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104. Activated macrophages release microvesicles containing polarized M1 or M2 mRNAs

Author

Garzetti, Livia, Menon, Ramesh, Finardi, Annamaria, Bergami, Alessandra, Sica, Antonio, Martino, Gianvito, Comi, Giancarlo, Verderio, Claudia, Farina, Cinthia, and Furlan, Roberto

Abstract

Microvesicles released by activated macrophages, and detected in biological fluids, may constitute a valuable biomarker to identify myeloid cell activation phenotype during disease. MVs are known vehicles of horizontal communication among cells, currently under scrutiny as powerful biomarkers in several pathological processes. The potential advantage of MVs relies on the assumption that their content reflects processes ongoing in pathologically relevant cell types. We have described that MVs of myeloid origin in the CSF are a marker of microglia/macrophage activation. Myeloid cells have different activation types, resulting in diverse functional phenotypes. Knowledge on the activation type of myeloid cells during disease would be of paramount importance for the understanding of ongoing pathogenic processes. We show here that macrophages activated in vitro in different ways all release increased amounts of MVs compared with NS cells. Moreover, we show that macrophage‐derived MVs contain a repertoire of mRNAs that is not the result of casual sampling from the parental cells, as it is characterized by distinct mRNA enrichments and species. Nevertheless, mRNA content of MVs clearly allows identification in vivo of the activated phenotype of the cell of origin, indicating carryover of functional macrophage traits. We propose that detection of mRNAs in myeloid MVs permits identification of myeloid cell activation type during disease, allowing for further stratification of pathological processes.

Published
2014
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105. Base induced rearrangement reactions of N-phosphinoyl-O-sulfonylhydroxylamines. Observation of a phosphonamidic–sulfonic anhydride intermediate by NMR spectroscopy 1

Author

J. P. Harger, Martin and Sreedharan-Menon, Ramesh

Abstract

The hydroxylamine derivative PhRP(O)NHOSO2Me (R 4;= 4;PhMeCH) reacts with ButNH2 to give the rearrangement product RP(O)(NHPh)NHBut by way of a reactive but non-transient intermediate. At low amine concentrations the intermediate can be observed by 31P NMR spectroscopy; it is thought to be the mixed anhydride RP(O)(NHPh)OSO2Me as it has the same chemical shift as an authentic sample generated from RP(O)(NHPh)Cl and AgOSO2Me. The intermediate is formed with high (or complete) stereospecificity but it reacts with ButNH2 with low stereospecificity.

Published
1999
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106. High blood tacrolimus and hyperkalemia in a heart transplant patient.

Author

Kumar Sahu, Manoj, Pal Singh, Sarvesh, Das, Anupam, Abraham, Atul, Airan, Balram, Alam, Intekhab, Menon, Ramesh, Devagourou, V., Gupta, Anish, Sahu, Manoj Kumar, and Singh, Sarvesh Pal

Subjects
HEART transplantation complications, TACROLIMUS, HYPERKALEMIA, DILATED cardiomyopathy, ECHOCARDIOGRAPHY, CORTISONE, THERAPEUTICS, HEART transplantation, IMMUNOSUPPRESSIVE agents
Abstract

The article presents a case study of a 43-year-old woman who experienced complications after undergoing an orthotopic heart transplantation (OHT) for her dilated cardiomyopathy. The patient then went for an echocardiography test which showed a mild right ventricle dysfunction and risk of developing hyperkalemia. The article also discusses the drug effectiveness of fludrocortisone as treatment for hyperkalemia.

