Your search keyword '"Trevisiol C."' showing total 14 results

1. Effect of Martensite Morphology on Tribological Behaviour of a Low-Alloy Steel.

Author

Trevisiol, C., Jourani, A., and Bouvier, S.

Published

2019

2. Analysis of DEFB1 regulatory SNPs in cystic fibrosis patients from North-Eastern Italy.

Author

Segat, L., Morgutti, M., Athanasakis, E., Trevisiol, C., Amaddeo, A., Poli, F., and Crovella, S.

Subjects

CYSTIC fibrosis, GENETIC disorders, PEPTIDES, GENETIC polymorphisms

Abstract

Cystic fibrosis (CF) transmembrane regulator protein (CFTR) gene is undoubtedly the main genetic factor involved in the modulation of CF phenotype. However, other factors such as human defensins and the genes encoding for these antimicrobial peptides have been hypothesized as possible modifiers influencing airways infection in CF patients, but their role in the pathogenesis of lung disease is still debated. Since DEFB1 gene encoding for human beta-defensin 1 displays features such as antimicrobial or chemotactic activity playing a role in inflammation, it has been considered as a possible candidate CF modifier gene. We analysed three single nucleotide polymorphisms (SNPs) in the 5′-untranslated region of the DEFB1 gene (namely g-52G>A, g-44C>G and g-20G>A) in a group of 62 CF patients from North Eastern Italy, and in 130 healthy controls, with the aim of verifying the possible association of these functional SNPs with the pulmonary phenotype of CF patients. DEFB1 SNPs have been genotyped by using Taqman allele-specific fluorescent probes and a real-time PCR platform. No significant differences were found for allele, genotype and haplotype frequencies of DEFB1 g-52G>A, g-44C>G and g-20G>A SNPs in CF patients stratified for Pseudomonas aeruginosa infection, as well as in patients with a severe and mild clinical phenotype or in patients stratified for CFTR genotypes. DEFB1 allele, genotype and haplotype frequencies of CF patients globally considered were similar to those of healthy controls. Our findings are discordant with respect to another recent study performed on CF patients coming from Southern Italy, probably due to different ethnicity of the patients. [ABSTRACT FROM AUTHOR]

Published

2010

3. Mass screening for coeliac disease using antihuman transglutaminase antibody assay.

Author

Tommasini A, Not T, Kiren V, Baldas V, Santon D, Trevisiol C, Berti I, Neri E, Geraduzzi T, Bruno I, Lenhardt A, Zamuner E, Spanò A, Crovella S, Martellossi S, Torre G, Sblattero D, Marzari R, Bradbury A, and Tamburlini G

Abstract

Aims: To determine coeliac disease prevalence by an anti-transglutaminase antibody assay in a large paediatric population; to evaluate acceptance of the screening programme, dietary compliance, and long term health effects.Methods: Cross-sectional survey of 3188 schoolchildren (aged 6-12) and prospective follow up of diagnosed cases. Main outcome measures were: prevalence of coeliac disease defined by intestinal biopsy or positivity to both human tissue transglutaminase and anti-endomysium antibodies in HLA DQ2-8 positive subjects; percentage of children whose families accepted screening; dietary compliance as defined by negativity for anti-transglutaminase antibodies; and presence of clinical or laboratory abnormalities at 24 month follow up.Results: The families of 3188/3665 children gave their consent (87%). Thirty biopsy proven coeliacs were identified (prevalence 1:106). Three other children testing positive for both coeliac related autoantibodies and HLA DQ2-8 but refusing biopsy were considered as having coeliac disease (prevalence 1:96). Of 33 cases, 12 had coeliac related symptoms. The 30 biopsy proven coeliacs followed a gluten-free diet. Of 28 subjects completing 18-24 months follow up, 20 (71.4%) were negative for anti-transglutaminase antibodies, while eight were slightly positive; symptoms resolved in all 12 symptomatic children.Conclusions: Prevalence of coeliac disease is high in Italian schoolchildren. Two thirds of cases were asymptomatic. Acceptance of the programme was good, as was dietary compliance. Given the high prevalence and possible complications of untreated coeliac disease, the availability of a valid screening method, and evidence of willingness to comply with dietary treatment population mass screening deserves careful consideration. [ABSTRACT FROM AUTHOR]

Published

2004

4. Mass screening for coeliac disease using antihuman transgulutaminase antibody assay.

Author

Tommasini, A., Not, T., Kiren, V., Baldas, V., Santon, D., Trevisiol, C., Berti, I., Neri, E., Gerarduzzi, T., Bruno, I., Lenhardt, A., Zamuner, E., Spanà, A., Crovella, S., Martellossi, S., Torre, G., Sblattero, D., Marzari, R., Bradbury, A., and Tamburlini, G.

