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1. Correction: Evaluation of molecular inversion probe versus TruSeq® custom methods for targeted next-generation sequencing.

Author

Rowida Almomani, Margherita Marchi, Maurice Sopacua, Patrick Lindsey, Erika Salvi, Bart de Koning, Silvia Santoro, Stefania Magri, Hubert J M Smeets, Filippo Martinelli Boneschi, Rayaz A Malik, Dan Ziegler, Janneke G J Hoeijmakers, Gidon Bönhof, Sulayman Dib-Hajj, Stephen G Waxman, Ingemar S J Merkies, Giuseppe Lauria, Catharina G Faber, Monique M Gerrits, and on behalf on the PROPANE Study Group

Subjects
Medicine, Science
Abstract

[This corrects the article DOI: 10.1371/journal.pone.0238467.].

Published
2021
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2. Evaluation of molecular inversion probe versus TruSeq® custom methods for targeted next-generation sequencing.

Author

Rowida Almomani, Margherita Marchi, Maurice Sopacua, Patrick Lindsey, Erika Salvi, Bart de Koning, Silvia Santoro, Stefania Magri, Hubert J M Smeets, Filippo Martinelli Boneschi, Rayaz R Malik, Dan Ziegler, Janneke G J Hoeijmakers, Gidon Bönhof, Sulayman Dib-Hajj, Stephen G Waxman, Ingemar S J Merkies, Giuseppe Lauria, Catharina G Faber, Monique M Gerrits, and on behalf on the PROPANE Study Group

Subjects
Medicine, Science
Abstract

Resolving the genetic architecture of painful neuropathy will lead to better disease management strategies. We aimed to develop a reliable method to re-sequence multiple genes in a large cohort of painful neuropathy patients at low cost. In this study, we compared sensitivity, specificity, targeting efficiency, performance and cost effectiveness of Molecular Inversion Probes-Next generation sequencing (MIPs-NGS) and TruSeq® Custom Amplicon-Next generation sequencing (TSCA-NGS). Capture probes were designed to target nine sodium channel genes (SCN3A, SCN8A-SCN11A, and SCN1B-SCN4B). One hundred sixty-six patients with diabetic and idiopathic neuropathy were tested by both methods, 70 patients were validated by Sanger sequencing. Sensitivity, specificity and performance of both techniques were comparable, and in agreement with Sanger sequencing. The average targeted regions coverage for MIPs-NGS was 97.3% versus 93.9% for TSCA-NGS. MIPs-NGS has a more versatile assay design and is more flexible than TSCA-NGS. The cost of MIPs-NGS is >5 times cheaper than TSCA-NGS when 500 or more samples are tested. In conclusion, MIPs-NGS is a reliable, flexible, and relatively inexpensive method to detect genetic variations in a large cohort of patients. In our centers, MIPs-NGS is currently implemented as a routine diagnostic tool for screening of sodium channel genes in painful neuropathy patients.

Published
2020
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3. Transcriptomic Analysis of Peripheral Monocytes upon Fingolimod Treatment in Relapsing Remitting Multiple Sclerosis Patients

Author

Melissa Sorosina, Ferdinando Clarelli, P. Provero, G. Comi, F. Martinelli Boneschi, Laura Ferrè, Federica Esposito, Massimo Filippi, Elisabetta Mascia, Linda Ottoboni, Giacomo Sferruzza, Silvia Santoro, Lucia Moiola, and Vittorio Martinelli

Subjects
Adult, Male, Sphingosine 1 Phosphate Receptor Modulators, 0301 basic medicine, CD14, Lipopolysaccharide Receptors, Neuroscience (miscellaneous), Transcriptome, 03 medical and health sciences, Cellular and Molecular Neuroscience, Multiple Sclerosis, Relapsing-Remitting, 0302 clinical medicine, Immune system, medicine, Humans, Interleukin-7 receptor, Wnt Signaling Pathway, Cells, Cultured, Fingolimod Hydrochloride, business.industry, Gene Expression Profiling, Monocyte, Multiple sclerosis, Wnt signaling pathway, medicine.disease, Fingolimod, Treatment Outcome, 030104 developmental biology, medicine.anatomical_structure, Neurology, Immunology, Leukocytes, Mononuclear, Female, business, 030217 neurology & neurosurgery, Follow-Up Studies, medicine.drug
Abstract