Published
2017
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107. Transcript profiling of different types of multiple sclerosis lesions yields FGF1 as a promoter of remyelination

Author

Mohan, Hema, Friese, Anita, Albrecht, Stefanie, Krumbholz, Markus, Elliott, Christina L., Arthur, Ariel, Menon, Ramesh, Farina, Cinthia, Junker, Andreas, Stadelmann, Christine, Barnett, Susan C., Huitinga, Inge, Wekerle, Hartmut, Hohlfeld, Reinhard, Lassmann, Hans, Kuhlmann, Tanja, Linington, Christopher, Meinl, Edgar, and Netherlands Institute for Neuroscience (NIN)

Subjects
Multiple Sclerosis, Gene Expression Profiling, Interleukin-8, Fibroblast growth factor, Brain, Leukemia Inhibitory Factor, White Matter, Mice, Inbred C57BL, Rats, Sprague-Dawley, Tissue Culture Techniques, Mice, Oligodendroglia, Remyelination, Spinal Cord, Astrocytes, Animals, Fibroblast Growth Factor 1, Humans, RNA, Messenger, Demyelination, Rats, Wistar, Cells, Cultured, Myelin Sheath, Research Article
Abstract

Chronic demyelination is a pathological hallmark of multiple sclerosis (MS). Only a minority of MS lesions remyelinates completely. Enhancing remyelination is, therefore, a major aim of future MS therapies. Here we took a novel approach to identify factors that may inhibit or support endogenous remyelination in MS. We dissected remyelinated, demyelinated active, and demyelinated inactive white matter MS lesions, and compared transcript levels of myelination and inflammation-related genes using quantitative PCR on customized TaqMan Low Density Arrays. In remyelinated lesions, fibroblast growth factor (FGF) 1 was the most abundant of all analyzed myelination-regulating factors, showed a trend towards higher expression as compared to demyelinated lesions and was significantly higher than in control white matter. Two MS tissue blocks comprised lesions with adjacent de- and remyelinated areas and FGF1 expression was higher in the remyelinated rim compared to the demyelinated lesion core. In functional experiments, FGF1 accelerated developmental myelination in dissociated mixed cultures and promoted remyelination in slice cultures, whereas it decelerated differentiation of purified primary oligodendrocytes, suggesting that promotion of remyelination by FGF1 is based on an indirect mechanism. The analysis of human astrocyte responses to FGF1 by genome wide expression profiling showed that FGF1 induced the expression of the chemokine CXCL8 and leukemia inhibitory factor, two factors implicated in recruitment of oligodendrocytes and promotion of remyelination. Together, this study presents a transcript profiling of remyelinated MS lesions and identified FGF1 as a promoter of remyelination. Modulation of FGF family members might improve myelin repair in MS. Electronic supplementary material The online version of this article (doi:10.1186/s40478-014-0168-9) contains supplementary material, which is available to authorized users.

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108. Coronavirus disease 2019 in children: Clinical & epidemiological implications.

Author

Kuttiatt, Vijesh, Abraham, Philip, Menon, Ramesh, Vaidya, Pankaj, and Rahi, Manju

Subjects
*COVID-19, *JUVENILE diseases, *INFECTION prevention, *SYMPTOMS, *INFECTION control
Abstract

Despite the global spread of the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) pandemic, there are limited data emerging in children. This review provides an update on clinical features, diagnosis, epidemiology, management and prevention of coronavirus disease 2019 (COVID-19) in children. Specific characteristics noted in children and their implications in disease management as well as transmission control are highlighted. Besides respiratory symptoms, gastrointestinal and atypical features such as chilblains, neurological symptoms and multisystem inflammation are also reported. Younger infants and those with comorbidity were found to be at risk of severe illness. Infected pregnant women and neonates were reported to have good prognosis. It is possible to manage the children with mild disease at home, with strict infection prevention control measures; severely affected require respiratory support and intensive care management. There are anecdotal reports of using antiviral and immunomodulatory drugs, benefit of which needs to be confirmed in clinical trials. A significant percentage of asymptomatic infection in children has epidemiological implication as these may act as links in transmission chain in the community. There is a need for systematic data on extra-pulmonary manifestations and atypical features, risk factors of severity, role of imaging and biomarkers, testing and management strategies and trials with antivirals and immunomodulatory drugs in children. The psychosocial effects of quarantine, closure of schools, lack of play activities and impact of lockdown need to be addressed. Understanding the biological basis for the profound age-dependent differential outcome of COVID-19 infection is important. Elucidating the protective mechanisms in children may aid in developing novel treatment strategies. [ABSTRACT FROM AUTHOR]

Published
2020
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111. Discover The Untapped UPS Market.

