Your search keyword '"Fornasiero, Arianna"' showing total 11 results

1. Analysis of coding and non-coding transcriptome of peripheral B cells reveals an altered interferon response factor (IRF)-1 pathway in multiple sclerosis patients

Author

Annibali, Viviana, Umeton, Renato, Palermo, Antonia, Severa, Martina, Etna, Marilena Paola, Giglio, Simona, Romano, Silvia, Ferraldeschi, Michela, Buscarinu, Maria Chiara, Vecchione, Andrea, Annese, Anita, Policano, Claudia, Mechelli, Rosella, Pizzolato Umeton, Raffaella, Fornasiero, Arianna, Angelini, Daniela Francesca, Guerrera, Gisella, Battistini, Luca, Coccia, Eliana Marina, Salvetti, Marco, and Ristori, Giovanni

Published

2018

2. Intestinal Permeability and Circulating CD161+CCR6+CD8+T Cells in Patients With Relapsing–Remitting Multiple Sclerosis Treated With Dimethylfumarate.

Author

Buscarinu, Maria C., Gargano, Francesca, Lionetto, Luana, Capi, Matilde, Morena, Emanuele, Fornasiero, Arianna, Reniè, Roberta, Landi, Anna C., Pellicciari, Giulia, Romano, Carmela, Mechelli, Rosella, Romano, Silvia, Borsellino, Giovanna, Battistini, Luca, Simmaco, Maurizio, Fagnani, Corrado, Salvetti, Marco, and Ristori, Giovanni

Subjects

INTESTINES, MULTIPLE sclerosis, PERMEABILITY, DISEASE relapse, T cells

Abstract

Background: The changes of the gut-brain axis have been recently recognized as important components in multiple sclerosis (MS) pathogenesis. Objectives: To evaluate the effects of DMF on intestinal barrier permeability and mucosal immune responses. Methods: We investigated intestinal permeability (IP) and circulating CD161+CCR6+CD8+T cells in 25 patients with MS, who met eligibility criteria for dimethyl-fumarate (DMF) treatment. These data, together with clinical/MRI parameters, were studied at three time-points: baseline (before therapy), after one (T1) and 9 months (T2) of treatment. Results: At baseline 16 patients (64%) showed altered IP, while 14 cases (56%) showed active MRI. During DMF therapy we found the expected decrease of disease activity at MRI compared to T0 (6/25 at T1, p = 0.035 and 3/25 at T2, p < 0.00), and a reduction in the percentage of CD161+CCR6+CD8+ T cells (16/23 at T2; p < 0.001). The effects of DMF on gut barrier alterations was variable, without a clear longitudinal pattern, while we found significant relationships between IP changes and drop of MRI activity (p = 0.04) and circulating CD161+CCr6+CD8+ T cells (p = 0.023). Conclusions: The gut barrier is frequently altered in MS, and the CD161+ CCR6+CD8+ T cell-subset shows dynamics which correlate with disease course and therapy. [ABSTRACT FROM AUTHOR]

Published

2021

3. The Contribution of Gut Barrier Changes to Multiple Sclerosis Pathophysiology.

Author

Buscarinu, Maria Chiara, Fornasiero, Arianna, Romano, Silvia, Ferraldeschi, Michela, Mechelli, Rosella, Reniè, Roberta, Morena, Emanuele, Romano, Carmela, Pellicciari, Giulia, Landi, Anna Chiara, Salvetti, Marco, and Ristori, Giovanni

Subjects

ANIMAL disease models, MULTIPLE sclerosis, ANTIGEN presenting cells, VITAMIN D deficiency, NATALIZUMAB, PATHOLOGICAL physiology