Subjects

CELIAC disease, DIGESTIVE system diseases, MALABSORPTION syndromes, CLINICAL pathology, IMMUNOGLOBULINS, TRANSGLUTAMINASES

Abstract

Aims: To determine coeliac disease prevalence by an anti-transglutaminase antibody assay in a large paediatric population; to evaluate acceptance of the screening programme, dietary compliance, and long term health effects. Methods: Cross-sectional survey of 3188 schoolchildren (aged 6-12) and prospective follow up of diagnosed cases. Main outcome measures were: prevalence of coeliac disease defined by intestinal biopsy or positivity to both human tissue transglutaminase and anti-endomysium antibodies in HLA DQ2-8 positive subjects; percentage of children whose families accepted screening; dietary compliance as defined by negativity for anti-transglutaminase antibodies; and presence of clinical or laboratory abnormalities at 24 month follow up. Results: The families of 3188/3665 children gave their consent (87%). Thirty biopsy proven coeliacs were identified (prevalence 1:106). Three other children testing positive for both coeliac related autoantibodies and HLA DQ2-8 but refusing biopsy were considered as having coeliac disease (prevalence 1:96). Of 33 cases, 12 had coeliac related symptoms. The 30 biopsy proven coeliacs followed a gluten-free diet. Of 28 subjects completing 18-24 months follow up, 20 (71 .4%) were negative for anti-transglutaminase antibodies, while eight were slightly positive; symptoms resolved in all 12 symptomatic children. Conclusions: Prevalence of coeliac disease is high in Italian schoolchildren. Two thirds of cases were asymptomatic. Acceptance of the programme was good, us was dietary compliance. Given the high prevalence and possible complications of untreated coeliac disease, the availability of a valid screening method, and evidence of willingness to comply with dietary treatment population mass screening deserves careful consideration. [ABSTRACT FROM AUTHOR]

Published

2004

5. A Reliable Screening Procedure for Coeliac Disease in Clinical Practice.

Author

Trevisiol, C., Ventura, A., Baldas, V., Tommasini, A., Santon, D., Martelossi, S., Torre, G., Berti, I., Spanò, A., Crovella, S., Amoroso, A., Sblattero, D., Marzari, R., Bradbury, A., and Not, T.

Subjects

CELIAC disease diagnosis, MEDICAL screening

Abstract

Background: The main autoantigen recognized by the sera of patients with coeliac disease (CD) is tissue transglutaminase (tTG). A human-recombinant form of tTG was used to develop an ELISA to measure anti-tTG serum antibodies for the diagnosis of CD. Preliminary retrospective reports suggest that the human tTG-based ELISA could identify coeliac patients missed by the IgA-anti-endomysium antibody test (AEA). Whether the human recombinant tTG ELISA is sufficiently accurate to become the main diagnostic CD tool in everyday clinical practice is unknown. The objective was to determine, in a prospective study, the sensitivity and specificity of an ELISA test based on the use of human tTG compared with AEA, to analyse the discordant cases for HLA DQ2-8 and for clinical and intestinal biopsy characteristics. Methods: 1106 patients referred to a gastrointestinal outpatient clinic for symptoms attributable to CD, 52 first-degree relatives of CD patients and 200 healthy controls were tested for both anti-human tTG and AEA antibodies. Results: Out of 1158 subjects, 146 were tested positive for anti-tTG antibodies and 140 were biopsy-proven coeliacs. The AEA test identified 126/1158 coeliacs who also tested positive for anti-tTG antibodies. The 14 patients missed by the AEA test carried the typical HLA-DQ for CD; they had normal levels of total serum IgA and had milder pathology than those with both anti-tTG and AEA positivity (P < 0001). Conclusions: These results prove that human tTG-based ELISA is an excellent diagnostic tool for CD, for mass screening by both the specialist and the general clinic. [ABSTRACT FROM AUTHOR]

Published

2002

6. Undiagnosed coeliac disease and risk of autoimmune disorders in subjects with Type I diabetes mellitus.

Author

Not, T., Tommasini, A., Tonini, G., Buratti, E., Pocecco, M., Tortul, C., Valussi, M., Crichiutti, G., Berti, I., Trevisiol, C., Azzoni, E., Neri, E., Torre, G., Martelossi, S., Soban, M., Lenhardt, A., Cattin, L., and Ventura, A.