Fingolimod (FTY), a second-line oral drug approved for relapsing remitting Multiple Sclerosis (RRMS) acts in preventing lymphocyte migration outside lymph nodes; moreover, several lines of evidence suggest that it also inhibits myeloid cell activation. In this study, we investigated the transcriptional changes induced by FTY in monocytes in order to better elucidate its mechanism of action. CD14+ monocytes were collected from 24 RRMS patients sampled at baseline and after 6 months of treatment and RNA profiles were obtained through next-generation sequencing. We conducted pathway and sub-paths analysis, followed by centrality analysis of cell-specific interactomes on differentially expressed genes (DEGs). We investigated also the predictive role of baseline monocyte transcription profile in influencing the response to FTY therapy. We observed a marked down-regulation effect (60 down-regulated vs. 0 up-regulated genes). Most of the down-regulated DEGs resulted related with monocyte activation and migration like IL7R, CCR7 and the Wnt signaling mediators LEF1 and TCF7. The involvement of Wnt signaling was also confirmed by subpaths analyses. Furthermore, pathway and network analyses showed an involvement of processes related to immune function and cell migration. Baseline transcriptional profile of the HLA class II gene HLA-DQA1 and HLA-DPA1 were associated with evidence of disease activity after 2 years of treatment. Our data support the evidence that FTY induces major transcriptional changes in monocytes, mainly regarding genes involved in cell trafficking and immune cell activation. The baseline transcriptional levels of genes associated with antigen presenting function were associated with disease activity after 2 years of FTY treatment.

Published
2021

4. Assessment of the genetic contribution to brain magnetic resonance imaging lesion load and atrophy measures in multiple sclerosis patients

Author

Laura Ferrè, Maria A. Rocca, Federica Esposito, Ermelinda De Meo, Melissa Sorosina, Filippo Martinelli Boneschi, Silvia Santoro, Massimo Filippi, Ferdinando Clarelli, Clarelli, Ferdinando, Rocca, Maria Assunta, Santoro, Silvia, De Meo, Ermelinda, Ferrè, Laura, Sorosina, Melissa, Martinelli Boneschi, Filippo, Esposito, Federica, and Filippi, Massimo

Subjects
Oncology, medicine.medical_specialty, Multiple Sclerosis, Single-nucleotide polymorphism, Grey matter, Multiple sclerosis, Lesion, White matter, 03 medical and health sciences, Multiple Sclerosis, Relapsing-Remitting, 0302 clinical medicine, Atrophy, Neuroimaging, Internal medicine, medicine, Humans, Magnetic resonance imaging (MRI), 030212 general & internal medicine, Gray Matter, Genetic association study, medicine.diagnostic_test, business.industry, Brain, Magnetic resonance imaging, medicine.disease, Magnetic Resonance Imaging, medicine.anatomical_structure, Neurology, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery
Abstract

BACKGROUND AND PURPOSE Multiple sclerosis (MS) susceptibility is influenced by genetics; however, little is known about genetic determinants of disease expression. We aimed at assessing genetic factors influencing quantitative neuroimaging measures in two cohorts of progressive MS (PMS) and relapsing-remitting MS (RRMS) patients. METHODS Ninety-nine PMS and 214 RRMS patients underwent a 3-T brain magnetic resonance imaging (MRI) scan, with the measurement of five MRI metrics including T2 lesion volumes and measures of white matter, grey matter, deep grey matter, and hippocampal volumes. A candidate pathway strategy was adopted; gene set analysis was carried out to estimate cumulative contribution of genes to MRI phenotypes, adjusting for relevant confounders, followed by single nucleotide polymorphism (SNP) regression analysis. RESULTS Seventeen Kyoto Encyclopedia of Genes and Genomes pathways and 42 Gene Ontology (GO) terms were tested. We additionally included in the analysis genes with enriched expression in brain cells. Gene set analysis revealed a differential pattern of association across the two cohorts, with processes related to sodium homeostasis being associated with grey matter volume in PMS (p = 0.002), whereas inflammatory-related GO terms such as adaptive immune response and regulation of inflammatory response appeared to be associated with T2 lesion volume in RRMS (p = 0.004 and p = 0.008, respectively). As for SNPs, the rs7104613T mapping to SPON1 gene was associated with reduced deep grey matter volume (β = -0.731, p = 3.2*10-7 ) in PMS, whereas we found evidence of association between white matter volume and rs740948A mapping to SEMA3A gene (β = 22.04, p = 5.5*10-6 ) in RRMS. CONCLUSIONS Our data suggest a different pattern of associations between MRI metrics and functional processes across MS disease courses, suggesting different phenomena implicated in MS.

Published
2021

5. Identification of differential DNA methylation associated with multiple sclerosis: A family-based study

Author

Ferdinando Clarelli, S. Bonfiglio, Massimo Filippi, Federica Esposito, A. Protti, Giulia Barbiera, Filippo Martinelli-Boneschi, Vittorio Martinelli, E. Stupka, Silvia Santoro, Elisabetta Mascia, Clara Guaschino, Francesca Giannese, Melissa Sorosina, Dejan Lazarevic, Jose Manuel Garcia-Manteiga, Davide Cittaro, Garcia-Manteiga, J. M., Clarelli, F., Bonfiglio, S., Mascia, E., Giannese, F., Barbiera, G., Guaschino, C., Sorosina, M., Santoro, S., Protti, A., Martinelli, V., Cittaro, D., Lazarevic, D., Stupka, E., Filippi, M., Esposito, F., and Martinelli-Boneschi, F.

