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1. Emerging roles for HMGB1 protein in immunity, inflammation, and cancer

Author

Martinotti S, Patrone M, and Ranzato E

Subjects
HMGB1, alarmin, inflammation, DNA replication, wound repair, immunity, post-translational modifications, cancer, Immunologic diseases. Allergy, RC581-607
Abstract

Simona Martinotti, Mauro Patrone, Elia Ranzato DiSIT – Dipartimento di Scienze e Innovazione Tecnologica, University of Piemonte Orientale, Alessandria, Italy Abstract: High-mobility group box 1 (HMGB1) protein is a member of the highly conserved non-histone DNA binding protein family. First identified in 1973, as one of a group of chromatin-associated proteins with high acidic and basic amino acid content, it was so named for its characteristic rapid mobility in polyacrylamide gel electrophoresis. HMGB1 was later discovered to have another function. It is released from a variety of cells into the extracellular milieu to act on specific cell-surface receptors. In this latter role, HMGB1 is a proinflammatory cytokine that may contribute to many inflammatory diseases, including sepsis. Therefore, HMGB1 regulates intracellular cascades influencing immune cell functions, including chemotaxis and immune modulation. The bioactivity of the HMGB1 is determined by specific posttranslational modifications that regulate its role in inflammation and immunity. During tumor development, HMGB1 has been reported to play paradoxical roles in promoting both cell survival and death by regulating multiple signaling pathways. In this review, we focus on the role of HMGB1 in physiological and pathological responses, as well as the mechanisms by which it contributes to immunity, inflammation, and cancer progression. Keywords: alarmin, DNA replication, HMGB1, posttranslational modifications, wound repair

Published
2015

2. New aspect of allergic contact dermatitis, an inflammatory skin disorder mediated by mast cells: Can IL-38 help?

Author

Lauritano, D, Ronconi, G, Caraffa, A, Enrica Gallenga, C, Kritas, S, Di Emidio, P, Martinotti, S, Tete, G, Ross, R, Conti, P, Lauritano D., Ronconi G., Caraffa A., Enrica Gallenga C., Kritas S. K., Di Emidio P., Martinotti S., Tete G., Ross R., Conti P., Lauritano, D, Ronconi, G, Caraffa, A, Enrica Gallenga, C, Kritas, S, Di Emidio, P, Martinotti, S, Tete, G, Ross, R, Conti, P, Lauritano D., Ronconi G., Caraffa A., Enrica Gallenga C., Kritas S. K., Di Emidio P., Martinotti S., Tete G., Ross R., and Conti P.

Abstract

Atopic dermatitis (AD) is an inflammatory reaction of the skin that can occur in several parts of the body and can be provoked or exacerbated by food and/or environmental compounds. Allergic contact dermatitis (ACD) is a potential enhancer of AD, and an epidermal barrier breaker which induces greater penetration of allergens and other compounds. ACD presents an eczematous rash, red and itchy, with inflammation mediated by cytokines. ACD is an immunological disorder caused by contact with an allergic substance (haptens) that involves immunotoxicity, irritation and inflammation. Mast cells (MCs) are important immune cells that intervene, as effector cells, in allergic and anaphylactic reactions, asthma, autoimmune diseases and cancer. In dermatitis, activated MCs release inflammatory chemical mediators and secrete pro-inflammatory cytokines, including interleukin (IL)-1, TNF, and IL-33. In addition, IL-1 activates MCs to generate a number of cytokines and chemokines, which aggravate inflammation. IL-38 cytokine, an IL-1 family member, is secreted by activated immune cells, including macrophages and lymphocytes, and possesses anti-inflammatory activity. IL-38, by binding IL-36 receptor (IL-36R), provokes suppression of inflammation in many immune diseases. In particular, IL-38 inhibits the generation of IL-1, IL-6 and IL-8 along with other cytokines/chemokines. Here, we hypothesize for the first time that IL-38 may suppresses the inflammatory response in dermatitis, exerting beneficial therapeutic effect.