Subjects

CELIAC disease, PATIENTS, INSULIN, DIABETES, IMMUNOGLOBULINS, BIOPSY

Abstract

Aims/hypothesis. We tested the hypothesis that silent coeliac disease is more frequent than expected in both patients with Type I (insulin-dependent) diabetes mellitus and their first-degree relatives. We evaluated how the presence of other autoimmune disorders in diabetic patients and their first-degree relatives is related to silent, unrecognized coeliac disease. Methods. Sera from 491 subjects with Type I diabetes, 824 relatives and 4000 healthy control subjects were screened for anti-endomysial antibodies and all those subjects who tested positive for anti-endomysial antibodies underwent intestinal biopsy. Results. We found that the prevalence of coeliac disease was 5.7 % among the diabetic patients and 1.9 % among the relatives, values significantly higher than those found among the control subjects (p < 0.0001; p < 0.001). The prevalence of autoimmune disorders in diabetic patients with coeliac disease was significantly higher than in subjects with Type I diabetes alone (p < 0.0001). The prevalence of autoimmune disorders in the relatives with coeliac disease was significantly higher than in those who tested negative for anti-endomysial antibodies (p = 0.01). Conclusion/interpretation. This report provides further confirmation of the high prevalence of undiagnosed coeliac disease among diabetic patients and their relatives. This interesting new finding is the increased presence of other autoimmune diseases in these patients, as well as in their relatives with a delayed diagnosis for coeliac disease. Patients newly diagnosed with coeliac disease showed excellent compliance with the gluten-free diet. This should encourage policymakers to consider introducing an easy-to-use screening programme for diabetic patients and their relatives into everyday clinical practice, in order to prevent coeliac-associated symptoms and the onset of additional, more serious auto-immune disorders. [Diabetologia (2001) 44: 151–155] [ABSTRACT FROM AUTHOR]

Published

2001

7. Development of a novel rapid non-invasive screening test for coeliac disease.

Author

Baldas, V., Tommasini, A., Trevisiol, C., Berti, I., Fasano, A., Sblattero, D., Bradbury, A., Marzari, R., Barillari, G., Ventura, A., and Not, T.

Published

2000

8. Human Recombinant Tissue Transglutaminase ELISA: An Innovative Diagnostic Assay for Celiac Disease.

Author

Sblattero, D., Berti, I., Trevisiol, C., Marzari, R., Tommasini, A., Bradbury, A., Fasano, A., Ventura, A., and Not, T.

Subjects

ENZYME-linked immunosorbent assay, TRANSGLUTAMINASES, RECOMBINANT blood proteins, CELIAC disease, DIAGNOSIS of digestive system diseases

Abstract

OBJECTIVE: Tissue transglutaminase is the autoantigen recognized by the sera of celiac patients. An enzyme-linked immunosorbent assay (ELISA) based on guinea-pig tissue transglutaminase was recently used to measure serum tissue transglutaminase antibodies for the diagnosis of celiac disease. We determine the sensitivity and specificity of an ELISA test based on the use of human recombinant transglutaminase, compared with the guinea pig transglutaminase ELISA and IgA antiendomysium antibodies. METHODS: Serum samples were tested from 65 patients with intestinal biopsy proven celiac disease, from 10 patients with Crohn's disease, and from 150 healthy blood donors. RESULTS: Human transglutaminase ELISA identified 64 of 65 celiac patients, whereas the guinea pig transglulaminase ELISA and IgA antiendomysium antibodies identified 58 of 65 and 60 of 65 subjects, respectively. The three tests showed comparable specificity. CONCLUSIONS: These results proved that the human tissue transglutaminase-based ELISA represents a cost-effective strategy for identifying both symptomatic and atypical forms of celiac disease and could mean that intestinal biopsy need no longer be the gold standard for diagnosing this clinical condition. Furthermore, early identification and treatment of patients with celiac disease in an outpatient setting could have significant implications for reducing long-term morbidity and can produce major savings in future health care costs. [ABSTRACT FROM AUTHOR]

Published

2000

9. Usefulness of screening program for celiac disease in autoimmune thyroiditis.

Author

Berti, Irene, Trevisiol, Chiara, Tommasini, Alberto, Città, Angelo, Neri, Elena, Geatti, Onelio, Giammarini, Alberto, Ventura, Alessandro, Not, Tarcisio, Berti, I, Trevisiol, C, Tommasini, A, Città, A, Neri, E, Geatti, O, Giammarini, A, Ventura, A, and Not, T

Subjects

CELIAC disease diagnosis, IMMUNOGLOBULIN analysis, CELIAC disease complications, AUTOIMMUNE thyroiditis, FLUORESCENT antibody technique, MEDICAL screening, DISEASE complications