Subjects
0301 basic medicine, Adult, Male, Multiple Sclerosis, Immunology, Genomics, Biology, Epigenesis, Genetic, 03 medical and health sciences, Young Adult, 0302 clinical medicine, medicine, Immunology and Allergy, Humans, Multiplex, Epigenetics, Gene, Aged, Genetics, Multiple sclerosis, Methylation, DNA Methylation, Middle Aged, medicine.disease, Pedigree, 030104 developmental biology, Differentially methylated regions, Neurology, Italy, DNA methylation, Female, Neurology (clinical), 030217 neurology & neurosurgery, Genome-Wide Association Study
Abstract

Multiple Sclerosis (MS) is caused by a still unknown interplay between genetic and environmental factors. Epigenetics, including DNA methylation, represents a model for environmental factors to influence MS risk. Twenty-six affected and 26 unaffected relatives from 8 MS multiplex families were analysed in a multicentric Italian study using MeDIP-Seq, followed by technical validation and biological replication in two additional families of differentially methylated regions (DMRs) using SeqCap Epi Choice Enrichment kit (Roche®). Associations from MeDIP-Seq across families were combined with aggregation statistics, yielding 162 DMRs at FDR ≤ 0.1. Technical validation and biological replication led to 2 hypo-methylated regions, which point to NTM and BAI3 genes, and to 2 hyper-methylated regions in PIK3R1 and CAPN13. These 4 novel regions contain genes of potential interest that need to be tested in larger cohorts of patients.

Published
2021

6. Evaluation of molecular inversion probe versus TruSeq® custom methods for targeted next-generation sequencing

Author

Stefania Magri, Sulayman D. Dib-Hajj, Ingemar S. J. Merkies, Filippo Martinelli Boneschi, Rayaz A. Malik, Silvia Santoro, Bart de Koning, Janneke G. J. Hoeijmakers, Gidon J. Bönhof, Margherita Marchi, Giuseppe Lauria, Hubert J.M. Smeets, Rowida Almomani, Erika Salvi, Dan Ziegler, Patrick J. Lindsey, Stephen G. Waxman, Catharina G. Faber, Monique M. Gerrits, Maurice Sopacua, Klinische Neurowetenschappen, RS: MHeNs - R3 - Neuroscience, RS: GROW - R4 - Reproductive and Perinatal Medicine, Klinische Genetica, MUMC+: DA KG Lab Centraal Lab (9), RS: FHML MaCSBio, MUMC+: MA Med Staf Spec Neurologie (9), and RS: MHeNs - R1 - Cognitive Neuropsychiatry and Clinical Neuroscience

Subjects
0301 basic medicine, Cost effectiveness, Molecular biology, Oligonucleotides, Artificial Gene Amplification and Extension, Molecular Inversion Probe, Biochemistry, Polymerase Chain Reaction, 0302 clinical medicine, Sequencing techniques, Medicine and Health Sciences, Medicine, DNA sequencing, Paired-end tag, ASSOCIATIONS, Sanger sequencing, Multidisciplinary, medicine.diagnostic_test, Nucleotides, High-Throughput Nucleotide Sequencing, Genomics, Gene Pool, 3. Good health, 030220 oncology & carcinogenesis, symbols, DNA Probes, Molecular probe, Transcriptome Analysis, Research Article, Next-Generation Sequencing, GENES, DISORDERS, Science, Pain, Computational biology, Research and Analysis Methods, Sensitivity and Specificity, 03 medical and health sciences, symbols.namesake, Idiopathic Neuropathy, Signs and Symptoms, Genetics, Humans, Genetic Testing, Molecular Biology Techniques, Genetic testing, Neuropathic Pain, Evolutionary Biology, Biology and life sciences, Population Biology, business.industry, Dideoxy DNA sequencing, Correction, Computational Biology, Human Genetics, Sequence Analysis, DNA, Genome Analysis, 030104 developmental biology, Molecular Probes, Chromosome Inversion, Mutation, Genetics of Disease, Neuralgia, Clinical Medicine, business, Population Genetics
Abstract

Resolving the genetic architecture of painful neuropathy will lead to better disease management strategies. We aimed to develop a reliable method to re-sequence multiple genes in a large cohort of painful neuropathy patients at low cost. In this study, we compared sensitivity, specificity, targeting efficiency, performance and cost effectiveness of Molecular Inversion Probes-Next generation sequencing (MIPs-NGS) and TruSeq® Custom Amplicon-Next generation sequencing (TSCA-NGS). Capture probes were designed to target nine sodium channel genes (SCN3A, SCN8A-SCN11A, and SCN1B-SCN4B). One hundred sixty-six patients with diabetic and idiopathic neuropathy were tested by both methods, 70 patients were validated by Sanger sequencing. Sensitivity, specificity and performance of both techniques were comparable, and in agreement with Sanger sequencing. The average targeted regions coverage for MIPs-NGS was 97.3% versus 93.9% for TSCA-NGS. MIPs-NGS has a more versatile assay design and is more flexible than TSCA-NGS. The cost of MIPs-NGS is >5 times cheaper than TSCA-NGS when 500 or more samples are tested. In conclusion, MIPs-NGS is a reliable, flexible, and relatively inexpensive method to detect genetic variations in a large cohort of patients. In our centers, MIPs-NGS is currently implemented as a routine diagnostic tool for screening of sodium channel genes in painful neuropathy patients.

