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1. Metalloproteinases in Inflammatory Bowel Diseases

Author

Marônek M, Marafini I, Gardlík R, Link R, Troncone E, and Monteleone G

Subjects
tissue inhibitor of metalloproteinases, crohn’s disease, ulcerative colitis, intestinal inflammation, Pathology, RB1-214, Therapeutics. Pharmacology, RM1-950
Abstract

Martin Marônek,1,* Irene Marafini,2,* Roman Gardlík,1 René Link,3 Edoardo Troncone,2 Giovanni Monteleone2 1Institute of Molecular Biomedicine, Faculty of Medicine, Comenius University in Bratislava, Bratislava, 81108, Slovakia; 2Department of Systems Medicine, University of Rome “Tor Vergata”, Rome, 00133, Italy; 3Institute of Experimental Medicine, Faculty of Medicine, University of Pavol Jozef Šafárik, Košice, 040 11, Slovakia*These authors contributed equally to this workCorrespondence: Giovanni MonteleoneDipartimento di Medicina dei Sistemi, Università di Roma “Tor Vergata”, Via Montpellier 1, Rome, 00133, ItalyTel +39 06 20903702Fax +39 06 72596391Email Gi.Monteleone@Med.uniroma2.itAbstract: Inflammatory bowel diseases (IBD) are chronic inflammatory diseases of the gastrointestinal tract, encompassing two main disorders: Crohn’s disease (CD) and ulcerative colitis (UC). In both these pathologies, excessive and local immune response against luminal antigens promotes a pathological process leading to various degrees of gut damage. Matrix metalloproteinases (MMPs) are a family of neutral proteases with the ability to degrade all components of extracellular matrix. In physiological conditions, MMPs are produced at very low level and generally in the latent form and are involved in the normal tissue turnover. Their function is inhibited by tissue inhibitors of metalloproteinases (TIMPs). However, in inflamed tissue of IBD patients, MMPs are produced in excess and/or the activity of TIMPs is not sufficient to block MMPs, thereby making a major contribution to the IBD-related mucosal degradation. In this review, we summarize the available evidence on the expression and role of MMPs in IBD.Keywords: tissue inhibitor of metalloproteinases, Crohn’s disease, ulcerative colitis, intestinal inflammation

Published
2021

2. Therapeutic Oligonucleotides for Patients with Inflammatory Bowel Diseases

Author

Marafini I and Monteleone G

Subjects
crohn’s disease, ulcerative colitis, icam-1, smad7, Medicine (General), R5-920
Abstract

Irene Marafini, Giovanni Monteleone Department of Systems Medicine, University of Rome “Tor Vergata”, Rome, ItalyCorrespondence: Giovanni MonteleoneDipartimento di Medicina dei Sistemi, Università di Roma “Tor Vergata”, via Montpellier, 1, Rome 00133, ItalyTel +390620903702Fax +390672596391Email Gi.Monteleone@Med.uniroma2.itIntroduction: The better understanding of the molecular mechanisms, which drive the pathological process in the gut of patients with Crohn’s disease (CD) and patients with ulcerative colitis (UC), the major forms of inflammatory bowel diseases (IBD) in humans, has facilitated the development of novel therapeutic compounds. Among these, antisense oligonucleotides (ASOs) have been used to inhibit the expression of molecules, which sustain the IBD-associated mucosal inflammation.Areas Covered: In this short review, we summarize experimental and clinical data on the use of ASOs in IBD.Expert Opinion: Preclinical work indicates that the modulation of specific inflammatory pathways through the use of ASOs is highly effective and associates with low risk of adverse events. Initial clinical studies have confirmed the benefit of some ASOs even though no compound has yet reached the market. Further experimentation is warranted to establish the optimal route of administration for each ASO, ascertain whether and how long ASOs maintain their activity following administration, and identify which patient can benefit from specific ASO treatment.Keywords: Crohn’s disease, ulcerative colitis, ICAM-1, Smad7

Published
2020

3. Novel Therapeutic Options for People with Ulcerative Colitis: An Update on Recent Developments with Janus Kinase (JAK) Inhibitors

Author

Troncone E, Marafini I, Del Vecchio Blanco G, Di Grazia A, and Monteleone G

Subjects
inflammatory bowel disease, tofacitinib, jak/stat pathway, small molecule drugs, Diseases of the digestive system. Gastroenterology, RC799-869
Abstract