Abstract

We determined the prevalence of celiac disease in subjects with autoimmune thyroiditis compared with sick and healthy subjects. The screening was performed with IgA-class endomysium antibody, by indirect immunofluorescence using human umbilical cord as the antigenic substrate. Six of the 172 patients with autoimmune thyroiditis were found to be anti-endomysium positive (3.4%) and five of these underwent intestinal biopsy, which showed total villous atrophy. By contrast, 3 (0.75%) of 396 patients with nongastroenterologic malignancies and 10 (0.25%) of 4000 blood donors were found to have celiac disease. The prevalence of autoimmune diseases was significantly higher in patients with both celiac disease and autoimmune thyroiditis than in patients with autoimmune thyroiditis alone (P = 0.01). This study confirms that celiac disease is increased among patients with autoimmune thyroiditis. We suggest that these patients may benefit from screening for celiac disease so as to eliminate symptoms and limit the risk of developing other autoimmune disorders. [ABSTRACT FROM AUTHOR]

Published

2000

10. Serologic response to Bartonella henselae in patients with cat scratch disease and in sick and healthy children.

Author

Not, T, Canciani, M, Buratti, E, Dal Molin, G, Tommasini, A, Trevisiol, C, and Ventura, A

Subjects

IMMUNODIAGNOSIS, BARTONELLA infections, HODGKIN'S disease in children

Abstract

Indirect fluorescent antibody assay (IFA) is the most reliable test for detecting antibody to Bartonella henselae in the diagnosis of cat scratch disease (CSD). Recently, an ELISA test has been proposed, but conflicting results are reported. We compared IgG-IFA and IgG-IgM ELISA methods in CSD patients and in healthy children. We also tested ELISA specificity in a large group of healthy controls and in children with lymphoma-associated lymphadenopathy and with pyogenic lymphadenitis. The ELISA procedure was positive in 69/78 patients with CSD (sensitivity 89.6%), in 5/100 healthy children (specificity 95%), in 2/51 patients with non-Hodgkin's lymphoma or pyogenic lymphadenitis (specificity 96%) and in 27/296 blood donors (specificity 91.6%). In 34 patients with CSD, ELISA IgM and IgG responses decreased significantly between time of diagnosis of the disease and recovery. We found significantly higher IgG-ELISA titres in cat-owners, whether blood donors or healthy children, than in non-cat-owners. The IgG-IFA test gave positive results in 69/78 patients with CSD (sensitivity 89.6%) and in 5/62 healthy controls (specificity 92.5%). The ELISA method is a cheap, sensitive method for determining antibody response to Bartonella henselae infection and is also important for evaluating the clinical course of the disease and the efficacy of antibiotic therapy. The high specificity of ELISA in patients with non-Hodgkin's lymphoma will help the clinician to exclude a potentially life-threatening disease associated with lymphadenopathy. [ABSTRACT FROM AUTHOR]

Published

1999

11. P0424 CELIAC DISEASE (CD) IN A FRAME: CASE SERIES COLLECTED IN A PEDIATRIC DEPARTMENT IN THE LAST 25 YEARS.

Author

Gerarduzzi, T., Katsadorou, E., Biasotto, E., Giuseppin, I., Trevisiol, C., Verucci, E., Berti, I., Baldas, V., Martelossi, S., and Ventura, A.

Published

2004

12. HUMAN TISSUE TRANSGLUTAMINASE ELISA: A POWERFUL MASS SCREENING DIAGNOSTIC ASSAY FOR COELIAC DISEASE.

Author

Sblattero, D., Berti, I., Trevisiol, C., Marzari, R., Bradbury, A., Not, T., Fasano, A., and Ventura, A.

Published

1999

13. RAPID AND SIMPLE DOT IMMUNOBINDING ASSAY TO DETECT ANTI HUMAN-TRANSGLUTAMINASE ANTIBODIES IN COELIAC DISEASE.

Author

Not, T., Baldas, V., Tommasini, A., Trevisiol, C., Neri, E., Sblattero, D., Marzari, R., Bradbury, A., and Ventura, A.

Published

1999

14. PREVALENCE OF COELIAC DIESASE IN FIRST DEGREE RELATIVES OF NON-COELIAC INSULIN DEPENDENT DIABETES MELLITUS SUBJECTS.

Author

Not, T., Pocecco, M., Buratti, E., Cian, F., Tommasini, A., Città, A., Berti, I., Trevisiol, C., and Ventura, A.

Published

1998