Published
2020

7. Laser capture microdissection for transcriptomic profiles in human skin biopsies

Author

Filippo Martinelli Boneschi, Raffaella Lombardi, Margherita Marchi, Silvia Peroni, Giancarlo Comi, Ignazio Diego Lopez, Ferdinando Clarelli, Silvia Santoro, Andrea Zauli, Ana Maria Osiceanu, Daniele Cazzato, Angelo Quattrini, Melissa Sorosina, Raffaele A. Calogero, and Giuseppe Lauria

Subjects
0301 basic medicine, Male, lcsh:QH426-470, RNase P, Biopsy, Human skin, Computational biology, Biology, Transcriptome, 03 medical and health sciences, Idiopathic neuropathy, medicine, Skin biopsy, Humans, lcsh:QH573-671, Transcriptomics, Molecular Biology, Laser capture microdissection, Aged, Skin, medicine.diagnostic_test, Sequence Analysis, RNA, lcsh:Cytology, Methodology Article, Gene Expression Profiling, RNA, High-Throughput Nucleotide Sequencing, RNA sequencing, Middle Aged, Gene expression profiling, lcsh:Genetics, 030104 developmental biology, MRNA Sequencing, Female
Abstract

Background The acquisition of reliable tissue-specific RNA sequencing data from human skin biopsy represents a major advance in research. However, the complexity of the process of isolation of specific layers from fresh-frozen human specimen by laser capture microdissection, the abundant presence of skin nucleases and RNA instability remain relevant methodological challenges. We developed and optimized a protocol to extract RNA from layers of human skin biopsies and to provide satisfactory quality and amount of mRNA sequencing data. Results The protocol includes steps of collection, embedding, freezing, histological coloration and relative optimization to preserve RNA extracted from specific components of fresh-frozen human skin biopsy of 14 subjects. Optimization of the protocol includes a preservation step in RNALater® Solution, the control of specimen temperature, the use of RNase Inhibitors and the time reduction of the staining procedure. The quality of extracted RNA was measured using the percentage of fragments longer than 200 nucleotides (DV200), a more suitable measurement for successful library preparation than the RNA Integrity Number (RIN). RNA was then enriched using the TruSeq® RNA Access Library Prep Kit (Illumina®) and sequenced on HiSeq® 2500 platform (Illumina®). Quality control on RNA sequencing data was adequate to get reliable data for downstream analysis. Conclusions The described implemented and optimized protocol can be used for generating transcriptomics data on skin tissues, and it is potentially applicable to other tissues. It can be extended to multicenter studies, due to the introduction of an initial step of preservation of the specimen that allowed the shipment of biological samples. Electronic supplementary material The online version of this article (10.1186/s12867-018-0108-5) contains supplementary material, which is available to authorized users.

Published
2018

8. A gene-set analysis suggests the possible involvement of iron homeostasis in neurodegeneration in progressive multiple sclerosis

Author

Laura Ferrè, Miryam Cannizzaro, Federica Esposito, Silvia Santoro, Melissa Sorosina, Massimo Filippi, Elisabetta Mascia, Antonino Giordano, and Ferdinando Clarelli

Subjects
Progressive multiple sclerosis, Neurology, Iron homeostasis, Neurodegeneration, medicine, Neurology (clinical), Biology, medicine.disease, Set (psychology), Gene, Neuroscience
Published
2021

11. Use of contrast-enhanced ultrasound for assessment of nodular lymphoid hyperplasia (NLH) in canine spleen

Author

Francesco Macrì, Nicola Maria Iannelli, Massimo De Majo, Cyndi Mangano, Giuseppe Mazzullo, Michela Pugliese, Simona Di Pietro, Rosalia Crupi, and Silvia Santoro

Subjects
Male, Pathology, medicine.medical_specialty, 040301 veterinary sciences, Nodular lymphoid hyperplasia, Sulfur Hexafluoride, Spleen, Qontrast, 0403 veterinary science, 03 medical and health sciences, Dogs, Cytology, Dog, medicine, Animals, Contrast-enhanced ultrasonography, Dog Diseases, Prospective Studies, Lymphatic Diseases, Phospholipids, Splenic Diseases, Ultrasonography, 030304 developmental biology, Dog, contrast-enhanced ultrasonography, diagnostic ultrasound, nodular lymphoid hyperplasia, spleen, sonovue, qontrast, 0303 health sciences, Hyperplasia, lcsh:Veterinary medicine, Sonovue, General Veterinary, business.industry, Histology, 04 agricultural and veterinary sciences, General Medicine, Contrast medium, medicine.anatomical_structure, lcsh:SF600-1100, Female, Diagnostic ultrasound, business, Perfusion, Mechanical index, Research Article, Contrast-enhanced ultrasound
Abstract