Edoardo Troncone, Irene Marafini, Giovanna Del Vecchio Blanco, Antonio Di Grazia, Giovanni Monteleone Department of Systems Medicine, University of Rome “Tor Vergata”, Rome, ItalyCorrespondence: Giovanni MonteleoneDipartimento di Medicina dei Sistemi, Università di Roma “Tor Vergata”, Via Montpellier, 1, Rome 00133, ItalyTel +390620903702Fax +390672596391Email Gi.Monteleone@Med.uniroma2.itAbstract: Crohn’s disease (CD) and ulcerative colitis (UC), the main forms of inflammatory bowel disease (IBD) in human beings, are chronic relapsing-remitting disorders of the gastrointestinal tract, which usually require lifelong therapies. For many years, IBD have been managed with corticosteroids, aminosalicylates and immunosuppressants (ie, thiopurines). The advent of biologic therapies (anti-TNF-α agents) has significantly improved the outcome of IBD patients in terms of prolonged clinical remission, corticosteroid sparing, achievement of mucosal healing and prevention of disease-related complications. Nevertheless, primary failure or loss of response to biologics occur in about 50% of patients treated with these drugs. Therefore, the need for new effective treatments for such patients has critically emerged as an urgent priority. With this regard, several small-molecule drugs (SMDs) targeting lymphocyte trafficking (ie, sphingosine-1-phosphate receptor modulators) and the JAK/STAT pathway (eg, tofacitinib) have been recently developed and tested in IBD. In particular, JAK inhibitors are oral compounds characterized by short half-life, low antigenicity and the ability to dampen several pro-inflammatory pathways simultaneously. Tofacitinib, a pan-JAK inhibitor, has shown good efficacy and safety in UC clinical trials and has been recently approved for the treatment of UC patients. In this review, we analyze the main evidence supporting the use of JAK inhibitors in UC and explore the unanswered questions about the use of this class of drug in UC.Keywords: inflammatory bowel disease, tofacitinib, JAK/STAT pathway, small molecule drugs

Published
2020

4. T.05.3: NEW OR RECURRENT CANCER IN INFLAMMATORY BOWEL DISEASE PATIENTS TREATED WITH IMMUNOMODULATORS OR BIOLOGICS AFTER CANCER

Author

Mancone, R., primary, Neri, B., additional, Fiorillo, M., additional, Moscardelli, A., additional, Galbusera, A., additional, Schiavone, S.C., additional, Festa, S., additional, Migliozzi, S., additional, Marafini, I., additional, Lolli, E., additional, Calabrese, E., additional, Monteleone, G., additional, and Biancone, L., additional

Published
2024
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5. OC.13.1: PREVENTABLE FACTORS OF POST-COLONOSCOPY COLORECTAL CANCER IN INFLAMMATORY BOWEL DISEASE PATIENTS

Author

De Cristofaro, E., primary, Sena, G., additional, Fiorillo, M., additional, Mancone, R., additional, Neri, B., additional, Marafini, I., additional, Lolli, E., additional, Zorzi, F., additional, Troncone, E., additional, Biancone, L., additional, Del Vecchio Blanco, G., additional, Calabrese, E., additional, and Monteleone, G., additional

Published
2024
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7. T.05.6: DEVELOPMENT OF AN IBD FRAILTY SCORE

Author

Marafini, I., primary, Salvatori, S., additional, Lavigna, D., additional, Brigida, M., additional, Di Venanzio, M., additional, Franchin, M., additional, Giannarelli, D., additional, Della Morte Canosci, D., additional, and Monteleone, G., additional

Published
2024
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13. An essential role of adenosine deaminase acting on RNA 1 in coeliac disease mucosa

Author

Di Fusco, D, Segreto, Mt, Iannucci, A, Maresca, C, Franzè, E, Di Maggio, G, Di Grazia, A, Boccanera, S, Laudisi, F, Marafini, I, Paoluzi, Oa, Michenzi, A, Monteleone, G, and Monteleone, I

Subjects
Immunology, Immunology and Allergy, dsRNA, virus, Settore MED/50, IFN, ADAR, celiac disease
Abstract

