Your search keyword '"for G.R.O.U.P."' showing total 72 results

1. Serum S100B: A proxy marker for grey and white matter status in the absence and presence of (increased risk of) psychotic disorder?

Author

Christine van der Leeuw, Sanne Peeters, Ed Gronenschild, Stijn Michielse, Marcel Verbeek, Paul Menheere, Jim van Os, Machteld Marcelis, and Genetic Risk and Outcome in Psychosis (G.R.O.U.P.)

Subjects

Medicine, Science

Abstract

S100B is a protein with dose-dependent neurotrophic and neurotoxic effects. Whether S100B in psychotic disorder mirrors pathophysiological mechanisms (which elicit exacerbation of disease) or compensatory action is unclear, as is its validity as a proxy marker for brain status. Insight may be gained by examining associations between serum S100B and indices of grey (cortical thickness (CT)) and white matter (fractional anisotropy (FA)), in relation to the absence or presence of (increased risk of) psychotic disorder. Blood samples and cerebral magnetic resonance imaging (MRI) scans were acquired in 32 patients with psychotic disorder, 44 non-psychotic siblings of patients with psychotic disorder and 26 controls. Interactions between S100B and group were examined in separate models of CT and FA measures with multilevel regression analyses weighted for number of vertices and voxels (i.e. units of volume) respectively. All analyses were adjusted for sex, age, body mass index (BMI), scan sequence, handedness and highest level of education. Neither CT nor FA was associated with S100B. There were no significant S100B × group interactions (CT: χ2 = 0.044, p = 0.978; FA: χ2 = 3.672, p = 0.159). No evidence was present for S100B as a proxy marker of grey or white matter status. The association between S100B and brain measures was not moderated by psychosis risk.

Published

2017

2. No Evidence of Association between Childhood Urban Environment and Cortical Thinning in Psychotic Disorder.

Author

Aleida Frissen, Jim van Os, Petra Habets, Ed Gronenschild, Machteld Marcelis, and Genetic Risk and Outcome in Psychosis (G.R.O.U.P.)

Subjects

Medicine, Science

Abstract

BACKGROUNDThe alterations in cortical morphology, such as cortical thinning, observed in psychotic disorder, may be the outcome of interacting genetic and environmental effects. It has been suggested that urban upbringing may represent a proxy environmental effect impacting cortical thickness (CT). Therefore, the current study examined whether the association between group as a proxy genetic variable (patients with psychotic disorder [high genetic risk], healthy siblings of patients [intermediate risk] and healthy control subjects [average risk]) and CT was conditional on different levels of the childhood urban environment and whether this was sex-dependent.METHODST1-weighted MRI scans were acquired from 89 patients with a psychotic disorder, 95 non-psychotic siblings of patients with psychotic disorder and 87 healthy control subjects. Freesurfer software was used to measure CT. Developmental urban exposure was classified as low, medium, and high, reflecting the population density and the number of moves between birth and the 15th birthday, using data from the Dutch Central Bureau of Statistics and the equivalent database in Belgium. Multilevel regression analyses were used to examine the association between group, sex, and urban upbringing (as well as their interactions) and cortical CT as the dependent variable.RESULTSCT was significantly smaller in the patient group compared to the controls (B = -0.043, p CONCLUSIONThe negative association between (familial risk for) psychotic disorder and CT was not moderated by developmental urbanicity, suggesting that reduced CT is not the outcome of familial sensitivity to the proxy environmental factor 'urban upbringing'.

Published

2017

3. Vitamin D concentration and psychotic disorder

Author

C van der Ley, R.S. Kahn, A Stellinga, Machteld Marcelis, J. van Os, L.D. de Witte, C. van der Leeuw, for G.R.O.U.P., Richard Bruggeman, Clinical Cognitive Neuropsychiatry Research Program (CCNP), Psychiatrie & Neuropsychologie, RS: MHeNs - R2 - Mental Health, and MUMC+: Hersen en Zenuw Centrum (3)

