition of neutralizing TNFα, IL-11 or anti-IL-6R monoclonal antibodies to these cocultures resulted in restoration of bone mineralization, indicating the involvement of these cytokines. These findings were further supported by silencing TNFα, IL-11 and IL-6 in leukemic cells. We also demonstrated that the addition of CLL-cm to monocytes, previously stimulated with MCSF and RANKL, significantly amplified the formation of large, mature osteoclasts as well as their bone resorption activity. Moreover, enhanced osteoclastogenesis, induced by CLL-cm, was significantly reduced by treating cultures with the anti-TNFα monoclonal antibody infliximab. An analogous effect was observed with the use of the BTK inhibitor, ibrutinib. Interestingly, CLL cells co-cultured with mature osteoclasts were protected from apoptosis and upregulated Ki-67. These experimental results parallel the direct correlation between amounts of TNFα in CLL-sr and the degree of compact bone erosion that we previously described, further strengthening the indication of a reciprocal influence between leukemic cell expansion and bone structure derangement.

Published

2021

6. Cerebellar synaptogenesis is compromised in mouse models of DYT1 dystonia

Author

Antonio Pisani, Georgia Mandolesi, Paola Bonsi, Valentina Vanni, Francesca Puglisi, Giulia Ponterio, and Marta Maltese

Subjects

Genetically modified mouse, Cerebellum, Neurogenesis, Synaptogenesis, Mice, Transgenic, Parallel fiber, Development, Biology, Glutamatergic synapse, Torsion dystonia, Mice, Developmental Neuroscience, medicine, Animals, Humans, ΔGAG mutant torsinA, GABAergic synapse, Cells, Cultured, gamma-Aminobutyric Acid, Neurons, Dystonia, DYT1 dystonia, Age Factors, Climbing fiber, medicine.disease, Coculture Techniques, Purkinje cells, Disease Models, Animal, HEK293 Cells, medicine.anatomical_structure, Animals, Newborn, Gene Expression Regulation, Receptors, Glutamate, Neurology, Mutation, Synapses, Vesicular Glutamate Transport Protein 1, Knockout mouse, Settore MED/26 - Neurologia, Neuroscience, Molecular Chaperones

Abstract

Early-onset torsion dystonia (DYT1) is an autosomal-dominant movement disorder characterized by sustained muscle contractions and abnormal posturing. It is caused by a three base-pair deletion (ΔGAG) in the gene encoding the AAA(+) protein torsinA, which gives rise to a loss of function mutation responsible of neuronal functional abnormalities. Symptoms typically appear during childhood, suggesting the presence of an early critical period of sensorimotor circuit susceptibility to torsinA dysfunction. Here, we identified in two different DYT1 mouse strains, heterozygous torsinA knockout mice (Tor1a+/-) and human ΔGAG mutant torsinA transgenic mice (hMT), the anatomical abnormalities in the cerebellum, during a critical age for synaptogenesis (postnatal day 14, P14). By means of immunofluorescence, confocal analysis and western blot quantification, we observed a reduced inhibitory input on Purkinje cells (PCs) as well as an unbalanced excitatory innervation; a significant reduction of the parallel fiber (PF) synaptic terminals and an increase of the climbing fiber (CF) inputs. Finally, in support of the in vivo results, we also provide evidence of an impaired PF synaptogenesis in a co-culture system. Of note, these alterations were rescued and in part over-compensated in the adult age in both mouse strains, suggesting that torsinA dysfunction can induce an altered maturation of cerebellar synaptic contacts. Altogether these results indicate that a loss of function of torsinA during cerebellar synaptogenesis induces important developmental alterations, that might contribute to the age-dependent susceptibility to develop dystonia in mutation carriers.