Background Nodular lymphoid hyperplasia (NLH) is one of the most common non-neoplastic splenic lesions in dogs, especially in old ones, showing a splenic enlargement. More recent studies have been focused on Contrast Enhanced Ultrasonography (CEUS) analysis of the spleen for establishing normal perfusion patterns and blood pool phase peculiarities of focal lesions. The aim of the study was to evaluate the qualitative and quantitative CEUS analysis of the canine splenic NLH, characterizing the CEUS pattern of this pathology on 20 clinical cases. Results A prospective, observational study was performed using a system equipped with contrast-tuned imaging technology. Mechanical Index was set from 0.08 to 0.11; the contrast medium was a second generation contrast medium composed of sulphur hexafluoride encapsulated of a shell of phospholipids (SonoVue®). Qualitative and quantitative assessment of the enhancement pattern of splenic NLH were performed. Cytology and histology identified 20 splenic NLH. All of the benign hyperplastic lesions assessed were isoechoic with a homogeneous pattern than the surrounding normal spleen, during the wash-in phase (10–20 s) of the CEUS exam. Before finishing the wash-in phase, 20–45 s from the contrast medium inoculation, 19/20 benign nodules became markedly hypoechoic to the adjacent spleen. Sensitivity of hypoechoic pattern for NLH was 95%. Conclusions These findings should prove useful in the evaluation of focal splenic masses in dogs. Since enhancement and perfusion patterns of NLH seem to coincide with some neoplastic lesions of the spleen previously reported, in clinical practice attention must be paid to the final diagnosis of canine splenic lesions using only the CEUS exam.

Published
2019

12. COL6A5 variants in familial neuropathic chronic itch

Author

Daniele Cazzato, Stephen G. Waxman, Raffaella Lombardi, Paola Grammatico, Nicoletta Zoppi, Margherita Marchi, Sulayman D. Dib-Hajj, Roberto Eleopra, Jenny Sassone, Hassan Fadavi, Marco Ritelli, Claudio Doglioni, Catharina G. Faber, Monique M. Gerrits, Daniela Toniolo, Grazia Devigili, Ingemar S. J. Merkies, Silvia Santoro, Marina Colombi, Chiara Dordoni, Massimiliano Cocca, Marco Castori, Michela Taiana, Giuseppe Lauria, Filippo Martinelli-Boneschi, Andrea Zauli, Rowida Almomani, Rayaz A. Malik, Melissa Sorosina, Martinelli Boneschi, Filippo, Colombi, Marina, Castori, Marco, Devigili, Grazia, Eleopra, Roberto, Malik, Rayaz A, Ritelli, Marco, Zoppi, Nicoletta, Dordoni, Chiara, Sorosina, Melissa, Grammatico, Paola, Fadavi, Hassan, Gerrits, Monique M, Almomani, Rowida, Faber, Catharina G, Merkies, Ingemar S. J, Toniolo, Daniela, Cocca, Massimiliano, Doglioni, Claudio, Waxman, Stephen G, Dib Hajj, Sulayman D, Taiana, Michela M, Sassone, Jenny, Lombardi, Raffaella, Cazzato, Daniele, Zauli, Andrea, Santoro, Silvia, Marchi, Margherita, Lauria, Giuseppe, MUMC+: DA KG Lab Centraal Lab (9), MUMC+: MA Med Staf Spec Neurologie (9), RS: MHeNs - R1 - Cognitive Neuropsychiatry and Clinical Neuroscience, Klinische Neurowetenschappen, Filippo, Martinelli Boneschi, Marina, Colombi, Marco, Castori, Grazia, Devigili, Roberto, Eleopra, Rayaz, Malik, Marco, Ritelli, Nicoletta, Zoppi, Chiara, Dordoni, Melissa, Sorosina, Paola, Grammatico, Hassan, Fadavi, Monique, M. Gerrit, Rowida, Almomani, Catharina, G. Faber, Ingemar, S. J. Merkie, Daniela, Toniolo, Massimiliano, Cocca, Stephen, G. Waxman, Sulayman, D. Dib Hajj, Michela, M. Taiana, SASSONE PAGANO, Jenny, Raffaella, Lombardi, Daniele, Cazzato, Andrea, Zauli, Silvia, Santoro, Margherita, Marchi, and Giuseppe, Lauria

Subjects
0301 basic medicine, Male, Pathology, Diabetic neuropathy, SYMPTOMS, NOCICEPTORS, DNA Mutational Analysis, 0302 clinical medicine, Missense mutation, ATOPIC-DERMATITIS, CHAINS, itch, Exome sequencing, Skin, medicine.diagnostic_test, small fibre neuropathy, Medicine (all), COL6A5, neuropathic pain, PAIN, Peripheral Nervous System Diseases, SODIUM-CHANNELS, Middle Aged, Itch, Neuropathic pain, Small fibre neuropathy, Arts and Humanities (miscellaneous), Neurology (clinical), GABAPENTIN, Female, Haploinsufficiency, medicine.drug, Joint hypermobility, Adult, medicine.medical_specialty, Gabapentin, Collagen Type VI, 03 medical and health sciences, CHRONIC PRURITUS, medicine, Humans, Family Health, business.industry, Pruritus, Genetic Variation, SMALL FIBER NEUROPATHY, medicine.disease, 030104 developmental biology, Immunology, Skin biopsy, SENSORY NEURONS, business, 030217 neurology & neurosurgery
Abstract