Published
2020

4. Glutamate triggers intracellular Ca 2+ oscillations and nitric oxide release by inducing NAADP- and InsP 3 -dependent Ca 2+ release in mouse brain endothelial cells

Author

Zuccolo, E, Kheder, DA, Lim, D, Perna, A, Di Nezza, F, Botta, L, Scarpellino, G, Negri, S, Martinotti, S, Soda, T, Forcaia, G, Riboni, L, Ranzato, E, Sancini, G, Ambrosone, L, D'Angelo, E, Guerra, G, Moccia, F, Zuccolo, E, Kheder, D, Lim, D, Perna, A, Di Nezza, F, Botta, L, Scarpellino, G, Negri, S, Martinotti, S, Soda, T, Forcaia, G, Riboni, L, Ranzato, E, Sancini, G, Ambrosone, L, D'Angelo, E, Guerra, G, and Moccia, F

Subjects
Ca, nitric oxide, oscillations, 2+, endothelial cell, glutamate, Ca2+ oscillation, neurovascular coupling (NVC)
Abstract

The neurotransmitter glutamate increases cerebral blood flow by activating postsynaptic neurons and presynaptic glial cells within the neurovascular unit. Glutamate does so by causing an increase in intracellular Ca 2+ concentration ([Ca 2+ ] i ) in the target cells, which activates the Ca 2+ /Calmodulin-dependent nitric oxide (NO) synthase to release NO. It is unclear whether brain endothelial cells also sense glutamate through an elevation in [Ca 2+ ] i and NO production. The current study assessed whether and how glutamate drives Ca 2+ -dependent NO release in bEND5 cells, an established model of brain endothelial cells. We found that glutamate induced a dose-dependent oscillatory increase in [Ca 2+ ] i , which was maximally activated at 200 μM and inhibited by α-methyl-4-carboxyphenylglycine, a selective blocker of Group 1 metabotropic glutamate receptors. Glutamate-induced intracellular Ca 2+ oscillations were triggered by rhythmic endogenous Ca 2+ mobilization and maintained over time by extracellular Ca 2+ entry. Pharmacological manipulation revealed that glutamate-induced endogenous Ca 2+ release was mediated by InsP 3 -sensitive receptors and nicotinic acid adenine dinucleotide phosphate (NAADP) gated two-pore channel 1. Constitutive store-operated Ca 2+ entry mediated Ca 2+ entry during ongoing Ca 2+ oscillations. Finally, glutamate evoked a robust, although delayed increase in NO levels, which was blocked by pharmacologically inhibition of the accompanying intracellular Ca 2+ signals. Of note, glutamate induced Ca 2+ -dependent NO release also in hCMEC/D3 cells, an established model of human brain microvascular endothelial cells. This investigation demonstrates for the first time that metabotropic glutamate-induced intracellular Ca 2+ oscillations and NO release have the potential to impact on neurovascular coupling in the brain.

Published
2019

5. Characterization of the modification in mitochondrial proteome due to eIF6 depletion by SWATH-MS analysis and multivariate statistical tools

Author

Robotti, E, Martinotti, S, Manfredi, M, Conte, E, Scagliola, A, Calamita, P, Gosetti, F, Marengo, E, Ranzato, E, Biffo, S, Robotti, E, Martinotti, S, Manfredi, M, Conte, E, Scagliola, A, Calamita, P, Gosetti, F, Marengo, E, Ranzato, E, and Biffo, S

Subjects
CHIM/01 - CHIMICA ANALITICA, mitochondrial proteome, eIF6, SWATH-MS, multivariate analysis, chemometrics
Published
2018

7. Molecular Pathogenesis of B-Cell Chronic Lymphocytic Leukemia: Analysis of 13q14 Chromosomal Deletions

Author

Migliazza, A., primary, Cayanis, E., additional, Bosch-Albareda, F., additional, Komatsu, H., additional, Martinotti, S., additional, Toniato, E., additional, Kalachikov, S., additional, Bonaldo, M. F., additional, Jelenc, P., additional, Ye, X., additional, Rzhetsky, A., additional, Qu, X., additional, Chien, M., additional, Inghirami, G., additional, Gaidano, G., additional, Vitolo, U., additional, Saglio, G., additional, Resegotti, L., additional, Zhang, P., additional, Soares, M. B., additional, Russo, J., additional, Fischer, S. G., additional, Edelman, I. S., additional, Efstratiadis, A., additional, and Dalla-Favera, R., additional