Author

Menon, Ramesh

Subjects
UNINTERRUPTIBLE power supply, COMPUTER value-added resellers, DATA protection, DATA corruption, BACK up systems
Abstract

The article focuses on the uninterrupted power supply (UPS) market. It notes that the risk of data loss or system damage related to power problems can be prevented or mitigated with a proper power protection system. It is said that UPS has obtained importance in which its cost is outweighed by the cost of failure and of data and productivity loss. Several opportunities associated with UPS overlooked by value-added resellers (VARs) are cited, one is the new revenues from power audits.

Published
2012

112. Virtual Environments Make Business Opportunities A Reality For VARs.

Author

Menon, Ramesh

Subjects
CLOUD computing, COMPUTER value-added resellers, UNINTERRUPTIBLE power supply, DISTRIBUTED computing, EMERGENCY power supply
Abstract

The article discusses the opportunity provided by virtual environments to expand business by offering cloud-complementary solutions. It was said that giving power protection lets resellers design a comprehensive solutions package. Uninterruptible power systems are available that monitor energy use and run at 99-percent efficiency. It was mentioned that satisfaction with the solutions and services provided is one of the most important metrics in business.

Published
2012

113. Building the CFPB.

Author

Menon, Ramesh

Subjects
BANKING industry, COMPUTER architecture, INFORMATION resources management, PRODUCT safety, TECHNOLOGICAL innovations
Abstract

In this article, the author discusses the challenges of creating new bureau's internal architecture and data strategies Consumer Financial Protection Bureau (CFPB) in the U.S. It states that one of the challenges of CFPB is the need for comprehensive and innovative data management strategies. In addition, CFPB need more empirical information to assess product safety.

Published
2010

115. Neural precursor cell-secreted TGF-β2 redirects inflammatory monocyte-derived cells in CNS autoimmunity

Author

Gianvito Martino, Jose Manuel Garcia Manteiga, Melanie Greter, Giancarlo Comi, Sundararajan Srinivasan, Arianna Merlini, Cinthia Farina, Marco Bacigaluppi, Cecilia Laterza, Donatella De Feo, Elena Brambilla, Ramesh Menon, Linda Ottoboni, Erica Butti, University of Zurich, Martino, Gianvito, Feo, Donatella De, Merlini, Arianna, Brambilla, Elena, Ottoboni, Linda, Laterza, Cecilia, Menon, Ramesh, Srinivasan, Sundararajan, Farina, Cinthia, Manteiga, Jose Manuel Garcia, Butti, Erica, Bacigaluppi, Marco, Comi, Giancarlo, and Greter, Melanie

Subjects
0301 basic medicine, Multiple Sclerosis, Mice, 129 Strain, Cellular differentiation, Inflammation, 610 Medicine & health, 2700 General Medicine, Dendritic Cell, Monocyte, 10263 Institute of Experimental Immunology, Monocytes, Transcriptome, Immunomodulation, 03 medical and health sciences, Transforming Growth Factor beta2, 0302 clinical medicine, Neural Stem Cells, Precursor cell, Multiple Sclerosi, Animals, Medicine, Neural Stem Cell, Cytokine, Neuroinflammation, Cells, Cultured, business.industry, Animal, Medicine (all), Experimental autoimmune encephalomyelitis, Brain, Cell Differentiation, Dendritic Cells, General Medicine, T-Lymphocytes, Helper-Inducer, medicine.disease, Transplantation, Mice, Inbred C57BL, 030104 developmental biology, Cancer research, Cytokines, 570 Life sciences, biology, Female, Microglia, medicine.symptom, business, Reprogramming, 030217 neurology & neurosurgery, Research Article
Abstract