Itch is thought to represent the peculiar response to stimuli conveyed by somatosensory pathways shared with pain through the activation of specific neurons and receptors. It can occur in association with dermatological, systemic and neurological diseases, or be the side effect of certain drugs. However, some patients suffer from chronic idiopathic itch that is frequently ascribed to psychological distress and for which no biomarker is available to date. We investigated three multigenerational families, one of which diagnosed with joint hypermobility syndrome/Ehlers-Danlos syndrome hypermobility type (JHS/EDS-HT), characterized by idiopathic chronic itch with predominantly proximal distribution. Skin biopsy was performed in all eight affected members and revealed in six of them reduced intraepidermal nerve fibre density consistent with small fibre neuropathy. Whole exome sequencing identified two COL6A5 rare variants co-segregating with chronic itch in eight affected members and absent in non-affected members, and in one unrelated sporadic patient with type 1 painless diabetic neuropathy and chronic itch. Two families and the diabetic patient carried the nonsense c.6814G>T (p.Glu2272*) variant and another family carried the missense c.6486G>C (p.Arg2162Ser) variant. Both variants were predicted as likely pathogenic by in silico analyses. The two variants were rare (minor allele frequency < 0.1%) in 6271 healthy controls and absent in 77 small fibre neuropathy and 167 JHS/EDS-HT patients without itch. Null-allele test on cDNA from patients' fibroblasts of both families carrying the nonsense variant demonstrated functional haploinsufficiency due to activation of nonsense mediated RNA decay. Immunofluorescence microscopy and western blotting revealed marked disorganization and reduced COL6A5 synthesis, respectively. Indirect immunofluorescence showed reduced COL6A5 expression in the skin of patients carrying the nonsense variant. Treatment with gabapentinoids provided satisfactory itch relief in the patients carrying the mutations. Our findings first revealed an association between COL6A5 gene and familiar chronic itch, suggesting a new contributor to the pathogenesis of neuropathic itch and identifying a new candidate therapeutic target.

Published
2017

13. The Multiple Sclerosis Genomic Map: Role of peripheral immune cells and resident microglia in susceptibility

Author

Ashley Beecham, David A. Hafler, Colombe J, Ublick K, Stephen Sawcer, Marcus C. S. Lee, Adam Santaniello, An Goris, Frank Seibold, Xavier Montalban, G. Comi, Christiane Gasperi, Sandra D'Alfonso, Federica Esposito, Laurent Peyrin-Biroulet, Frauke Zipp, Ioanna Konidari, Elisabeth Gulowsen Celius, Achim Berthele, Amoroso A, Rogier Q. Hintzen, Johan Van Limbergen, Marieme Dembele, Fredrik Karpe, Zhang W, Robbins A, Moiola L, Annette Bang Oturai, Cristin McCabe, Filippo Martinelli-Boneschi, M Lindén, Keith R Edwards, Hanne F. Harbo, Zuccalà M, Marc Lémann, Felix Luessi, Noriko Isobe, Nadia Barizzone, Renata D'Incà, Croft A, Ioannis S. Vlachos, Frohlich I, Martinelli, Daniela Galimberti, Efthimios Dardiotis, Lisa F. Barcellos, Brendan T. Keenan, Maja Jagodic, Ferdinando Clarelli, Bénédicte Dubois, Nicholas A. Kennedy, Lohith Madireddy, Grant W. Montgomery, Tommy Olsson, Phil De Jager, Lo A, Peter A. Calabresi, Brandes A, Chris Cotsapas, Bakker Pd, Steffan D. Bos, Christina M. Lill, Karban A, Thoerner Lw, Tojo James, Wong G, Harald Peeters, M.-M. Hoshi, Roberts R, Fredrik Piehl, Lars Alfredsson, Giorgos M. Hadjigeorgiou, Bertrand Fontaine, Melissa Sorosina, Benedetti M, Maria Ban, Jorge R. Oksenberg, Howard L. Weiner, Ingrid Kockum, Mireia Sospedra, Taylor Km, Henrik Ullum, Izaura Lima Bomfim, Stronati L, Molyneux P, Replogle J, Stacy J. Caillier, Zhang H, Till F. M. Andlauer, Margaret A. Pericak-Vance, Jan Hillert, Luisa Bernardinelli, Taibo Li, Helle Bach Søndergaard, Ilijas Jelcic, Nikolaos A. Patsopoulos, Silvia Delgado, Cathy Schaefer, Thomas Korn, Laura Piccio, Mark Mühlau, Deborah D. Proctor, B. Hemmer, Elizabeth M. Bradshaw, Hysi P, Megan C Neville, Mary F. Davis, Dorlan J. Kimbrough, Jyoti Khadake, Jean-Pierre Hugot, David Gomez-Cabrero, Murray L. Barclay, Anne H. Cross, Kasper Lage, Stephen L. Hauser, A Compston, Zimmer A, Ivinson A, Anne Spurkland, Jonas Halfvarson, Charles C. White, Biberacher, Zarzycki O, Kathryn C. Fitzgerald, Finn Sellebjerg, Ellis Patrick, Andrea Zauli, Bruce V. Taylor, Maurizio Leone, Genevieve Lachance, Marta Olah, B. Cree, Manuel Comabella, Arie Levine, Domizia Vecchio, Mathias Chamaillard, Mark Lathrop, Clara Guaschino, Roland Martin, Hanigan K, Pierre-Antoine F. D. Gourraud, Maria Cimpean, Jonathan L. Haines, Dorothea Buck, Marco Salvetti, Per Soelberg Sørensen, Noel Lg, Mitja Mitrovic, Graeme J. Stewart, Benjamin Knier, Ellen Lathi, Cottone M, Laura Ferrè, Winn P, Duijn Cv, Monica Milla, Tune H. Pers, I. Oikonomou, An D, David R. Booth, Rebeix Ic, Clara P. Manrique, Massey D, Evelyn Ng Sm, Törkvist L, Daniele Cusi, Shoostari P, Vatn Mh, Paola Cavalla, Silvia Santoro, Gossum Av, Seema Kalra, Paul Rutgeerts, Clive Hawkins, Sandra Vukusik, Khan Ma, Hakon Hakonarson, Paul Henderson, Christiane Graetz, Julia Y Mescheriakova, Jean-François Rahier, Panteliadis I, Cristina Agliardi, Grummel, Jacob L. McCauley, Amie Baker, Janna Saarela, Sergio E. Baranzini, J W Thorpe, and Damotte