Published
2000
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8. Mast Cells Mediate Rheumatoid Arthritis-Inhibitory Role of IL-37

Author

Conti, P, Lauritano, D, Caraffa, A, Gallenga, Ce, Carinci, F, Ronconi, Gianpaolo, Kritas, Sk, Di Emidio, P, Martinotti, S, Pandolfi, Franco, Ronconi, G, Pandolfi, F (ORCID:0000-0001-8799-8173), Conti, P, Lauritano, D, Caraffa, A, Gallenga, Ce, Carinci, F, Ronconi, Gianpaolo, Kritas, Sk, Di Emidio, P, Martinotti, S, Pandolfi, Franco, Ronconi, G, and Pandolfi, F (ORCID:0000-0001-8799-8173)

Abstract

Rheumatoid arthritis (RA) is an autoimmune, chronic inflammatory, disabling arthropathy that severely affects the quality of life. This disease involves several proinflammatory cytokines, including interleukin (IL)-1 beta and tumor necrosis factor (TNF). IL-1 induces TNF and vice versa, causing joint damage and cartilage degradation. Current antirheumatic drugs may be effective, but they possess many unwanted side effects. In recent years, inhibitors of proinflammatory cytokines have increasingly entered mainstream clinical practice. Recent evidence indicates that IL-37, which has anti-inflammatory properties, is increased in the serum and is released from white blood cells in patients with RA. Mast cells (MCs), stimulated by the neuropeptide substance P (SP) and IL-33, release IL-1 beta and TNF. Recent evidence indicates that large amounts of IL-1 beta and TNF can be released from human MCs, which also secrete CXCL8, which promotes migration of immune cells, causing erosion of the bone and cartilage. Treatment with IL-37 can block the MC stimulation and release of inflammatory compounds, attenuating the severity of the disease and/or altering its progression.

Published
2019

10. Mitochondrial proteome modifications due to eIF6 depletion by UHPLCQTOF MS/MS with SWATH-MS acquisition

Author

Robotti, E, Martinotti, S, Manfredi, M, Brina, D, Scagliola, A, Ranzato, E, Biffo, S, Gosetti, F, Marengo, E, Robotti, E, Martinotti, S, Manfredi, M, Brina, D, Scagliola, A, Ranzato, E, Biffo, S, Gosetti, F, and Marengo, E

Subjects
CHIM/01 - CHIMICA ANALITICA, Mitochondrial proteome, eIF6 depletion, UHPLC- MS/MS, SWATH-MS, Mitochondrial Proteome, eIF6, UHPLC-MS/MS, SWATH-MS
Published
2017

12. Identification of the active species from the aqueous extract of Pterocarpus marsupium heartwood against cancer cell proliferation and investigation of the anticancer mechanism by a proteomic approach

Author

Gosetti, F, Martinotti, S, Bolfi, B, Mazzucco, E, Ranzato, E, Manfredi, E, Marengo, E, Gosetti, F, Martinotti, S, Bolfi, B, Mazzucco, E, Ranzato, E, Manfredi, E, and Marengo, E

Subjects
aqueous extract, Pterocarpus marsupium, heartwood, cancer cell, anticancer, proteomic approach, CHIM/01 - CHIMICA ANALITICA
Published
2016

13. SWATH-MS Proteomics and Chemometrics to Study the Cardiovascular Disease

Author

Manfredi, M, Conte, E, Chiariello, C, Robotti, E, Ranzato, E, Martinotti, S, Mazzucco, E, Gosetti, F, Castagna, A, Cecconi, D, Olivieri, O, Marengo, E, Manfredi, M, Conte, E, Chiariello, C, Robotti, E, Ranzato, E, Martinotti, S, Mazzucco, E, Gosetti, F, Castagna, A, Cecconi, D, Olivieri, O, and Marengo, E

Subjects
SWATH-MS, Proteomics, Chemometrics, Cardiovascular Disease, CHIM/01 - CHIMICA ANALITICA
Published
2016

14. miR-2861 is involved in osteogenic commitment of human periodontal ligament stem cells grown onto 3D scaffold

Author

Diomede F, Merciaro I, Martinotti S, Mf, Cavalcanti, Caputi S, emanuela mazzon, and Trubiani O