In multiple sclerosis, the pathological interaction between autoreactive Th cells and mononuclear phagocytes in the CNS drives initiation and maintenance of chronic neuroinflammation. Here, we found that intrathecal transplantation of neural stem/precursor cells (NPCs) in mice with experimental autoimmune encephalomyelitis (EAE) impairs the accumulation of inflammatory monocyte-derived cells (MCs) in the CNS, leading to improved clinical outcome. Secretion of IL-23, IL-1, and TNF-α, the cytokines required for terminal differentiation of Th cells, decreased in the CNS of NPC-treated mice, consequently inhibiting the induction of GM-CSF-producing pathogenic Th cells. In vivo and in vitro transcriptome analyses showed that NPC-secreted factors inhibit MC differentiation and activation, favoring the switch toward an antiinflammatory phenotype. Tgfb2-/-NPCs transplanted into EAE mice were ineffective in impairing MC accumulation within the CNS and failed to drive clinical improvement. Moreover, intrathecal delivery of TGF-β2 during the effector phase of EAE ameliorated disease severity. Taken together, these observations identify TGF-β2 as the crucial mediator of NPC immunomodulation. This study provides evidence that intrathecally transplanted NPCs interfere with the CNS-restricted inflammation of EAE by reprogramming infiltrating MCs into antiinflammatory myeloid cells via secretion of TGF-β2.

Published
2017
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116. Transcriptional dysregulation of Interferome in experimental and human Multiple Sclerosis

Author

Sundararajan Srinivasan, Fabiana Rizzo, Elena Brini, Paul J. Hertzog, Martina Severa, Gianvito Martino, Cinthia Farina, Vittorio Martinelli, Eliana M. Coccia, Rosella Mechelli, Marco Salvetti, Giancarlo Comi, Roberto Furlan, Ramesh Menon, Srinivasan, Sundararajan, Severa, Martina, Rizzo, Fabiana, Menon, Ramesh, Brini, Elena, Mechelli, Rosella, Martinelli, Vittorio, Hertzog, Paul, Salvetti, Marco, Furlan, Roberto, Martino, Gianvito, Comi, Giancarlo, Coccia, Eliana, and Farina, Cinthia

Subjects
CD4-Positive T-Lymphocytes, Central Nervous System, Male, 0301 basic medicine, experimental autoimmune encephalomyelitis, caspase-1, Transcriptome, Interferon, Multidisciplinary, Experimental autoimmune encephalomyelitis, regulated genes, Middle Aged, Medicine, Female, roles, signature, medicine.drug, Adult, Encephalomyelitis, Autoimmune, Experimental, Multiple Sclerosis, multidisciplinary, ifn-beta, fingolimod, responses, cells, Science, Interferome, Biology, Article, Young Adult, 03 medical and health sciences, Immune system, medicine, Animals, Humans, Immunologic Factors, Author Correction, Neuroinflammation, Aged, Blood Cells, Gene Expression Profiling, Multiple sclerosis, medicine.disease, Mice, Inbred C57BL, Gene expression profiling, 030104 developmental biology, Case-Control Studies, Immunology, Interferons
Abstract

Recent evidence indicates that single multiple sclerosis (MS) susceptibility genes involved in interferon (IFN) signaling display altered transcript levels in peripheral blood of untreated MS subjects, suggesting that responsiveness to endogenous IFN is dysregulated during neuroinflammation. To prove this hypothesis we exploited the systematic collection of IFN regulated genes (IRG) provided by the Interferome database and mapped Interferome changes in experimental and human MS. Indeed, central nervous system tissue and encephalitogenic CD4 T cells during experimental autoimmune encephalomyelitis were characterized by massive changes in Interferome transcription. Further, the analysis of almost 500 human blood transcriptomes showed that (i) several IRG changed expression at distinct MS stages with a core of 21 transcripts concordantly dysregulated in all MS forms compared with healthy subjects; (ii) 100 differentially expressed IRG were validated in independent case-control cohorts; and (iii) 53 out of 100 dysregulated IRG were targeted by IFN-beta treatment in vivo. Finally, ex vivo and in vitro experiments established that IFN-beta administration modulated expression of two IRG, ARRB1 and CHP1, in immune cells. Our study confirms the impairment of Interferome in experimental and human MS, and describes IRG signatures at distinct disease stages which can represent novel therapeutic targets in MS.