Subjects
0303 health sciences, Microglia, Multiple sclerosis, Central nervous system, Biology, medicine.disease, Major histocompatibility complex, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine.anatomical_structure, Autoimmune Process, Immunology, medicine, biology.protein, Gene, 030217 neurology & neurosurgery, X chromosome, 030304 developmental biology
Abstract

We assembled and analyzed genetic data of 47,351 multiple sclerosis (MS) subjects and 68,284 control subjects and establish a reference map of the genetic architecture of MS that includes 200 autosomal susceptibility variants outside the major histocompatibility complex (MHC), one chromosome X variant, and 32 independent associations within the extended MHC. We used an ensemble of methods to prioritize up to 551 potentially associated MS susceptibility genes, that implicate multiple innate and adaptive pathways distributed across the cellular components of the immune system. Using expression profiles from purified human microglia, we do find enrichment for MS genes in these brain - resident immune cells. Thus, while MS is most likely initially triggered by perturbation of peripheral immune responses the functional responses of microglia and other brain cells are also altered and may have a role in targeting an autoimmune process to the central nervous system.One Sentence Summary:We report a detailed genetic and genomic map of multiple sclerosis, and describe the role of putatively affected genes in the peripheral immune system and brain resident microglia.

Published
2017

14. Pharmacogenetic study of long-term response to interferon-β treatment in multiple sclerosis

Author

Federica Esposito, Giuseppe Liberatore, Bruno Colombo, Ana Maria Osiceanu, Elisabetta Mascia, Melissa Sorosina, Giulia Pavan, Silvia Santoro, Ferdinando Clarelli, F. Martinelli-Boneschi, Lucia Moiola, Giancarlo Comi, Vittorio Martinelli, Clarelli, F., Liberatore, G., Sorosina, M., Osiceanu, A. M., Esposito, F., Mascia, E., Santoro, S., Pavan, G., Colombo, B., Moiola, L., Martinelli, V., Comi, Giancarlo, and Martinelli boneschi, F.

Subjects
0301 basic medicine, Male, Time Factors, Pharmacogenomic Variants, Genome-wide association study, Bioinformatics, Receptors, Metabotropic Glutamate, Pharmacogenetic Study, 0302 clinical medicine, Immunologic Factor, Receptors, Kainic Acid, Multiple Sclerosi, Pharmacogenetic, Middle Aged, Phenotype, Treatment Outcome, Italy, Pharmacogenomic Variant, Molecular Medicine, Female, Case-Control Studie, Human, Adult, Multiple Sclerosis, Time Factor, Adolescent, Genotype, Cell Adhesion Molecules, Neuronal, Quantitative Trait Loci, Quantitative trait locus, Biology, Peripheral blood mononuclear cell, Polymorphism, Single Nucleotide, 03 medical and health sciences, Young Adult, Genetic, Genetics, medicine, Humans, Immunologic Factors, Allele, Pharmacology, Multiple sclerosis, Gene Expression Profiling, Interferon-beta, medicine.disease, Pharmacogenomic Testing, Gene expression profiling, 030104 developmental biology, Pharmacogenetics, Case-Control Studies, Immunology, 030217 neurology & neurosurgery, Genome-Wide Association Study
Abstract

The aim of the study is the identification of genetic factors that influence the long-term response to interferon-β (IFNβ) (4-year follow-up). We performed a genome-wide association study in 337 IFNβ-treated Italian multiple sclerosis patients at the extreme of treatment response, and we meta-analyzed association effects, integrating results with pathway analysis, gene-expression profiling of IFNβ-stimulated peripheral blood mononuclear cells from 20 healthy controls (HC) and expression quantitative locus (eQTL) analyses. From meta-analysis, 43 markers were associated at P