Subjects
Bone Regeneration, Microscopy, Confocal, Tissue Engineering, Tissue Scaffolds, Periodontal Ligament, Swine, Stem Cells, Cell Differentiation, Core Binding Factor Alpha 1 Subunit, Flow Cytometry, Real-Time Polymerase Chain Reaction, MicroRNAs, Osteogenesis, Microscopy, Electron, Scanning, Animals, Humans, Cells, Cultured
Abstract

miR-2861 endorsing osteoblast differentiation through the overexpression of Runt-related transcription factor 2 (RUNX2) protein has been recently described. In this study we evaluated: the performance of living construct, composed by human Periodontal Ligament Stem Cells (hPDLSCs) and 3D scaffold (EXg), and the behaviour of miR-2861/RUNX2 expression pathway on the osteogenic commitment. Human PDLSCs were seeded with and without EXg scaffold and cultured under basal and osteogenic conditions. Morphological features, adhesiveness and differentiation abilities were analysed using scanning electron and confocal laser scanning microscopy. Time-course of RUNX2, ALP, OPN and miR-2861 were evaluated through RT-PCR analysis. Our results highlighted that the osteogenic differentiation was mostly obvious in the hPDLSCs, grown onto 3D scaffold in presence of osteoinductive medium. Moreover, the overexpression of miR-2861 and RUNX2 in hPDLSCs cultured in presence of EXg under osteogenic and standard conditions was demonstrated. In synthesis, the increased expression of miR-2861/RUNX2 provides new insights regarding miRNA signaling network in the presence of scaffold providing an additional method to evaluate the performance of biomaterial in bone regeneration.

Published
2017

22. The Human onc Gene c-myc: Structure, Expression, and Amplification in the Human Promyelocytic Leukemia Cell Line HL-60

Author

Favera, R. Dalla, Westin, E., Gelmann, E. P., Martinotti, S., Bregni, M., Wong-Staal, F., Gallo, R. C., Heimpel, H., editor, Huhn, D., editor, Mueller-Eckhardt, C., editor, Ruhenstroth-Bauer, G., editor, Neth, Rolf, editor, Gallo, Robert C., editor, Greaves, Melvyn F., editor, Moore, Malcolm A. S., editor, and Winkler, Kurt, editor

Published
1983
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24. Studio di caratterizzazione di fitocomposti mediante LC-MS/MS

Author

Gosetti, F, Chiuminatto, U, Mastroianni, R, Martinotti, S, Ranzato, E, Marengo, E, Gosetti, F, Chiuminatto, U, Mastroianni, R, Martinotti, S, Ranzato, E, and Marengo, E

Subjects
LC-MS/MS, fitocomposti, polifenoli, CHIM/01 - CHIMICA ANALITICA, characterization, plant extract, LC-MS/MS
Published
2014

27. HMGB1 Osteo-Modulatory Action on Osteosarcoma SaOS-2 Cell Line: An Integrated Study From Biochemical and -Omics Approaches

Author

Martinotti, S, Patrone, M, Manfredi, M, Gosetti, F, Pedrazzi, M, Marengo, E, Ranzato, E, MARTINOTTI, Simona, PATRONE, Mauro, MANFREDI, MARCELLO, GOSETTI, Fabio, Pedrazzi Marco, MARENGO, Emilio, RANZATO, Elia, Martinotti, S, Patrone, M, Manfredi, M, Gosetti, F, Pedrazzi, M, Marengo, E, Ranzato, E, MARTINOTTI, Simona, PATRONE, Mauro, MANFREDI, MARCELLO, GOSETTI, Fabio, Pedrazzi Marco, MARENGO, Emilio, and RANZATO, Elia

Abstract

High mobility group box protein-1 (HMGB1) is released from cells under various pathological conditions and it plays a pivotal role as an alarmin signaling tissue damage. Little is known about the impact of HMGB1 in bone repair and remodeling. To this aim, we focused on HMGB1-induced effects on the in vitro osteoblast model SaOS-2. Cell proliferation was stimulated with a maximum at concentration of 2.5 nM, and such a dose also stimulated cell migration and scratch wound healing. We then characterized the modulatory effect of HMGB1 on bone biology, by using osteogenesis/mineralization assays, a PCR array, and the analysis of a series of osteogenic markers. We performed also a proteomic screening using SWATH-MS on SaOS-2 cell exposed to HMGB1 and we provide evidence for proteins modulated in HMGB1 exposed cells. Taken together, our data demonstrate that SaOS-2 cell proliferation, migration, and osteogenic differentiation were increased by HMGB1. We, therefore, propose that HMGB1 could be a potent bone-remodeling signal but the physiological meaning of this property remains to be more ascertained. J. Cell. Biochem. 117: 2559–2569, 2016. © 2016 Wiley Periodicals, Inc.