Background and aimType I interferons (IFNs) are highly expressed in the gut mucosa of celiac disease (CD) gut mucosa and stimulates immune response prompted by gluten ingestion, but the processes that maintain the production of these inflammatory molecules are not well understood. Adenosine deaminase acting on RNA 1 (ADAR1), an RNA-editing enzyme, plays a crucial role in inhibiting self or viral RNAs from activating auto-immune mediated responses, most notably within the type-I IFN production pathway. The aim of this study was to assess whether ADAR1 could contribute to the induction and/or progression of gut inflammation in patients with celiac disease.Material and methodsADAR1 expression was assessed by Real time PCR and Western blotting in duodenal biopsy taken from inactive and active celiac disease (CD) patients and normal controls (CTR). To analyze the role of ADAR1 in inflamed CD mucosa, lamina propria mononuclear cells (LPMC) were isolated from inactive CD and ADAR1 was silenced in with a specific antisense oligonucleotide (AS) and then incubated with a synthetic analogue of viral dsRNA (poly I:C). IFN-inducing pathways (IRF3, IRF7) in these cells were evaluated with Western blotting and inflammatory cytokines were evaluated with flow cytometry. Lastly, the role of ADAR1 was investigated in a mouse model of poly I:C-driven small intestine atrophy.ResultsReduced ADAR1 expression was seen in duodenal biopsies compared to inactive CD and normal controls. Ex vivo organ cultures of duodenal mucosal biopsies, taken from inactive CD patients, stimulated with a peptic-tryptic digest of gliadin displayed a decreased expression of ADAR1. ADAR1 silencing in LPMC stimulated with a synthetic analogue of viral dsRNA strongly boosted the activation of IRF3 and IRF7 and the production of type-I IFN, TNF-α and IFN-γ. Administration of ADAR1 antisense but not sense oligonucleotide to mice with poly I:C-induced intestinal atrophy, significantly increased gut damage and inflammatory cytokines production.ConclusionsThese data show that ADAR1 is an important regulator of intestinal immune homeostasis and demonstrate that defective ADAR1 expression could provide to amplifying pathogenic responses in CD intestinal mucosa.

Published
2023
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14. T.04.3 FREQUENCY AND RISK FACTORS FOR FRAILTY IN IBD PATIENTS

Author

Salvatori, S., primary, Neri, B., additional, Marafini, I., additional, Venuto, C., additional, Essofi, S., additional, Franchin, M., additional, De Cristofaro, E., additional, Lolli, E., additional, Zorzi, F., additional, Biancone, L., additional, Calabrese, E., additional, and Monteleone, G., additional

Published
2022
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15. OC.13.1 SMAD7 REGULATES IMMUNOGENIC DEATH PATHWAY IN COLORECTAL CANCER CELLS

Author

Maresca, C., primary, Stolfi, C., additional, Laudisi, F., additional, Di Grazia, A., additional, Di Fusco, D., additional, Franze´, E., additional, Congiu, D., additional, Marafini, I., additional, Salvatori, S., additional, Troncone, E., additional, Segreto, M.T., additional, Di Maggio, G., additional, Monteleone, I., additional, and Monteleone, G., additional

Published
2022
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16. OC.13.3 SMAD7 KNOCKDOWN REDUCES THE ACTIVATION OF STAT3 IN COLORECTAL CANCER

Author

Maresca, C., primary, Stolfi, C., additional, Laudisi, F., additional, Di Grazia, A., additional, Di Fusco, D., additional, Franze´, E., additional, Congiu, D., additional, Marafini, I., additional, Lolli, E., additional, De Cristofaro, E., additional, Guida, A.M., additional, Sica, G., additional, Monteleone, I., additional, and Monteleone, G., additional

Published
2022
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20. OC.06.5 GATA6 DEFICIENCY LEADS TO EPITHELIAL BARRIER DYSFUNCTION AND ENHANCES SUSCEPTIBILITY TO GUT INFLAMMATION

Author

Laudisi, F., primary, Stolfi, C., additional, Bevivino, G., additional, Maresca, C., additional, Franzè, E., additional, Troncone, E., additional, Lolli, E., additional, Marafini, I., additional, Pietrucci, D., additional, Teofani, A., additional, Di Grazia, A., additional, Di Fusco, D., additional, Colantoni, A., additional, Ortenzi, A., additional, Desideri, A., additional, Monteleone, I., additional, and Monteleone, G., additional

Published
2021
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21. Low prevalence of SARS-CoV-2 infection in inflammatory bowel disease

Author

Scucchi, L, Neri, B, Sarmati, L, Mossa, M, Sena, G, Massoud, R, Petruzziello, C, Musumeci, M, Marafini, I, Calabrese, E, Lolli, E, Bernardini, S, Andreoni, M, and Biancone, L

Subjects
SARS-CoV-2 infection, Seroprevalence, Inflammatory bowel disease, Settore MED/17, Asymptomatic
Published
2021

23. SARS-CoV-2 Igg seroprevalence in IBD patients treated with biologics: first vs. second pandemic wave in a prospective study.

