Changes in glial cell activation and extracellular vesicles production precede the onset of disease symptoms in transgenic hSOD1<sup>G93A</sup> pigs.

Golia, Maria Teresa; Frigerio, Roberto; Pucci, Susanna; Sironi, Francesca; Margotta, Cassandra; Pasetto, Laura; Testori, Camilla; Berrone, Elena; Ingravalle, Francesco; Chiari, Marcella; Gori, Alessandro; Duchi, Roberto; Perota, Andrea; Bergamaschi, Luca; D'Angelo, Antonio; Cagnotti, Giulia; Galli, Cesare; Corona, Cristiano; Bonetto, Valentina; Bendotti, Caterina; Cretich, Marina; Colombo, Sara Francesca; Verderio, Claudia

Changes in glial cell activation and extracellular vesicles production precede the onset of disease symptoms in transgenic hSOD1^G93A pigs.

Golia, Maria Teresa; Frigerio, Roberto; Pucci, Susanna; Sironi, Francesca; Margotta, Cassandra; Pasetto, Laura; Testori, Camilla; Berrone, Elena; Ingravalle, Francesco; Chiari, Marcella; Gori, Alessandro; Duchi, Roberto; Perota, Andrea; Bergamaschi, Luca; D'Angelo, Antonio; Cagnotti, Giulia; Galli, Cesare; Corona, Cristiano; Bonetto, Valentina; Bendotti, Caterina; Cretich, Marina; Colombo, Sara Francesca; Verderio, Claudia.

Afiliação

Golia MT; National Research Council of Italy, Institute of Neuroscience (IN-CNR), Via Raoul Follereau 3, 20854 Vedano al Lambro, Italy.
Frigerio R; National Research Council of Italy, Institute of Chemical Science and Technologies (SCITEC-CNR), Via Mario Bianco 9, 20131 Milan, Italy.
Pucci S; National Research Council of Italy, Institute of Neuroscience (IN-CNR), Via Raoul Follereau 3, 20854 Vedano al Lambro, Italy.
Sironi F; Research Center for ALS, Istituto di Ricerche Farmacologiche Mario Negri IRCCS, Via Mario Negri, 2, 20156 Milano, Italy.
Margotta C; Research Center for ALS, Istituto di Ricerche Farmacologiche Mario Negri IRCCS, Via Mario Negri, 2, 20156 Milano, Italy.
Pasetto L; Research Center for ALS, Istituto di Ricerche Farmacologiche Mario Negri IRCCS, Via Mario Negri, 2, 20156 Milano, Italy.
Testori C; Istituto Zooprofilattico Sperimentale del Piemonte Liguria e Valle d'Aosta (IZSPLV), Via Bologna 148, 10154 Torino, Italy.
Berrone E; Istituto Zooprofilattico Sperimentale del Piemonte Liguria e Valle d'Aosta (IZSPLV), Via Bologna 148, 10154 Torino, Italy.
Ingravalle F; Istituto Zooprofilattico Sperimentale del Piemonte Liguria e Valle d'Aosta (IZSPLV), Via Bologna 148, 10154 Torino, Italy.
Chiari M; National Research Council of Italy, Institute of Chemical Science and Technologies (SCITEC-CNR), Via Mario Bianco 9, 20131 Milan, Italy.
Gori A; National Research Council of Italy, Institute of Chemical Science and Technologies (SCITEC-CNR), Via Mario Bianco 9, 20131 Milan, Italy.
Duchi R; Avantea, Laboratory of Reproductive Technologies, Via Porcellasco 7/F, 26100 Cremona, Italy.
Perota A; Avantea, Laboratory of Reproductive Technologies, Via Porcellasco 7/F, 26100 Cremona, Italy.
Bergamaschi L; Avantea, Laboratory of Reproductive Technologies, Via Porcellasco 7/F, 26100 Cremona, Italy.
D'Angelo A; Department of Veterinary Sciences, University of Turin, Largo Paolo Braccini 2, 10095 Grugliasco, Torino, Italy.
Cagnotti G; Department of Veterinary Sciences, University of Turin, Largo Paolo Braccini 2, 10095 Grugliasco, Torino, Italy.
Galli C; Avantea, Laboratory of Reproductive Technologies, Via Porcellasco 7/F, 26100 Cremona, Italy.
Corona C; Istituto Zooprofilattico Sperimentale del Piemonte Liguria e Valle d'Aosta (IZSPLV), Via Bologna 148, 10154 Torino, Italy.
Bonetto V; Research Center for ALS, Istituto di Ricerche Farmacologiche Mario Negri IRCCS, Via Mario Negri, 2, 20156 Milano, Italy.
Bendotti C; Research Center for ALS, Istituto di Ricerche Farmacologiche Mario Negri IRCCS, Via Mario Negri, 2, 20156 Milano, Italy.
Cretich M; National Research Council of Italy, Institute of Chemical Science and Technologies (SCITEC-CNR), Via Mario Bianco 9, 20131 Milan, Italy.
Colombo SF; National Research Council of Italy, Institute of Neuroscience (IN-CNR), Via Raoul Follereau 3, 20854 Vedano al Lambro, Italy.
Verderio C; National Research Council of Italy, Institute of Neuroscience (IN-CNR), Via Raoul Follereau 3, 20854 Vedano al Lambro, Italy. Electronic address: c.verderio@in.cnr.it.