Subjects

Adult, Male, medicine.medical_specialty, Clinical variables, D INSUFFICIENCY, SYMPTOMS, Urban Population, MIGRATION, Psychotic disorder, vitamin D, Gastroenterology, IMMIGRANTS, vitamin D deficiency, Young Adult, 03 medical and health sciences, D DEFICIENCY, 0302 clinical medicine, Risk Factors, Internal medicine, medicine, Vitamin D and neurology, Humans, INCREASED RISK, Applied Psychology, METAANALYSIS, Netherlands, Population Density, business.industry, MORTALITY, urbanicity, medicine.disease, Confidence interval, 030227 psychiatry, PREVALENCE, schizophrenia, Psychiatry and Mental health, Psychotic Disorders, Schizophrenia, Case-Control Studies, Etiology, Regression Analysis, Population study, Female, business, 030217 neurology & neurosurgery, Psychopathology

Abstract

BackgroundThe association between schizophrenia and decreased vitamin D levels is well documented. Low maternal and postnatal vitamin D levels suggest a possible etiological mechanism. Alternatively, vitamin D deficiency in patients with schizophrenia is presumably (also) the result of disease-related factors or demographic risk factors such as urbanicity.MethodsIn a study population of 347 patients with psychotic disorder and 282 controls, group differences in vitamin D concentration were examined. Within the patient group, associations between vitamin D, symptom levels and clinical variables were analyzed. Group × urbanicity interactions in the model of vitamin D concentration were examined. Both current urbanicity and urbanicity at birth were assessed.ResultsVitamin D concentrations were significantly lower in patients (B = −8.05; 95% confidence interval (CI) −13.68 to −2.42; p = 0.005). In patients, higher vitamin D concentration was associated with lower positive (B = −0.02; 95% CI −0.04 to 0.00; p = 0.049) and negative symptom levels (B = −0.03; 95% CI −0.05 to −0.01; p = 0.008). Group differences were moderated by urbanicity at birth (χ2 = 6.76 and p = 0.001), but not by current urbanicity (χ2 = 1.50 and p = 0.224). Urbanicity at birth was negatively associated with vitamin D concentration in patients (B = −5.11; 95% CI −9.41 to −0.81; p = 0.020), but not in controls (B = 0.72; 95% CI −4.02 to 5.46; p = 0.765).ConclusionsLower vitamin D levels in patients with psychotic disorder may in part reflect the effect of psychosis risk mediated by early environmental adversity. The data also suggest that lower vitamin D and psychopathology may be related through direct or indirect mechanisms.

Published

2020

4. Default mode network connectivity as a function of familial and environmental risk for psychotic disorder.

Author

Sanne C T Peeters, Vincent van de Ven, Ed H B M Gronenschild, Ameera X Patel, Petra Habets, Rainer Goebel, Jim van Os, Machteld Marcelis, and Genetic Risk and Outcome of Psychosis (G.R.O.U.P.)

Subjects

Medicine, Science

Abstract

BackgroundResearch suggests that altered interregional connectivity in specific networks, such as the default mode network (DMN), is associated with cognitive and psychotic symptoms in schizophrenia. In addition, frontal and limbic connectivity alterations have been associated with trauma, drug use and urban upbringing, though these environmental exposures have never been examined in relation to DMN functional connectivity in psychotic disorder.MethodsResting-state functional MRI scans were obtained from 73 patients with psychotic disorder, 83 non-psychotic siblings of patients with psychotic disorder and 72 healthy controls. Posterior cingulate cortex (PCC) seed-based correlation analysis was used to estimate functional connectivity within the DMN. DMN functional connectivity was examined in relation to group (familial risk), group × environmental exposure (to cannabis, developmental trauma and urbanicity) and symptomatology.ResultsThere was a significant association between group and PCC connectivity with the inferior parietal lobule (IPL), the precuneus (PCu) and the medial prefrontal cortex (MPFC). Compared to controls, patients and siblings had increased PCC connectivity with the IPL, PCu and MPFC. In the IPL and PCu, the functional connectivity of siblings was intermediate to that of controls and patients. No significant associations were found between DMN connectivity and (subclinical) psychotic/cognitive symptoms. In addition, there were no significant interactions between group and environmental exposures in the model of PCC functional connectivity.DiscussionIncreased functional connectivity in individuals with (increased risk for) psychotic disorder may reflect trait-related network alterations. The within-network "connectivity at rest" intermediate phenotype was not associated with (subclinical) psychotic or cognitive symptoms. The association between familial risk and DMN connectivity was not conditional on environmental exposure.