Published

2015

7. PINK1 heterozygous mutations induce subtle alterations in dopamine-dependent synaptic plasticity

Author

Graziella Madeo, Nicola Biagio Mercuri, E. Claudio Latagliata, Enza Maria Valente, Giuseppina Martella, Paola Bonsi, Stefano Puglisi-Allegra, Jie Shen, Mauro Federici, Francesca Puglisi, Antonio Pisani, and Tommaso Schirinzi

Subjects

medicine.medical_specialty, Synaptic cleft, Dopaminergic, Long-term potentiation, Substantia nigra, Biology, Compound heterozygosity, Endocrinology, nervous system, Neurology, Dopamine, Dopamine receptor, Internal medicine, Synaptic plasticity, medicine, Neurology (clinical), Neuroscience, medicine.drug

Abstract

Homozygous or compound heterozygous mutations in the phosphatase and tensin homolog-induced putative kinase 1 (PINK1) gene are causative of autosomal recessive, early onset Parkinson's disease. Single heterozygous mutations have been detected repeatedly both in a subset of patients and in unaffected individuals, and the significance of these mutations has long been debated. Several neurophysiological studies from non-manifesting PINK1 heterozygotes have demonstrated the existence of neural plasticity abnormalities, indicating the presence of specific endophenotypic traits in the heterozygous state. We performed a functional analysis of corticostriatal synaptic plasticity in heterozygous PINK1 knockout (PINK1(+/-) ) mice using a multidisciplinary approach and observed that, despite normal motor behavior, repetitive activation of cortical inputs to striatal neurons failed to induce long-term potentiation (LTP), whereas long-term depression was normal. Although nigral dopaminergic neurons exhibited normal morphological and electrophysiological properties with normal responses to dopamine receptor activation, a significantly lower dopamine release was measured in the striatum of PINK1(+/-) mice compared with control mice, suggesting that a decrease in stimulus-evoked dopamine overflow acts as a major determinant for the LTP deficit. Accordingly, pharmacological agents capable of increasing the availability of dopamine in the synaptic cleft restored normal LTP in heterozygous mice. Moreover, monoamine oxidase B inhibitors rescued physiological LTP and normal dopamine release. Our results provide novel evidence for striatal plasticity abnormalities, even in the heterozygous disease state. These alterations might be considered an endophenotype to this monogenic form of Parkinson's disease and a valid tool with which to characterize early disease stage and design possible disease-modifying therapies.

Published

2013

8. Review of Ultralingua Dictionaries 6.0

Author

John Gruber-Miller, Bettina Schnell, Francesca Puglisi, Esperanza Román-Mendoza, Nadia Rodríguez, and Germán Ruipérez

Subjects

Linguistics and Language, Language and Linguistics, Computer Science Applications, Education

Published

2013

9. Conformational modulation mediated by polyglutamine expansion in CAG repeat expansion disease-associated proteins

Author

Paola Martufi, Andreas Weiss, Cristina Cariulo, Manuel Daldin, Lucia Azzollini, Douglas Macdonald, Francesca Puglisi, Maria Blaire Bustamante, Andrea Caricasole, Valentina Fodale, Lara Petricca, and Margherita Verani

Subjects

0301 basic medicine, Cell Extracts, Conformational change, Huntingtin, Biophysics, Molecular Conformation, Biology, Transfection, Biochemistry, Epitope, 03 medical and health sciences, 0302 clinical medicine, medicine, Huntingtin Protein, Fluorescence Resonance Energy Transfer, Humans, Disease, Molecular Biology, Immunoassay, Neurodegeneration, Cell Biology, medicine.disease, Molecular biology, Cell biology, 030104 developmental biology, HEK293 Cells, Spinocerebellar ataxia, biology.protein, TATA-binding protein, Trinucleotide repeat expansion, Peptides, Trinucleotide Repeat Expansion, 030217 neurology & neurosurgery

Abstract

We have previously reported TR-FRET based immunoassays to detect a conformational change imparted on huntingtin protein by the polyglutamine expansion, which we confirmed using biophysical methodologies. Using these immunoassays, we now report that polyglutamine expansion influences the conformational properties of other polyglutamine disease proteins, exemplified by the androgen receptor (associated with spinal bulbar muscular atrophy) and TATA binding protein (associated with spinocerebellar ataxia 17). Using artificial constructs bearing short or long polyglutamine expansions or a multimerized, unrelated epitope (mimicking the increase in anti-polyglutamine antibody epitopes present in polyglutamine repeats of increasing length) we confirmed that the conformational TR-FRET based immunoassay detects an intrinsic conformational property of polyglutamine repeats. The TR-FRET based conformational immunoassay may represent a rapid, scalable tool to identify modulators of polyglutamine-mediated conformational change in different proteins associated with CAG triplet repeat disorders.