Abstract

The gut barrier consists of several components, including the mucus layer, made of mucins and anti-bacterial molecule, the epithelial cells, connected by tight junction proteins, and a mixed population of cells involved in the interplay with microbes, such as M cells, elongations of "antigen presenting cells" dwelling the lamina propria, intraepithelial lymphocytes and Paneth cells secreting anti-bacterial peptides. Recently, the influence of intestinal permeability (IP) changes on organs far from gut has been investigated, and IP changes in multiple sclerosis (MS) have been described. A related topic is the microbiota dysfunction that underpins the development of neuroinflammation in animal models and human diseases, including MS. It becomes now of interest to better understand the mechanisms through which IP changes contribute to pathophysiology of neuroinflammation. The following aspects seem of relevance: studies on other biomarkers of IP alterations; the relationship with known risk factors for MS development, such as vitamin D deficiency; the link between blood brain barrier and gut barrier breakdown; the effects of IP increase on microbial translocation and microglial activation; the parallel patterns of IP and neuroimmune changes in MS and neuropsychiatric disorders, that afflict a sizable proportion of patients with MS. We will also discuss the therapeutic implications of IP changes, considering the impact of MS-modifying therapies on gut barrier, as well as potential approaches to enhance or protect IP homeostasis. [ABSTRACT FROM AUTHOR]

Published

2019

4. Drug Holiday of Interferon Beta 1b in Multiple Sclerosis: A Pilot, Randomized, Single Blind Study of Non-inferiority.

Author

Romano, Silvia, Ferraldeschi, Michela, Bagnato, Francesca, Mechelli, Rosella, Morena, Emanuele, Caldano, Marzia, Buscarinu, Maria Chiara, Fornasiero, Arianna, Frontoni, Marco, Nociti, Viviana, Mirabella, Massimiliano, Mayer, Flavia, Bertolotto, Antonio, Pozzilli, Carlo, Vanacore, Nicola, Salvetti, Marco, and Ristori, Giovanni

Subjects

INTERFERON beta 1b, MULTIPLE sclerosis, CLINICAL trial registries, THERAPEUTICS, BLACK holes

Abstract

Introduction: To compare a schedule with cyclic withdrawal (CW) of interferon beta (IFN-b) 1b, respect to the full regimen (FR), in relapsing-remitting MS (RR-MS). Methods: Participants were randomly assigned to CW or FR schedule and monthly monitored with brain MRI scans for 12 months (three of run-in and 9 of treatment). CW schedule included drug withdrawal for 1 month after two of treatment for a total of three quarters over the 9-month treatment period. The assessing neurologist and the expert neuroradiologists were blind. After the blind phase of the study all participants took their indicated disease modifying therapies in a prospectively planned, open-label extension phase (up to 120 months). Results: Of 60 randomized subjects 56 (29 in FR and 27 in CW group) completed the single-blind phase: the two groups were comparable, except for a non-significant difference in the number of contrast-enhanced lesions (CEL) at the end of run-in. The two-sided 90% CI for the ratio between median number of cumulative CEL was 0.29–1.07, allowing to significantly reject the null hypothesis of a ratio ≥1.2 and to meet the primary end-point of non-inferiority (the threshold and the ratio between median were chosen according to the non-normal distribution of the data). The differences (CW vs. FR) were also non-significant for secondary end points: mean cumulative number of T2-weighted new and enlarging lesions (3.48 ± 5.34 vs. 3.86 ± 6.76); mean number and volume (cm3) of black holes (1.24 ± 1.61 vs. 2.71 ± 4.56; 489.11 ± 1488.12 vs. 204.48 ± 396.98); number of patients with at least an active scan (21 vs. 22); mean relapse rate (0.52 ± 0.89 vs. 0.34 ± 0.66), relapse risk ratio adjusted for baseline variables (2.15 [0.64–7.18]), EDSS score (1.0 [1–1.56] vs. 1.5 [1–1.78]), proportion of patients with antibodies anti-IFN (5 [21%] vs. 8 [36%]). Fifty-four patients (27 for each study arm) completed the open-label phase. The annualized RR, EDSS, proportion of patients shifting to progressive disease and hazard ratio of shifting, adjusting for baseline covariates, were comparable between the two study groups. Conclusions: A calendar with CW was non-inferior than FR at the beginning of IFN-b therapy, and may not affect the long-term outcome. Clinical Trial Registration: www.ClinicalTrials.gov, identifier: NCT00270816 [ABSTRACT FROM AUTHOR]