Published
2016

28. Characterization of the volatile and nonvolatile fractions of heartwood aqueous extract from Pterocarpus marsupium and evaluation of its cytotoxicity against cancer cell lines

Author

Gosetti, F, Chiuminatto, U, Martinotti, S, Bolfi, B, Ranzato, E, Manfredi, M, Marengo, E, Gosetti, F, Chiuminatto, U, Martinotti, S, Bolfi, B, Ranzato, E, Manfredi, M, and Marengo, E

Abstract

Pterocarpusmarsupium is awell-known plant due to its healing properties, in particular, the use of its aqueous extract is able to reduce blood sugar levels and blood triglyceride concentrations. Although this plant has already been widely studied, a complete characterization of its aqueous extract has not been reported. The present study deals with the characterization of the aqueous extract of P. marsupium in order to obtain a full fingerprint of the volatile and nonvolatile constituents. The volatile constituents were identified by CG-MS, whereas the nonvolatile fraction was characterized by UHPLC-MS/MS using a nontarget approach. Several compounds were identified, in particular, polyphenolic species belonging to the class of proanthocyanidins. Cytotoxicity tests were carried out on four different cancer cell lines and three different non-tumoral cell lines. Preliminary results indicate a selective cytotoxicity of the aqueous extract towards the cancer cells. The potential cytotoxicity due to the presence of metals in the aqueous extract was ruled out by testing an aqueous mixture of the metals at the same concentration found in the P. marsupium extract.

Published
2016

29. The secretome signature of malignant mesothelioma cell lines

Author

Manfredi, M, Martinotti, S, Gosetti, F, Ranzato, E, Marengo, E, Manfredi, M, Martinotti, S, Gosetti, F, Ranzato, E, and Marengo, E

Abstract

The secretome is the complex set of molecules secreted by cells; these molecules play a key role in cell signaling, communication and migration. Secretomics has been already used to discover new potential diagnostic biomarkers and therapeutic agents and to elucidate key autocrine pathways. Malignant mesothelioma (MMe), an extremely aggressive tumor, is characterized by a long latency period (20–30 years), a poor prognosis, and limited effective therapies. MMe has a highly secretory cell type, and the factors released by cells may act in an autocrine or paracrine fashion on tumor and stroma, where they may modulate the extracellular environment. The aim of this work is to characterize the secretome of two MMe cell lines, MM98 and REN, in comparison with a mesothelial cell line Met5A, in order to evaluate differences and similarities of these two different MMe cancer model systems, and to identify potential biomarkers. We performed quantitative shotgun proteomics using SWATH-MS technology and we identified a total of 421 proteins, 112 expressed in the secretome of REN cells, 208 expressed in the secretome of MM98 cells and 189 secreted by mesothelial cells; 25 proteins are shared by the two mesothelioma cell lines. Biological significance This study characterizes the secretome signature of the REN and MM98 cell lines, confirming the availability of a cell-culture based model in order to describe the cell-specific properties, and to provide a list of putative cancer biomarkers. This work constitutes the first qualitative and quantitative proteomic approach performed on MMe secretome. Moreover, since the data were acquired in SWATH-MS acquisition mode, they can be successively re-mined without performing a new analysis of the sample, which is extremely useful for retrospective analyses. The overall aim was to identify novel tumor-derived protein biomarkers with the potential to be applied for early diagnosis, prognosis, therapy prediction and/or disease monitoring of MM

Published
2016

30. Interleukin-2–Activated Rat Natural Killer Cells Express Inducible Nitric Oxide Synthase That Contributes to Cytotoxic Function and Interferon-γ Production

Author

Cifone, MARIA GRAZIA, D'Alo', S., Parroni, R., Millimaggi, D., Biordi, L., Martinotti, S., and Santoni, A.