Published

2016

10. Exposure to low-dose rotenone precipitates synaptic plasticità alterations in PINK1 heterozygous knockout mice

Author

Graziella Madeo, Laura Bonanni, Francesca Puglisi, Valentina Vanni, Jie Shen, Antonio Pisani, Elisabetta Ferraro, Enza Maria Valente, Giuseppina Martella, Nicola Biagio Mercuri, Paola Bonsi, Marta Maltese, Georgia Mandolesi, and Tommaso Schirinzi

Subjects

0301 basic medicine, medicine.medical_specialty, Electrophysiology, Mitochondria, PINK1 heterozygous mutations, Parkinson's disease, Rotenone, Striatum, Synaptic plasticity, Substantia nigra, Biology, Medium spiny neuron, Neuroprotection, lcsh:RC321-571, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Internal medicine, medicine, LTP induction, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Long-term potentiation, 030104 developmental biology, Endocrinology, Neurology, chemistry, Biochemistry, Knockout mouse, Settore MED/26 - Neurologia, 030217 neurology & neurosurgery

Abstract

Heterozygous mutations in the PINK1 gene are considered a susceptibility factor to develop early-onset Parkinson's disease (PD), as supported by dopamine hypometabolism in asymptomatic mutation carriers and subtle alterations of dopamine-dependent striatal synaptic plasticity in heterozygous PINK1 knockout (PINK1(+/-)) mice. The aim of the present study was to investigate whether exposure to low-dose rotenone of heterozygous PINK1(+/-) mice, compared to their wild-type PINK1(+/+) littermates, could impact on dopamine-dependent striatal synaptic plasticity, in the absence of apparent structural alterations. Mice were exposed to a range of concentrations of rotenone (0.01-1mg/kg). Chronic treatment with concentrations of rotenone up to 0.8mg/kg did not cause manifest neuronal loss or changes in ATP levels both in the striatum or substantia nigra of PINK1(+/-) and PINK1(+/+) mice. Moreover, rotenone (up to 0.8mg/kg) treatment did not induce mislocalization of the mitochondrial membrane protein Tom20 and release of cytochrome c in PINK1(+/-) striata. Accordingly, basic electrophysiological properties of nigral dopaminergic and striatal medium spiny neurons (MSNs) were normal. Despite the lack of gross alterations in neuronal viability in chronically-treated PINK1(+/-), a complete loss of both long-term depression (LTD) and long-term potentiation (LTP) was recorded in MSNs from PINK1(+/-) mice treated with a low rotenone (0.1mg/kg) concentration. Even lower concentrations (0.01mg/kg) blocked LTP induction in heterozygous PINK1(+/-) MSNs compared to PINK1(+/+) mice. Of interest, chronic pretreatment with the antioxidants alpha-tocopherol and Trolox, a water-soluble analog of vitamin E and powerful antioxidant, rescued synaptic plasticity impairment, confirming that, at the doses we utilized, rotenone did not induce irreversible alterations. In this model, chronic exposure to low-doses of rotenone was not sufficient to alter mitochondrial integrity and ATP production, but profoundly impaired the expression of long-term plasticity at corticostriatal synapses in PINK1 heterozygous knockout mice, suggesting that disruption of synaptic plasticity may represent an early feature of a pre-manifesting state of the disease, and a potential tool to test novel neuroprotective agents.