Published

2019

5. Genome-Wide Multiple Sclerosis Association Data and Coagulation.

Author

La Starza, Sara, Ferraldeschi, Michela, Buscarinu, Maria Chiara, Romano, Silvia, Fornasiero, Arianna, Mechelli, Rosella, Umeton, Renato, Ristori, Giovanni, and Salvetti, Marco

Subjects

HEMOSTASIS, INFLAMMATION, IMMUNE system, FIBRIN, MULTIPLE sclerosis, PLASMINOGEN activators

Abstract

The emerging concept of a crosstalk between hemostasis, inflammation, and immune system prompt recent works on coagulation cascade in multiple sclerosis (MS). Studies on MS pathology identified several coagulation factors since the beginning of the disease pathophysiology: fibrin deposition with breakdown of blood brain barrier, and coagulation factors within active plaques may exert pathogenic role, especially through the innate immune system. Studies on circulating coagulation factors showed complex imbalance involving several components of hemostasis cascade (thrombin, factor X, factor XII). To analyze the role of the coagulation process in connection with other pathogenic pathways, we implemented a systematic matching of genome-wide association studies (GWAS) data with an informative and unbiased network of coagulation pathways. Using MetaCore (version 6.35 build 69300, 2018) we analyzed the connectivity (i.e., direct and indirect interactions among two networks) between the network of the coagulation process and the network resulting from feeding into MetaCore the MS GWAS data. The two networks presented a remarkable over-connectivity: 958 connections vs. 561 expected by chance; z -score = 17.39; p -value < 0.00001. Moreover, genes coding for cluster of differentiation 40 (CD40) and plasminogen activator, urokinase (PLAU) shared both networks, pointed to an integral interplay between coagulation cascade and main pathogenic immune effectors. In fact, CD40 pathways is especially operative in B cells, that are currently a major therapeutic target in MS field. The potential interaction of PLAU with a signal of paramount importance for B cell pathogenicity, such as CD40, suggest new lines of research and pave the way to implement new therapeutic targets. [ABSTRACT FROM AUTHOR]

Published

2019

6. Fingolimod vs dimethyl fumarate in multiple sclerosis: A real-world propensity score-matched study.

Author

Prosperini, Luca, Lucchini, Matteo, Haggiag, Shalom, Bellantonio, Paolo, Bianco, Assunta, Buscarinu, Maria Chiara, Buttari, Fabio, Centonze, Diego, Cortese, Antonio, De Giglio, Laura, Fantozzi, Roberta, Ferraro, Elisabetta, Fornasiero, Arianna, Francia, Ada, Galgani, Simonetta, Gasperini, Claudio, Marfia, Girolama Alessandra, Millefiorini, Enrico, Nociti, Viviana, and Pontecorvo, Simona

Published

2018

7. Altered intestinal permeability in patients with relapsing–remitting multiple sclerosis: A pilot study.

Author

Buscarinu, Maria Chiara, Cerasoli, Benedetta, Annibali, Viviana, Policano, Claudia, Mechelli, Rosella, Romano, Silvia, Fornasiero, Arianna, Mattei, Gianluca, Umeton, Renato, Salvetti, Marco, Ristori, Giovanni, Lionetto, Luana, Capi, Matilde, Simmaco, Maurizio, Piras, Eleonora, Angelini, Daniela Francesca, and Battistini, Luca

Subjects

MULTIPLE sclerosis diagnosis, INTESTINAL diseases, DISEASE relapse, PATHOGENIC microorganisms, MULTIPLE sclerosis treatment, T cells