Exp Neurol ; 374: 114716, 2024 Apr.

Article em En | MEDLINE | ID: mdl-38331161

ABSTRACT

ABSTRACT

SOD1 gene is associated with progressive motor neuron degeneration in the familiar forms of amyotrophic lateral sclerosis. Although studies on mutant human SOD1 transgenic rodent models have provided important insights into disease pathogenesis, they have not led to the discovery of early biomarkers or effective therapies in human disease. The recent generation of a transgenic swine model expressing the human pathological hSOD1G93A gene, which recapitulates the course of human disease, represents an interesting tool for the identification of early disease mechanisms and diagnostic biomarkers. Here, we analyze the activation state of CNS cells in transgenic pigs during the disease course and investigate whether changes in neuronal and glial cell activation state can be reflected by the amount of extracellular vesicles they release in biological fluids. To assess the activation state of neural cells, we performed a biochemical characterization of neurons and glial cells in the spinal cords of hSOD1G93A pigs during the disease course. Quantification of EVs of CNS cell origin was performed in cerebrospinal fluid and plasma of transgenic pigs at different disease stages by Western blot and peptide microarray analyses. We report an early activation of oligodendrocytes in hSOD1G93A transgenic tissue followed by astrocyte and microglia activation, especially in animals with motor symptoms. At late asymptomatic stage, EV production from astrocytes and microglia is increased in the cerebrospinal fluid, but not in the plasma, of transgenic pigs reflecting donor cell activation in the spinal cord. Estimation of EV production by biochemical analyses is corroborated by direct quantification of neuron- and microglia-derived EVs in the cerebrospinal fluid by a Membrane Sensing Peptide enabled on-chip analysis that provides fast results and low sample consumption. Collectively, our data indicate that alteration in astrocytic EV production precedes the onset of disease symptoms in the hSODG93A swine model, mirroring donor cell activation in the spinal cord, and suggest that EV measurements from the cells first activated in the ALS pig model, i.e. OPCs, may further improve early disease detection.

Assuntos

Esclerose Lateral Amiotrófica; Vesículas Extracelulares; Camundongos; Animais; Humanos; Suínos; Superóxido Dismutase-1/genética; Neurônios Motores/metabolismo; Superóxido Dismutase/genética; Camundongos Transgênicos; Esclerose Lateral Amiotrófica/patologia; Medula Espinal/patologia; Neuroglia/patologia; Biomarcadores/metabolismo; Peptídeos/metabolismo; Modelos Animais de Doenças

Palavras-chave

Biological fluids; Disease biomarkers; Extracellular vesicles; hSOD(G93A) swine model

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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Vesículas Extracelulares / Esclerose Lateral Amiotrófica Tipo de estudo: Diagnostic_studies Limite: Animals / Humans Idioma: En Ano de publicação: 2024 Tipo de documento: Article

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