Published

2016

11. Torsin A Localization in the Mouse Cerebellar Synaptic Circuitry

Author

Giulia Ponterio, Francesca Puglisi, Paola Bonsi, Valentina Vanni, Antonio Pisani, Annalisa Tassone, Giuseppe Sciamanna, and Georgia Mandolesi

Subjects

Cerebellum, Neurite, Population, Synaptogenesis, Glutamic Acid, lcsh:Medicine, Biology, Deep cerebellar nuclei, Bioinformatics, Synaptic vesicle, chemistry.chemical_compound, Mice, medicine, Animals, Neurotransmitter, education, lcsh:Science, gamma-Aminobutyric Acid, education.field_of_study, Multidisciplinary, lcsh:R, Mice, Inbred C57BL, medicine.anatomical_structure, chemistry, nervous system, Cerebellar cortex, Synapses, Settore MED/26 - Neurologia, lcsh:Q, Neuroscience, Research Article, Molecular Chaperones

Abstract

Torsin A (TA) is a ubiquitous protein belonging to the superfamily of proteins called "ATPases associated with a variety of cellular activities" (AAA(+) ATPase). To date, a great deal of attention has been focused on neuronal TA since its mutant form causes early-onset (DYT1) torsion dystonia, an inherited movement disorder characterized by sustained muscle contractions and abnormal postures. Interestingly, it has been proposed that TA, by interacting with the cytoskeletal network, may contribute to the control of neurite outgrowth and/or by acting as a chaperone at synapses could affect synaptic vesicle turnover and neurotransmitter release. Accordingly, both its peculiar developmental expression in striatum and cerebellum and evidence from DYT1 knock-in mice suggest that TA may influence dendritic arborization and synaptogenesis in the brain. Therefore, to better understand TA function a detailed description of its localization at synaptic level is required. Here, we characterized by means of rigorous quantitative confocal analysis TA distribution in the mouse cerebellum at postnatal day 14 (P14), when both cerebellar synaptogenesis and TA expression peak. We observed that the protein is broadly distributed both in cerebellar cortex and in the deep cerebellar nuclei (DCN). Of note, Purkinje cells (PC) express high levels of TA also in the spines and axonal terminals. In addition, abundant expression of the protein was found in the main GABA-ergic and glutamatergic inputs of the cerebellar cortex. Finally, TA was observed also in glial cells, a cellular population little explored so far. These results extend our knowledge on TA synaptic localization providing a clue to its potential role in synaptic development.

Published

2013

12. Developmental profile of the aberrant dopamine D2 receptor response in striatal cholinergic interneurons in DYT1 dystonia

Author

Grazia Madeo, Giuseppina Martella, Antonio Pisani, Francesca Puglisi, Paola Bonsi, Giulia Ponterio, Georgia Mandolesi, David G. Standaert, Giuseppe Sciamanna, Annalisa Tassone, and Dario Cuomo

Subjects

Anatomy and Physiology, Dopamine, lcsh:Medicine, GTP-Binding Protein alpha Subunits, Gi-Go, Gi-Go, Mice, 0302 clinical medicine, Receptors, lcsh:Science, Dystonia, 0303 health sciences, Multidisciplinary, Movement Disorders, Dopaminergic, Neurochemistry, GTP-Binding Protein alpha Subunits, Electrophysiology, Neurology, Dopamine receptor, Medicine, Settore MED/26 - Neurologia, Neurochemicals, Receptor, medicine.drug, Signal Transduction, Research Article, Agonist, medicine.medical_specialty, Receptor, Adenosine A2A, medicine.drug_class, Electrophysiological Processes, Biology, Adenosine A2A, 03 medical and health sciences, Quinpirole, Interneurons, Internal medicine, Dopamine receptor D2, Dopamine D2, medicine, Animals, Humans, 030304 developmental biology, Receptors, Dopamine D2, lcsh:R, Calcium, Neostriatum, Acetylcholine, Molecular Chaperones, Mutation, medicine.disease, Electrophysiological Phenomena, Endocrinology, Cholinergic, lcsh:Q, Sulpiride, 030217 neurology & neurosurgery, Neuroscience