Author

MOSSA, M., NERI, B., MONTESANO, L., SALVATORI, S., MARAFINI, I., SCUCCHI, L., LOLLI, E., MASSOUD, R., PETRUZZIELLO, C., BERNARDINI, S., CALABRESE, E., MONTELEONE, G., and BIANCONE, L.

Abstract

OBJECTIVE: In a prospective study, SARS-CoV-2 IgG seroprevalence was assessed during the second pandemic wave (W2) in a cohort of Inflammatory Bowel Disease (IBD) patients using biologics. The secondary aim was to compare, in the same cohort, the frequency of seropositivity and of COVID-19 during the second vs. the first (W1) wave. PATIENTS AND METHODS: From November 2020 to March 2021, SARS-CoV-2 IgG seropositivity and the prevalence of COVID-19 were assessed in a cohort of IBD patients using biologics already studied at W1. Inclusion criteria: age ≥ 18 years; diagnosis of IBD; follow-up; written consent. Exclusion criteria: SARS-CoV-2 vaccination. Risk factors for infection, compatible symptoms, history of infection or COVID-19, nasopharyngeal swab test were recorded. Data were expressed as median [range]. The X2 test, Student's t-test, logistic regression analysis was used. RESULTS: IBD cohort at W1 and W2 included 85 patients: 45 CD (52.9%), 40 UC (47.1%). When comparing the same 85 patients at W2 vs. W1, a higher SARS-CoV-2 seroprevalence at W2 was at the limit of the statistical significance (9.4% vs. 2.3%; p=0.05). The prevalence of COVID-19 at W2 vs. W1 was 3.5% (3/85) vs. 0% (0/85) (p=0.08). Contacts with COVID-19 patients and symptoms compatible with COVID-19 were more frequent at W2 vs. W1 (18.8 % vs. 0%; p=0.0001; 34.1% vs. 15.3%; p=0.004). At W2, history of contacts and new onset diarrhea were more frequent in seropositive patients [4/8 (50%) vs. 12/77 (15.6%); p=0.01 and 4/8 (50%) vs. 2/77 (2.6%); p=0.0001]. At W2, the risk factors for seropositivity included cough, fever, new onset diarrhea, rhinitis, arthromyalgia, dysgeusia/anosmia at univariate (p<0.05), but not at multivariate analysis. History of contacts was the only risk factor for seropositivity at univariate (p=0.03), but not at multivariate analysis (p=0.1). CONCLUSIONS: During W2, characterized by a high viral spread, IBD and biologics appeared not to increase the prevalence of SARS-CoV-2 infection or COVID-19 disease. New onset diarrhea mimicking IBD relapse may be observed in patients with SARS-CoV-2 infection. [ABSTRACT FROM AUTHOR]

Published
2022

25. OC.16.3 THE FRAGILE X MENTAL RETARDATION PROTEIN REGULATES RIP1K AND COLORECTAL CANCER RESISTANCE TO NECROPTOSIS

Author

Di Grazia, A., primary, Marafini, I., additional, Pedini, G., additional, Di Fusco, D., additional, Laudisi, F., additional, Dinallo, V., additional, Pacini, L., additional, Stolfi, C., additional, Franzè, E., additional, Sileri, P., additional, Sica, G., additional, Monteleone, G., additional, Bagni, C., additional, and Monteleone, I., additional

Published
2020
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28. OC.11.1 A NOVEL GENETIC VARIANT OF SMAD7 IS ASSOCIATED WITH CROHN'S DISEASE AND DOES NOT AFFECT THE EFFICACY OF SMAD7 ANTISENSE OLIGONUCLEOTIDE

Author

Di Fusco, D., primary, Marafini, I., additional, Stolfi, C., additional, Dinallo, V., additional, Laudisi, F., additional, Troncone, E., additional, Giuffrida, P., additional, Caprioli, F., additional, Ciccacci, C., additional, Borgiani, P., additional, Antonio, D.S., additional, Monteleone, I., additional, and Monteleone, G., additional

Published
2020
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30. OC.12.4 EXTENT OF MUCOSAL INFLAMMATION IN ULCERATIVE COLITIS INFLUENCES THE CLINICAL RESPONSE TO VEDOLIZUMAB

Author

Scarozza, P., primary, Laudisi, F., additional, Troncone, E., additional, Marafini, I., additional, Schmitt, H., additional, Lenti, M.V., additional, Costa, S., additional, Rocchetti, I., additional, De Cristofaro, E., additional, Salvatori, S., additional, Frezzati, L., additional, Di Sabatino, A., additional, Atreya, R., additional, Neurath, M.F., additional, and Monteleone, G., additional

Published
2020
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33. Low prevalence of SARS-CoV-2 infection in inflammatory bowel disease.