Published
2015

15. Reliability and usefulness of random fecal alpha 1-antitrypsin concentration: further simplification of the method

Author

Francesco Musso, Sergio Conti Nibali, Giuseppe Jacono, Giuseppe Di Pasquale, Giuseppe Magazzù, Concetta Sferlazzas, V. Balsamo, A. Tedeschi, and Silvia Santoro

Subjects
medicine.medical_specialty, Time Factors, Adolescent, Protein-Losing Enteropathies, Gastroenterology, Intestinal malabsorption, Feces, Animal science, Internal medicine, Medicine, Humans, Child, Reliability (statistics), business.industry, Feces analysis, Infant, Milk intolerance, Celiac Disease, α1 antitrypsin, Close relationship, Evaluation Studies as Topic, Concomitant, Child, Preschool, alpha 1-Antitrypsin, Pediatrics, Perinatology and Child Health, business
Abstract

The reliability of random fecal alpha 1-antitrypsin (FA-1-AT) concentration has been evaluated by comparing FA-1-AT values on random specimens and on concomitant 24-72 h fecal collections. In order to simplify the method, FA-1-AT data derived from lyophilized fecal samples were compared with those obtained from 37 degrees C heat-dried fecal samples. Random FA-1-AT concentration was assayed in 80 children with various gastrointestinal illnesses and 36 healthy age-matched controls. There was a close relationship between FA-1-AT values obtained from random samples and 1-day or 3-day collections. There was also a significant relationship between FA-1-AT values derived from the two different ways of drying the stools. Mean FA-1-AT values were statistically different when compared to the controls in the following groups of disorders: untreated and after-gluten-challenge celiac disease, post-enteritis syndrome, and cow's milk intolerance. The possible meanings of the abnormal FA-1-AT concentration in the various disorders are discussed. We conclude that FA-1-AT is a simple and reliable test for enteric protein loss. The simplification of the method proposed by us should reduce the cost of the test and moreover make it feasible in all laboratories.

Published
1985

16. Impact of multiple sclerosis risk loci in postinfectious neurological syndromes

Author

Ferdinando Clarelli, Silvia Peroni, Laura Ferrè, Silvia Santoro, Andrea Cortese, Giancarlo Comi, Angelo Gugliemi, Filippo Martinelli-Boneschi, Riccardo Currò, Elisabetta Mascia, Giulia Berzero, Enrico Marchioni, Massimo Filippi, Federica Esposito, Elisa Vegezzi, Ilaria Callegari, Melissa Sorosina, Martinelli-Boneschi, F., Curro, R., Santoro, S., Berzero, G., Sorosina, M., Ferre, L., Mascia, E., Peroni, S., Comi, G., Gugliemi, A., Vegezzi, E., Callegari, I., Filippi, M., Cortese, A., Esposito, F., Clarelli, F., and Marchioni, E.

Subjects
Adult, Male, medicine.medical_specialty, Multiple Sclerosis, Genotype, Myelitis, Single-nucleotide polymorphism, Disease, Postinfectious neurological syndrome, Multiple sclerosis, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Genetics, Humans, 030212 general & internal medicine, Genetic variability, Alleles, Acquired demyelinating disease, business.industry, Retrospective cohort study, General Medicine, Syndrome, Middle Aged, medicine.disease, Magnetic Resonance Imaging, 3. Good health, Neurology, Female, Neurology (clinical), Differential diagnosis, business, 030217 neurology & neurosurgery, Cohort study, Weighted genetic risk score
Abstract

Background: The genetic component of multiple sclerosis (MS) is now set to 200 autosomal common variants. However, it is unclear how genetic knowledge be clinically used in the differential diagnosis between MS and other inflammatory conditions like adult-onset postinfectious neurological syndromes (PINS). The aim of this study was to investigate whether PINS and MS have a shared genetic background using an updated polygenic risk scores. Methods: Eighty-eight PINS patients have been consecutively recruited between 1996 and 2016 at Mondino Foundation of Pavia, diagnosed according to clinical, MRI and CSF findings and followed-up for several years. Patients were typed using Illumina array, and genotypes imputed using the 1000 Genomes Project reference panel. A weighted genetic risk score (wGRS) has been calculated based on autosomal MS risk loci derived from large-scale studies, and an HLA genetic burden (HLAGB) was also calculated on loci associated to MS. Results: PINS occurred as an episode of myelitis in 44% of patients, encephalomyelitis in 44%, and encephalitis in remaining cases, with an involvement of peripheral nervous system in 41% of patients. Mean age of onset was 50.1 years, and female:male ratio was 1.4. Patients were followed-up for a mean of 7.2 years, and at last visit 55% had a low disability grade (mRS 0–1). Disease was monophasic in 67% of patients, relapsing in 18% and chronic-progressive in 15%. The wGRS of PINS cases was comparable to 370 healthy controls, while significantly lower compared to 907 bout-onset MS (BOMS) cases (wGRS= 20.9 vs 21.2; p

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