Abstract

Background DYT1 dystonia, a severe form of genetically determined human dystonia, exhibits reduced penetrance among carriers and begins usually during adolescence. The reasons for such age dependence and variability remain unclear. Methods and Results We characterized the alterations in D2 dopamine receptor (D2R) signalling in striatal cholinergic interneurons at different ages in mice overexpressing human mutant torsinA (hMT). An abnormal excitatory response to the D2R agonist quinpirole was recorded at postnatal day 14, consisting of a membrane depolarization coupled to an increase in spiking frequency, and persisted unchanged at 3 and 9 months in hMT mice, compared to mice expressing wild-type human torsinA and non-transgenic mice. This response was blocked by the D2R antagonist sulpiride and depended upon G-proteins, as it was prevented by intrapipette GDP-β-S. Patch-clamp recordings from dissociated interneurons revealed a significant increase in the Cav2.2-mediated current fraction at all ages examined. Consistently, chelation of intracellular calcium abolished the paradoxical response to quinpirole. Finally, no gross morphological changes were observed during development. Conclusions These results suggest that an imbalanced striatal dopaminergic/cholinergic signaling occurs early in DYT1 dystonia and persists along development, representing a susceptibility factor for symptom generation.

Published

2011

13. Activation of 5-HT6 receptors inhibits corticostriatal glutamatergic transmission

Author

Annalisa Tassone, Franco Borsini, Graziella Madeo, Antonio Pisani, Paola Bonsi, Francesca Puglisi, Daniela Vita, Tommaso Schirinzi, and Giulia Ponterio

Subjects

Male, Indoles, Postsynaptic Current, Glutamic Acid, Inhibitory postsynaptic potential, Medium spiny neuron, Synaptic Transmission, Cellular and Molecular Neuroscience, Glutamatergic, Postsynaptic potential, Ethylamines, Animals, Rats, Wistar, Pharmacology, Cerebral Cortex, Post-tetanic potentiation, Chemistry, Excitatory Postsynaptic Potentials, Neural Inhibition, Corpus Striatum, Rats, Serotonin Receptor Agonists, Receptors, Serotonin, Excitatory postsynaptic potential, Settore MED/26 - Neurologia, Neuroscience, Postsynaptic density

Abstract

We investigated the effect of 5-HT6 receptor subtype activation on glutamatergic transmission by means of whole-cell patch-clamp electrophysiological recordings from medium spiny neurons of the striatum and layer V pyramidal neurons of the prefrontal cortex. To this aim, we took advantage of a novel ligand, ST1936, showing nM affinity and agonist activity at the 5-HT6 receptor subtype. Our data show that 5-HT6 receptor activation by ST1936 reduces the frequency of spontaneous excitatory postsynaptic currents, with an IC50 of 1.3 μM. Moreover, 5-HT6 receptor activation also reduced the amplitude of spontaneous excitatory postsynaptic currents recorded from medium spiny neurons, suggesting a mechanism of action involving postsynaptic 5-HT6 receptors,as further confirmed by the paired-pulse analysis on evoked excitatory postsynaptic currents and by recordings of miniature glutamatergic events. The inhibitory effect of ST1936 on glutamatergic transmission was prevented by the selective 5-HT6 receptor antagonist SB258585 and mimicked by a different agonist, WAY-181187. Conversely, in the cortex ST1936 reduced the frequency, but not the amplitude, of spontaneous excitatory postsynaptic currents suggesting a presynaptic or indirect effect of the 5-HT6 receptor.

Published

2010

14. Distribution of the SNAP25 and SNAP23 synaptosomal-associated protein isoforms in rat cerebellar cortex

Author

V. Vanni, P. Cesare, Georgia Mandolesi, Roberta Cesa, Giorgio Grasselli, Francesca Puglisi, and Piergiorgio Strata

Subjects

Cerebellum, Synaptosomal-Associated Protein 25, Vesicular glutamate transporter 1, Purkinje cell, Presynaptic Terminals, Vesicular Transport Proteins, Glutamic Acid, Parallel fiber, Synaptic Transmission, Cerebellar Cortex, Nerve Fibers, Interneurons, medicine, Animals, Protein Isoforms, Rats, Wistar, Microscopy, Immunoelectron, Microscopy, Confocal, biology, General Neuroscience, SNAP25, Climbing fiber, Immunohistochemistry, Cell biology, Rats, Synaptic vesicle exocytosis, medicine.anatomical_structure, Cerebellar cortex, Vesicular Glutamate Transport Protein 1, biology.protein, Vesicular Glutamate Transport Protein 2, Neuroscience, Synaptosomes