Abstract

Background: Alterations of intestinal permeability (IP) may contribute to the pathophysiology of immune-mediated diseases. Objective: We investigated the possible association between IP changes and multiple sclerosis (MS). Methods: We studied 22 patients with relapsing–remitting multiple sclerosis (RRMS) and 18 age- and sex-matched healthy donors (HDs), including five twin pairs (one concordant, and four discordant for disease). Measurement of lactulose (L) and mannitol (M; two non-metabolized sugars) levels in urine samples, after an oral load, allowed to quantify gut dysfunction. Results: The proportion of participants with increased IP was significantly higher in patients than in HDs (16/22 (73%) versus 5/18 (28%); p = 0.001). Accordingly, the L/M urinary ratio showed significantly higher values in patients than in controls (p = 0.0284). Urinary mannitol concentration was significantly lower in patients than in controls (p = 0.022), suggesting a deficit of absorption from intestinal lumen. Such changes did not appear related to patients’ clinical–radiological features. Conclusion: The relatively high proportion of IP changes in RR-MS patients seems to confirm our work hypothesis and warrants more work to confirm the result on a larger sample, and to understand the implications for related immunological disturbances and intestinal microbiota alterations. Our finding may also have relevance for oral treatments, recently introduced in clinical practice. [ABSTRACT FROM AUTHOR]

Published

2017

8. IFN-β Therapy Regulates TLR7-Mediated Response in Plasmacytoid Dendritic Cells of Multiple Sclerosis Patients Influencing an Anti-Inflammatory Status.

Author

Severa, Martina, Rizzo, Fabiana, Giacomini, Elena, Annibali, Viviana, Gafa, Valerie, Romano, Silvia, Buscarinu, Maria Chiara, Fornasiero, Arianna, Salvetti, Marco, and Coccia, Eliana Marina

Subjects

MULTIPLE sclerosis, DENDRITIC cells, INTERFERONS, TOLL-like receptors, ANTI-inflammatory agents, IMMUNOREGULATION, BLOOD plasma, PHYSIOLOGY, IMMUNOLOGY

Abstract

Plasmacytoid dendritic cells (pDCs) display altered immune-phenotype in multiple sclerosis (MS) patients and are found actively recruited in postmortem MS brain lesions, implying that their immune regulation may represent an important aspect of MS pathogenesis. Because of the reported Toll-like receptor 7 (TLR7) implication in autoimmunity, in this study we characterized how IFN-β therapy impacts on pDC activation to TLR7 triggering in MS patients, aspect only poorly investigated so far. In vivo IFN-β administration regulates pDC functions in TLR7-treated peripheral blood mononuclear cell (PBMC) cultures differently from what is observed in isolated cells, suggesting that IFN-β may activate inhibitory mechanisms in MS peripheral blood involved in turning off pDC response to dampen the ongoing inflammation. Indeed, IL-10, a key regulatory cytokine found increased upon TLR7 stimulation in in vivo IFN-β-exposed PBMCs, directly reduced pDC-mediated IFN-α production. IFN-β therapy also shaped T-cell responses by decreasing TLR7-induced pDC maturation and inducing T-cell inhibitory molecules. Accordingly, raised pDC-induced IL-27 and decreased IL-23 expression, together with high IL-10 level, contribute to inhibit Th17 cell differentiation. Our study uncovered a role for IFN-β in the regulation of TLR7-mediated pDC responses in MS toward an anti-inflammatory phenotype opening new opportunities to better understand mechanisms of action of this drug in controlling MS immunopathogenesis. [ABSTRACT FROM AUTHOR]

Published

2015

9. Epstein-Barr virus genetic variants are associated with multiple sclerosis.

Author

Mechelli, Rosella, Manzari, Caterina, Policano, Claudia, Annese, Anita, Picardi, Ernesto, Umeton, Renato, Fornasiero, Arianna, D'Erchia, Anna Maria, Buscarinu, Maria Chiara, Agliardi, Cristina, Annibali, Viviana, Serafini, Barbara, Rosicarelli, Barbara, Romano, Silvia, Angelini, Daniela F, Ricigliano, Vito A G, Buttari, Fabio, Battistini, Luca, Centonze, Diego, and Guerini, Franca R