Subjects
Immunology, Cell Biology, Hematology, Biochemistry
Abstract

Natural killer (NK) cells are large granular lymphocytes capable of destroying cells infected by virus or bacteria and susceptible tumor cells without prior sensitization and restriction by major histocompatability complex (MHC) antigens. Their cytotoxic activity could be strongly enhanced by interleukin-2 (IL-2). Previous findings, even if obtained with indirect experimental approaches, have suggested a possible involvement of the inducible nitric oxide (iNOS) pathway in the NK-mediated target cell killing. The aim of the present study was first to directly examine the induction of iNOS in IL-2–activated rat NK cells isolated from peripheral blood (PB-NK) or spleen (S-NK), and second to investigate the involvement of the iNOS-derived NO in the cytotoxic function of these cells. Our findings clearly indicate the induction of iNOS expression in IL-2–activated PB-NK and S-NK cells, as evaluated either at mRNA and protein levels. Accordingly, significantly high levels of iNOS activity were shown, as detected by the L-arginine to L-citrulline conversion in appropriate assay conditions. The consequent NO generation appears to partially account for NK cell-mediated DNA fragmentation and lysis of sensitive tumor target cells. In fact, functional inhibition of iNOS through specific inhibitors, as well as the almost complete abrogation of its expression through a specific iNOS mRNA oligodeoxynucleotide antisense, significantly reduced the lytic activity of IL-2–activated NK cells. Moreover, IL-2–induced interferon-γ production appears also to be dependent, at least in part, on iNOS induction.

Published
1999

31. Novel P53 mutations detected by FAMA in colorectal cancers

Author

DE GALITIIS, F, Cannita, K, Tessitore, A, Martella, F, DI ROCCO ZC, Russo, A, Adamo, V, Iacobelli, S, Martinotti, S, Marchetti, Paolo, Ficorella, C, Ricevuto, E, CONSORZIO INTERUNIVERSITARIO NAZIONALE BIO ONCOLOGIA, DE GALITIIS F, CANNITA K, TESSITORE A, MARTELLA F, DI ROCCO ZC, RUSSO A, ADAMO V, IACOBELLI S, MARTINOTTI S, MARCHETTI P, FICORELLA C, and RICEVUTO E

Subjects
Oncology, medicine.medical_specialty, Mutant, DNA Mutational Analysis, Mutation, Missense, Gene mutation, medicine.disease_cause, Exon, Internal medicine, medicine, Missense mutation, Humans, Key words: colon cancer, p53, mutations, FAMA, Allele, Gene, Mutation, business.industry, Hematology, DNA, Neoplasm, Exons, Genes, p53, Molecular biology, business, Colorectal Neoplasms, Heteroduplex
Abstract

Background The aim of the study was to identify p53 gene mutations by FAMA (fluorescence-assisted mismatch analysis) in colorectal cancers. Patients and methods Analytical scanning of the p53 gene (exons 5–9) was performed in colon cancer samples from 44 consecutive patients by FAMA. FAMA is a semiautomatic scanning approach based on the chemical cleavage of the mismatch in fluorescently labeled heteroduplex DNA, obtained from the combination of a normal and a mutated allele. FAMA has already shown optimal levels of diagnostic accuracy and sensitivity in detecting gene mutations (nucleotide substitutions, insertions/deletions) both at the germline and somatic level. The peculiar feature of FAMA is its ability to detect and localize mutations, by a redundant pattern of signals due to fluorescent DNA fragments generated by chemical cleavage. Moreover, previous data have demonstrated that normal contaminating DNA from stromal cells in the sample does not affect the sensitivity of the procedure, leading to the identification of the mutation even when the ratio mutant/normal allele is 10%. Results Eighteen mutations (12 missense, one nonsense, two deletions, three nucleotide substitutions at the level of the splice-junctions) and two polymorphisms were detected by FAMA in 17 patients (39%) and then confirmed by automated sequence analysis. Six of 18 mutations (33%) were not previously reported for colon cancer samples and two of 18 lesions (11%) were identified as novel p53 mutations. Conclusions Analytical scanning of the p53 gene by FAMA in DNA from colon cancer samples provides a sensitive, accurate and specific diagnostic procedure for routine clinical application.