Published

2015

5. Bone Mineral Density as a Marker of Cumulative Estrogen Exposure in Psychotic Disorder: A 3 Year Follow-Up Study.

Author

Christine van der Leeuw, Sanne Peeters, Patrick Domen, Marinus van Kroonenburgh, Jim van Os, Machteld Marcelis, and Genetic Risk and Outcome in Psychosis (G.R.O.U.P.)

Subjects

Medicine, Science

Abstract

Altered estrogen-induced neuroprotection has been implicated in the etiology of psychotic disorders. Using bone mineral density as a marker of lifetime estrogen exposure, a longitudinal family study was conducted to discriminate between etiological mechanisms and secondary effects of disease and treatment. Dual X-ray absorptiometry scans were acquired twice, with an interval of 3 years, in 30 patients with psychotic disorder (male (M)/female (F): 24/6, mean age of 32 years at second measurement), 44 non-psychotic siblings of patients with a psychotic disorder (M/F: 26/18, mean age 32) and 27 controls (M/F: 7/20, mean age 35). Total bone mineral density, Z-scores and T-scores were measured in the lumbar spine and proximal femur. Associations between group and bone mineral density changes were investigated with multilevel random regression analyses. The effect of prolactin-raising antipsychotic medication was evaluated. (Increased risk of) psychotic disorder was not associated with disproportionate bone mineral density loss over a three year period. Instead, femoral bone mineral density measures appeared to decrease less in the patient versus control comparison (total BMD: B = 0.026, 95% CI 0.002 to 0.050, p = 0.037; Z-score: B = 0.224, 95% CI 0.035 to 0.412, p = 0.020; and T-score: B = 0.193, 95% CI 0.003 to 0.382, p = 0.046). Current or past use of a prolactin-raising antipsychotic medication was not associated with bone mineral density changes. In this small longitudinal study, there was no evidence of ongoing estrogen deficiency in psychotic disorder as there was no excessive loss of bone mineral density over a 3-year period in patients using antipsychotic medication.

Published

2015

6. Brain-derived neurotrophic factor/FK506-binding protein 5 genotype by childhood trauma interactions do not impact on hippocampal volume and cognitive performance.

Author

Dennis Hernaus, Ruud van Winkel, Ed Gronenschild, Petra Habets, Gunter Kenis, Machteld Marcelis, Jim van Os, Inez Myin-Germeys, Dina Collip, and for Genetic Risk and Outcome in Psychosis (G.R.O.U.P.)

Subjects

Medicine, Science

Abstract

In the development of psychotic symptoms, environmental and genetic factors may both play a role. The reported association between childhood trauma and psychotic symptoms could therefore be moderated by single nucleotide polymorphisms (SNPs) associated with the stress response, such as FK506-binding protein 5 (FKBP5) and brain-derived neurotrophic factor (BDNF). Recent studies investigating childhood trauma by SNP interactions have inconsistently found the hippocampus to be a potential target underlying these interactions. Therefore, more detailed modelling of these effects, using appropriate covariates, is required. We examined whether BDNF/FKBP5 and childhood trauma interactions affected two proxies of hippocampal integrity: (i) hippocampal volume and (ii) cognitive performance on a block design (BD) and delayed auditory verbal task (AVLT). We also investigated whether the putative interaction was different for patients with a psychotic disorder (n = 89) compared to their non-psychotic siblings (n = 95), in order to elicit possible group-specific protective/vulnerability effects. SNPs were rs9296158, rs4713916, rs992105, rs3800373 (FKBP5) and rs6265 (BDNF). In the combined sample, no BDNF/FKBP5 by childhood trauma interactions were apparent for either outcome, and BDNF/FKBP5 by childhood trauma interactions were not different for patients and siblings. The omission of drug use and alcohol consumption sometimes yielded false positives, greatly affected explained error and influenced p-values. The consistent absence of any significant BDNF/FKBP5 by childhood trauma interactions on assessments of hippocampal integrity suggests that the effect of these interactions on psychotic symptoms is not mediated by hippocampal integrity. The importance of appropriate statistical designs and inclusion of relevant covariates should be carefully considered.