Abstract

Synaptosome-associated protein of 25 kDa (SNAP25) is a component of the fusion complex that mediates synaptic vesicle exocytosis, regulates calcium dynamics and neuronal plasticity. Despite its crucial role in vesicle release, SNAP25 is not distributed homogenously within the brain. It seems to be virtually absent in mature inhibitory terminals and is observed in a subtype of excitatory neurons defined by the expression of vesicular glutamate transporter 1 (VGluT1). Since a complementary distribution of VGluT1 and VGluT2 in excitatory synapses is correlated with different probabilities of release (Pr), we evaluated whether SNAP25 localization is associated with specific synaptic properties. In the cerebellum, climbing fiber (CF) and parallel fiber (PF) inputs, which impinge onto the same Purkinje cell (PC), have very different functional properties. In the cerebellum of adult rats, using confocal and electron microscopy, we observed that VGluT2-positive CFs, characterized by a high Pr, only weakly express SNAP25, while VGluT1-positive PFs that show a low Pr abundantly express SNAP25. Moreover, SNAP25 was less profuse in the VGluT2-positive rosettes of mossy fibers (MFs) and was almost absent in inhibitory terminals. We extended our analysis to the SNAP23 homolog; this is expressed at different levels in both gamma-aminobutyric acid-containing terminals (GABAergic) and glutamatergic terminals of the cerebellar cortex. In conclusion, the preferential localization of SNAP25 in specific synaptic boutons suggests a correlation between SNAP25 and the Pr. This evidence supports the hypothesis that SNAP25 has a modulatory role in shaping synaptic responses.

Published

2009

15. Detection of huntingtin exon 1 phosphorylation by Phos-Tag SDS-PAGE: Predominant phosphorylation on threonine 3 and regulation by IKKβ

Author

Cristina Cariulo, Lucia Azzollini, Lara Petricca, Jeppe Falsig Pedersen, Annalisa Ansaloni, Zhe Ming Wang, Hilal A. Lashuel, Francesca Puglisi, Maria Blaire Bustamante, Andrea Caricasole, Hyunsun Park, and Margherita Verani

Subjects

Threonine, congenital, hereditary, and neonatal diseases and abnormalities, Huntingtin, Mutant, Biophysics, Nerve Tissue Proteins, Biology, Biochemistry, Exon, SETD2, mental disorders, Humans, Phosphorylation, Molecular Biology, chemistry.chemical_classification, Huntingtin Protein, Exons, Cell Biology, Polyglutamine tract, nervous system diseases, Amino acid, HEK293 Cells, chemistry, Electrophoresis, Polyacrylamide Gel, I-kappa B Proteins

Abstract

Expansion of a CAG triplet repeat within the first exon of the HUNTINGTIN gene encoding for a polyglutamine tract is the cause of a progressive neurodegenerative disorder known as Huntington's disease. N-terminal fragments of mutant huntingtin have a strong propensity to form oligomers and aggregates that have been linked to the Huntington's disease pathology by different mechanisms, including gain of toxic functions. The biological and biophysical properties of the polyglutamine expansion within these huntingtin fragments are influenced by neighboring domains, in particular by the first 17 amino acids of huntingtin (N17), which precede the polyglutamine expansion. It has been suggested that N17 phosphorylation modulate mutant huntingtin aggregation and toxicity, but the study of its functional and pathological relevance requires the capacity to detect this modification in biological samples in a simple, robust way, that ideally provides information on the abundance of a phosphorylated species relative to the total pool of the protein of interest. Using a modified SDS-PAGE protocol (Phos-Tag) followed by Western blotting with specific anti-HUNTINGTIN antibodies, we efficiently resolved huntingtin fragments expressed in cellular contexts based on the presence of phosphorylated residues, we defined threonine 3 as the major site of huntingtin N17 phosphorylation and, finally, we identified IKK-beta as a kinase capable of phosphorylating threonine 3 in N-terminal hungtingtin fragments.