Published
2006

32. Small beam dosimetry: A multi-center multi-detector italian project

Author

Talamonti, C., primary, Russo, S., additional, Barone, Tonghi L., additional, Benecchi, G., additional, Borzi, G., additional, Bresciani, S., additional, Cagni, E, additional, Carbonino, C., additional, Casale, M., additional, Clemente, S., additional, Consorti, R., additional, D’Alessio, V., additional, Dicastro, E., additional, Donofrio, G., additional, Falco, M.D., additional, Fedele, D., additional, Fiandra, C., additional, Frassanito, C., additional, Gasperi, C., additional, Giglioli, F.R., additional, Iervolino, C., additional, Infusino, E., additional, Linsalata, S., additional, Loi, G., additional, Lorenzini, E., additional, Marino, C., additional, Martinotti, S., additional, Masi, L., additional, Menghi, E., additional, Miceli, R., additional, Moretti, E., additional, Nardiello, B., additional, Nigro, R., additional, Pastore, G., additional, Pressello, M.C., additional, Pimpinella, M., additional, Raza, G., additional, Rosica, F., additional, Ruggeri, R., additional, Spiazzi, L., additional, Stasi, M., additional, Strigari, L., additional, Tremolada, V., additional, Vaiano, A., additional, Vigorito, S., additional, Villaggi, E., additional, Vittorini, F., additional, and Mancosu, P., additional

Published
2016
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35. Large and fast quantitation of proteins with SWATH-MS in a knockdown cell line

Author

Manfredi, M, Martinotti, S, Biffo, S, Mazzucco, E, Gosetti, F, Ranzato, E, Marengo, E, M. Manfredi, Simona Martinotti, S. Biffo, E. Mazzucco, F. Gosetti, E. Ranzato, E. Marengo, Manfredi, M, Martinotti, S, Biffo, S, Mazzucco, E, Gosetti, F, Ranzato, E, Marengo, E, M. Manfredi, Simona Martinotti, S. Biffo, E. Mazzucco, F. Gosetti, E. Ranzato, and E. Marengo

Published
2015

36. A polymorphism in the cyclooxygenase 2 gene as an inherited protective factor against myocardial infarction and stroke

Author

CIPOLLONE F, TONIATO E, MARTINOTTI S, FAZIA M, IEZZI A, CUCCURULLO C, PINI B, URSI S, VITULLO G, AVERNA, Maurizio, ARCA M, MONTALI A, CAMPAGNA F, UCCHINO S, SPIGONARDO F, TADDEI S, VIRDIS A, CIABATTONI G, NOTARBARTOLO A, CUCCURULLO F, MEZZETTI A, IDENTIFICATION OF NEW ELEMENTS OF PLAQUE STABILITY INES STUDY GROUP, CIPOLLONE F, TONIATO E, MARTINOTTI S, FAZIA M, IEZZI A, CUCCURULLO C, PINI B, URSI S, VITULLO G, AVERNA M, ARCA M, MONTALI A, CAMPAGNA F, UCCHINO S, SPIGONARDO F, TADDEI S, VIRDIS A, CIABATTONI G, NOTARBARTOLO A, CUCCURULLO F, MEZZETTI A, and IDENTIFICATION OF NEW ELEMENTS OF PLAQUE STABILITY INES STUDY GROUP

Subjects
Male, Pathology, Settore MED/09 - Medicina Interna, Arteriosclerosis, Carotid Stenosi, Myocardial Infarction, Infarction, Prostacyclin, Gastroenterology, Cohort Studies, Cerebrovascular Accident, rteriosclerosi, Risk Factors, Genotype, Medicine, Carotid Stenosis, Prospective Studies, Myocardial infarction, Membrane Protein, Stroke, biology, General Medicine, Middle Aged, Isoenzymes, Phenotype, Matrix Metalloproteinase 9, Matrix Metalloproteinase 2, Female, Human, medicine.drug, medicine.medical_specialty, Arteriosclerosi, Internal medicine, Diabetes mellitus, Humans, Polymorphism, Genetic, business.industry, C-reactive protein, Prostaglandin-Endoperoxide Synthase, Membrane Proteins, medicine.disease, Epoprostenol, Isoenzyme, Prospective Studie, Atheroma, Cyclooxygenase 2, Prostaglandin-Endoperoxide Synthases, biology.protein, Cohort Studie, business
Abstract