Published
2017
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117. Developmentally coordinated extrinsic signals drive human pluripotent stem cell differentiation toward authentic DARPP-32+ medium-sized spiny neurons

Author

Alessia Delli Carri, Paolo Spaiardi, Gianvito Martino, Francesca Talpo, Mariah Jillian Lelos, Romina Vuono, Ramesh Menon, Valentina Castiglioni, Stefano Camnasio, Andrea Faedo, Marco Onorati, Gerardo Biella, Roger A. Barker, Elena Cattaneo, Mauro Toselli, Stephen B. Dunnett, Carri, Alessia Delli, Onorati, Marco, Lelos, Mariah J., Castiglioni, Valentina, Faedo, Andrea, Menon, Ramesh, Camnasio, Stefano, Vuono, Romina, Spaiardi, Paolo, Talpo, Francesca, Toselli, Mauro, Martino, Gianvito, Barker, Roger A., Dunnett, Stephen B., Biella, Gerardo, and Cattaneo, Elena

Subjects
Patch-Clamp Techniques, Time Factors, Cell Transplantation, Cellular differentiation, Patch-Clamp Technique, Striatum, Mice, 0302 clinical medicine, Striatal neuronal differentiation, Neuromodulation, GABAergic Neurons, Induced pluripotent stem cell, DARPP-32 (PPP1R1B), Directed differentiation, Human embryonic stem cells, Huntington's disease, Medium spiny neurons, Animals, Cell Adhesion, Cell Differentiation, Cell Lineage, Cell Survival, Dopamine and cAMP-Regulated Phosphoprotein 32, Embryonic Stem Cells, Female, Fibroblasts, Flow Cytometry, Humans, Huntington Disease, Neurons, Oligonucleotide Array Sequence Analysis, Pluripotent Stem Cells, Quinolinic Acid, RNA, Rats, Stem Cells, Developmental Biology, Molecular Biology, 0303 health sciences, Anatomy, medicine.anatomical_structure, Fibroblast, Stem cell, Human, Time Factor, Biology, Medium spiny neuron, 03 medical and health sciences, Embryonic Stem Cell, Stem Cell, medicine, GABAergic Neuron, 030304 developmental biology, Pluripotent Stem Cell, Human embryonic stem cell, Animal, Oligonucleotide Array Sequence Analysi, Neuron, Embryonic stem cell, nervous system, Rat, Neuroscience, 030217 neurology & neurosurgery
Abstract

Medium-sized spiny neurons (MSNs) are the only neostriatum projection neurons, and their degeneration underlies some of the clinical features of Huntington's disease. Using knowledge of human developmental biology and exposure to key neurodevelopmental molecules, human pluripotent stem (hPS) cells were induced to differentiate into MSNs. In a feeder-free adherent culture, ventral telencephalic specification is induced by BMP/TGFβ inhibition and subsequent SHH/DKK1 treatment. The emerging FOXG1/GSX2 telencephalic progenitors are then terminally differentiated, resulting in the systematic line-independent generation of FOXP1/FOXP2/CTIP2/calbindin/DARPP-32 MSNs. Similar to mature MSNs, these neurons carry dopamine and A2a receptors, elicit a typical firing pattern and show inhibitory postsynaptic currents, as well as dopamine neuromodulation and synaptic integration ability in vivo. When transplanted into the striatum of quinolinic acid-lesioned rats, hPS-derived neurons survive and differentiate into DARPP-32 neurons, leading to a restoration of apomorphine-induced rotation behavior. In summary, hPS cells can be efficiently driven to acquire a functional striatal fate using an ontogeny-recapitulating stepwise method that represents a platform for in vitro human developmental neurobiology studies and drug screening approaches. © 2013. Published by The Company of Biologists Ltd.