Author

SCUCCHI, L., NERI, B., SARMATI, L., MOSSA, M., SENA, G., MASSOUD, R., PETRUZZIELLO, C., MUSUMECI, M., MARAFINI, I., CALABRESE, E., LOLLI, E., BERNARDINI, S., ANDREONI, M., MONTELEONE, G., and BIANCONE, L.

Abstract

OBJECTIVE: Treatments used in Inflammatory Bowel Disease (IBD) have been associated with enhanced risk of viral infections and viral reactivation, however, it remains unclear whether IBD patients have increased risk of Severe Acute Respiratory Syndrome Coronavirus 2 (SARS-CoV-2) infection. The aim of the study was to examine the prevalence of SARSCoV-2 IgG positivity in IBD patients followed at our referral center. The role of treatments for IBD and risk factors for infection were also evaluated. PATIENTS AND METHODS: In a prospective study, all IBD patients followed at our referral centre between May 27th and July 21st, 2020 and fulfilling the inclusion criteria were tested for SARS-CoV-2 IgG. Specific IgG antibodies were evaluated by a commercial ELISA kit and SARSCoV-2 nasopharyngeal swab was performed in seropositive patients. RESULTS: Two-hundred and eighteen patients, 128 Crohn’s disease (CD) and 90 Ulcerative colitis (UC) [age 44, (19-77) years; ongoing biologics in 115 (52.7%)] were enrolled. No patient had major SARS-CoV-2-related symptoms. SARS-CoV-2 IgG were detected in 3 out of 218 (1.37%) patients with IBD (2 CD and 1 UC), all on biologics (2.6%). In all of the 3 seropositive patients, the nasopharyngeal swab was negative. There was no relationship between SARSCoV-2 seroprevalence and the demographic/ clinical characteristics of IBD patients. In contrast, history of recent travel was more frequent in the SARS-CoV-2 seropositive patients (2/3; 66.6%) than in SARS-CoV-2 seronegative patients [7/215 (3.25%); p<0.0001]. CONCLUSIONS: The prevalence of SARSCoV-2 IgG seropositivity in IBD patients appears to be comparable to the non-IBD population and not influenced by ongoing treatments. Risk factors for infection common to the general non-IBD population should be considered when managing patients with IBD. [ABSTRACT FROM AUTHOR]

Published
2021

35. INTERLEUKIN-34 INDUCES CC-CHEMOKINE LIGAND 20 IN GUT EPITHELIAL CELLS

Author

Franze E, Marafini I, De Simone V, Monteleone I, Caprioli F, Colantoni A, Ortenzi A, Crescenzi F, Sileri P, Sica G, Rossi P, Pallone F, Monteleone G, Franze, E, Marafini, I, De Simone, V, Monteleone, I, Caprioli, F, Colantoni, A, Ortenzi, A, Crescenzi, F, Sileri, P, Sica, G, Rossi, P, Pallone, F, and Monteleone, G

Published
2016

39. A FUNCTIONAL ROLE FOR IL-34 IN SUSTAINING INFLAMMATORY PATHWAYS IN IBD

Author

Franze E, Monteleone I, Stolfi C, Marafini I, Cupi ML, Caruso R, Caprioli F, Colantoni A, Ortenzi A, Sica G, Sileri P, Pallone F, Monteleone G, Franze, E, Monteleone, I, Stolfi, C, Marafini, I, Cupi, Ml, Caruso, R, Caprioli, F, Colantoni, A, Ortenzi, A, Sica, G, Sileri, P, Pallone, F, and Monteleone, G

Published
2014

40. Smad7 positively regulates keratinocyte proliferation in psoriasis

Author

Di Fusco, D., primary, Laudisi, F., additional, Dinallo, V., additional, Monteleone, I., additional, Di Grazia, A., additional, Marafini, I., additional, Troncone, E., additional, Colantoni, A., additional, Ortenzi, A., additional, Stolfi, C., additional, Picardo, M., additional, and Monteleone, G., additional

Published
2017
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