CONTEXT: Myocardial infarction (MI) and ischemic stroke are thought to be caused by matrix digestion by metalloproteinases (MMPs) leading to rupture of atherosclerotic plaques. Production of macrophage MMP-2 and MMP-9 is induced by cyclooxygenase 2 (COX-2) and prostaglandin E(2) synthesis. Although COX-2 expression may be genetically determined, the relation between COX-2 polymorphisms and the risk of MI and stroke is unclear. OBJECTIVE: To investigate the relationship between the -765G-->C polymorphism of the COX-2 gene and clinically evident plaque rupture. DESIGN, SETTING, AND PARTICIPANTS: Prospective, matched case-control study conducted between March 2002 and October 2003 among 864 patients with first MI or atherothrombotic ischemic stroke and 864 hospitalized controls. The groups were matched for age, sex, body mass index, smoking, hypertension, hypercholesterolemia, and diabetes. The -765G-->C variant of the COX-2 gene was genotyped by restriction endonuclease digestion of polymerase chain reaction products. MAIN OUTCOME MEASURES: Presence of the -765G-->C polymorphism of the COX-2 gene; COX-2, MMP-2, and MMP-9 expression and activity in plaques and in peripheral monocytes; urinary 6-keto PGF1alpha (marker of endothelial prostacyclin); and endothelium-dependent and -independent forearm blood flow vasodilation. RESULTS: The prevalence of -765GC was 2.41 times higher among controls than among cases (43.3% vs 17.9%; PC polymorphism did not affect endothelial prostacyclin biosynthesis or endothelium-dependent vasodilation in vivo. In subgroup analyses (n = 224 cases), serum high-sensitivity C-reactive protein was significantly lower in patients carrying the -765C allele (mean [SD], 0.78 [0.1] vs 2.56 [0.4] mg/L; P =.04). CONCLUSIONS: We found that the -765G-->C polymorphism of the COX-2 gene is associated with a decreased risk of MI and stroke. Detection of this genotype may be useful for predicting genetic risk of MI and stroke.

Published
2004

49. [Can analysis of the molecular status of the p53 gene contribute to improving the therapeutic strategy for breast carcinoma?]

Author

Enrico RICEVUTO, Marchetti P, Cannita K, De Galitiis F, Zc, Di Rocco, Tessitore A, Martella F, Bisegna R, Porzio G, Bafile A, Vicentini R, Resta V, Mattucci S, Ventura T, Martinotti S, Gp, Rubeis, and Ficorella C

Subjects
Drug Resistance, Neoplasm, Risk Factors, Lymphatic Metastasis, Cell Cycle, Humans, Apoptosis, Breast Neoplasms, Female, Tumor Suppressor Protein p53, Genes, p53, Prognosis, Case Management, Neoplasm Proteins
Abstract

The occurrence of mutations in the p53 tumor suppressor gene is a specific and recurring genetic event in solid tumors. P53 plays a pivotal role in multiple cellular processes such as cell growth control, DNA repair and programmed cell death. Genotoxic damage, also induced by chemotherapy or radiotherapy, induces p53 overexpression in order to control the rate of proliferating damaged cells, thus triggering the mismatch repair or apoptotic pathways. P53 inactivation determines a condition of genetic instability, justifying the subsequent susceptibility to acquire mutations of different other genes. P53 mutations are associated with worse prognosis and with chemo/radioresistance, due to the inability to trigger p53-dependent programmed cell death. Molecular diagnostic strategies show 32% p53 mutations in breast cancer. The analysis of the p53 gene performed by FAMA (Fluorescence Assisted Mismatch Analysis) in high-risk breast cancer patients withor = 10 involved axillary nodes may help identify a subset of very high risk BC patients (vHR-BC) with poorer prognosis and a subset with better prognosis, potentially responsive to medical treatments. The accurate evaluation of the p53 status can predict prognosis and sensitivity to chemotherapy, thus representing the first step toward better definition of therapeutic strategies according to the molecular characterization of the individual patient.

Published
2003

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