Published
2013

118. Dysregulation of MS risk genes and pathways at distinct stages of disease.

Author

Srinivasan S, Di Dario M, Russo A, Menon R, Brini E, Romeo M, Sangalli F, Costa GD, Rodegher M, Radaelli M, Moiola L, Cantarella D, Medico E, Martino G, Furlan R, Martinelli V, Comi G, and Farina C

Abstract

Objective: To perform systematic transcriptomic analysis of multiple sclerosis (MS) risk genes in peripheral blood mononuclear cells (PBMCs) of subjects with distinct MS stages and describe the pathways characterized by dysregulated gene expressions., Methods: We monitored gene expression levels in PBMCs from 3 independent cohorts for a total of 297 cases (including clinically isolated syndromes (CIS), relapsing-remitting MS, primary and secondary progressive MS) and 96 healthy controls by distinct microarray platforms and quantitative PCR. Differential expression and pathway analyses for distinct MS stages were defined and validated by literature mining., Results: Genes located in the vicinity of MS risk variants displayed altered expression in peripheral blood at distinct stages of MS compared with the healthy population. The frequency of dysregulation was significantly higher than expected in CIS and progressive forms of MS. Pathway analysis for each MS stage-specific gene list showed that dysregulated genes contributed to pathogenic processes with scientific evidence in MS., Conclusions: Systematic gene expression analysis in PBMCs highlighted selective dysregulation of MS susceptibility genes playing a role in novel and well-known pathogenic pathways.

Published
2017
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119. Developmentally coordinated extrinsic signals drive human pluripotent stem cell differentiation toward authentic DARPP-32+ medium-sized spiny neurons.

Author

Delli Carri A, Onorati M, Lelos MJ, Castiglioni V, Faedo A, Menon R, Camnasio S, Vuono R, Spaiardi P, Talpo F, Toselli M, Martino G, Barker RA, Dunnett SB, Biella G, and Cattaneo E

Subjects
Animals, Cell Adhesion, Cell Differentiation, Cell Lineage, Cell Survival, Cell Transplantation, Embryonic Stem Cells cytology, Female, Fibroblasts cytology, Fibroblasts metabolism, Flow Cytometry, GABAergic Neurons metabolism, Humans, Huntington Disease metabolism, Mice, Oligonucleotide Array Sequence Analysis, Patch-Clamp Techniques, Quinolinic Acid pharmacology, RNA metabolism, Rats, Stem Cells cytology, Time Factors, Dopamine and cAMP-Regulated Phosphoprotein 32 metabolism, Neurons metabolism, Pluripotent Stem Cells metabolism
Abstract

Medium-sized spiny neurons (MSNs) are the only neostriatum projection neurons, and their degeneration underlies some of the clinical features of Huntington's disease. Using knowledge of human developmental biology and exposure to key neurodevelopmental molecules, human pluripotent stem (hPS) cells were induced to differentiate into MSNs. In a feeder-free adherent culture, ventral telencephalic specification is induced by BMP/TGFβ inhibition and subsequent SHH/DKK1 treatment. The emerging FOXG1(+)/GSX2(+) telencephalic progenitors are then terminally differentiated, resulting in the systematic line-independent generation of FOXP1(+)/FOXP2(+)/CTIP2(+)/calbindin(+)/DARPP-32(+) MSNs. Similar to mature MSNs, these neurons carry dopamine and A2a receptors, elicit a typical firing pattern and show inhibitory postsynaptic currents, as well as dopamine neuromodulation and synaptic integration ability in vivo. When transplanted into the striatum of quinolinic acid-lesioned rats, hPS-derived neurons survive and differentiate into DARPP-32(+) neurons, leading to a restoration of apomorphine-induced rotation behavior. In summary, hPS cells can be efficiently driven to acquire a functional striatal fate using an ontogeny-recapitulating stepwise method that represents a platform for in vitro human developmental neurobiology studies and drug screening approaches.

Published
2013
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