Published

2015

10. A “Candidate-Interactome” Aggregate Analysis of Genome-Wide Association Data in Multiple Sclerosis

Author

Mechelli, Rosella, Umeton, Renato, Policano, Claudia, Annibali, Viviana, Coarelli, Giulia, Ricigliano, Vito A. G., Vittori, Danila, Fornasiero, Arianna, Buscarinu, Maria Chiara, Romano, Silvia, Salvetti, Marco, and Ristori, Giovanni

Subjects

GENOMES, DATA analysis, CYTOMEGALOVIRUSES, IMMUNODEFICIENCY, VITAMIN D receptors, HYDROCARBONS

Abstract

Though difficult, the study of gene-environment interactions in multifactorial diseases is crucial for interpreting the relevance of non-heritable factors and prevents from overlooking genetic associations with small but measurable effects. We propose a “candidate interactome” (i.e. a group of genes whose products are known to physically interact with environmental factors that may be relevant for disease pathogenesis) analysis of genome-wide association data in multiple sclerosis. We looked for statistical enrichment of associations among interactomes that, at the current state of knowledge, may be representative of gene-environment interactions of potential, uncertain or unlikely relevance for multiple sclerosis pathogenesis: Epstein-Barr virus, human immunodeficiency virus, hepatitis B virus, hepatitis C virus, cytomegalovirus, HHV8-Kaposi sarcoma, H1N1-influenza, JC virus, human innate immunity interactome for type I interferon, autoimmune regulator, vitamin D receptor, aryl hydrocarbon receptor and a panel of proteins targeted by 70 innate immune-modulating viral open reading frames from 30 viral species. Interactomes were either obtained from the literature or were manually curated. The P values of all single nucleotide polymorphism mapping to a given interactome were obtained from the last genome-wide association study of the International Multiple Sclerosis Genetics Consortium & the Wellcome Trust Case Control Consortium, 2. The interaction between genotype and Epstein Barr virus emerges as relevant for multiple sclerosis etiology. However, in line with recent data on the coexistence of common and unique strategies used by viruses to perturb the human molecular system, also other viruses have a similar potential, though probably less relevant in epidemiological terms. [ABSTRACT FROM AUTHOR]

Published

2013

11. Autoimmune Encephalitis and CSF Anti-GluR3 Antibodies in an MS Patient after Alemtuzumab Treatment.

Author

Buscarinu, Maria Chiara, Fornasiero, Arianna, Pellicciari, Giulia, Reniè, Roberta, Landi, Anna Chiara, Bozzao, Alessandro, Cappelletti, Cristina, Bernasconi, Pia, Ristori, Giovanni, and Salvetti, Marco

Subjects

*ANTI-NMDA receptor encephalitis, *ALEMTUZUMAB, *IDIOPATHIC thrombocytopenic purpura, *ENCEPHALITIS, *CEREBROSPINAL fluid, *IMMUNOGLOBULINS

Abstract

A 45-year-old Italian woman, affected by relapsing–remitting multiple sclerosis (RR-MS) starting from 2011, started treatment with alemtuzumab in July 2016. Nine months after the second infusion, she had an immune thrombocytopenic purpura (ITP) with complete recovery after steroid treatment. Three months after the ITP, the patient presented with transient aphasia, cognitive deficits, and focal epilepsy. Serial brain magnetic resonance imaging showed a pattern compatible with encephalitis. Autoantibodies to glutamate receptor 3 peptide A and B were detected in cerebrospinal fluid and serum, in the absence of any other diagnostic cues. After three courses of intravenous immunoglobulin (0.4 mg/kg/day for 5 days, 1 month apart), followed by boosters (0.4 mg/kg/day) every 4–6 weeks, her neurological status improved and is currently comparable with that preceding the encephalitis. Autoimmune complications of the central nervous system during alemtuzumab therapy are relatively rare: only one previous case of autoimmune encephalitis following alemtuzumab treatment has been reported to date. [ABSTRACT FROM AUTHOR]

Published

2019