Published

2014

7. Replicated evidence of absence of association between serum S100B and (risk of) psychotic disorder.

Author

Christine van der Leeuw, Machteld Marcelis, Sanne C T Peeters, Marcel M Verbeek, Paul P C A Menheere, Lieuwe de Haan, Jim van Os, Nico J M van Beveren, and Genetic Risk and Outcome in Psychosis (G.R.O.U.P.)

Subjects

Medicine, Science

Abstract

BACKGROUND: S100B is a potential marker of neurological and psychiatric illness. In schizophrenia, increased S100B levels, as well as associations with acute positive and persisting negative symptoms, have been reported. It remains unclear whether S100B elevation, which possibly reflects glial dysfunction, is the consequence of disease or compensatory processes, or whether it is an indicator of familial risk. METHODS: Serum samples were acquired from two large independent family samples (n = 348 and n = 254) in the Netherlands comprising patients with psychotic disorder (n = 140 and n = 82), non-psychotic siblings of patients with psychotic disorder (n = 125 and n = 94) and controls (n = 83 and n = 78). S100B was analyzed with a Liaison automated chemiluminescence system. Associations between familial risk of psychotic disorder and S100B were examined. RESULTS: Results showed that S100B levels in patients (P) and siblings (S) were not significantly different from controls (C) (dataset 1: P vs. C: B = 0.004, 95% CI -0.005 to 0.013, p = 0.351; S vs. C: B = 0.000, 95% CI -0.009 to 0.008, p = 0.926; and dataset 2: P vs. C: B = 0.008, 95% CI -0.011 to 0.028, p = 0.410; S vs. C: B = 0.002, 95% CI -0.016 to 0.021, p = 0.797). In patients, negative symptoms were positively associated with S100B (B = 0.001, 95% CI 0.000 to 0.002, p = 0.005) in one of the datasets, however with failure of replication in the other. There was no significant association between S100B and positive symptoms or present use or type of antipsychotic medication. CONCLUSIONS: S100B is neither an intermediate phenotype, nor a trait marker for psychotic illness.

Published

2013

8. Vitamin D concentration and psychotic disorder: Associations with disease status, clinical variables and urbanicity

Author

Psychiatrie_Medisch, Onderzoeksgroep 11, Brain, Hersenen-Medisch 1, for G.R.O.U.P., Psychiatrie_Medisch, Onderzoeksgroep 11, Brain, Hersenen-Medisch 1, and for G.R.O.U.P.

Published

2020

9. Microstructural white matter network-connectivity in individuals with psychotic disorder, unaffected siblings and controls

Author

for Genetic Risk and Outcome of Psychosis (G.R.O.U.P.)

Subjects

Connectivity, Neurology, Radiology Nuclear Medicine and imaging, Siblings, Cognitive Neuroscience, White matter, Schizophrenia, Clinical Neurology, Journal Article, Efficiency, Clustering

Abstract

Background: Altered structural network-connectivity has been reported in psychotic disorder but whether these alterations are associated with genetic vulnerability, and/or with phenotypic variation, has been less well examined. This study examined i) whether differences in network-connectivity exist between patients with psychotic disorder, siblings of patients with psychotic disorder and controls, and ii) whether network-connectivity alterations vary with (subclinical) symptomatology. Methods: Network-connectivity measures (global efficiency (GE), density, local efficiency (LE), clustering coefficient (CC)) were derived from diffusion weighted imaging (DWI) and were compared between 85 patients with psychotic disorder, 93 siblings without psychotic disorder and 80 healthy comparison subjects using multilevel regression models. In patients, associations between Positive and Negative Syndrome Scale (PANSS) symptoms and topological measures were examined. In addition, interactions between subclinical psychopathology and sibling/healthy comparison subject status were examined in models of topological measures. Results: While there was no main effect of group with respect to GE, density, LE and CC, siblings had a significantly higher CC compared to patients (B = 0.0039, p =.002). In patients, none of the PANSS symptom domains were significantly associated with any of the four network-connectivity measures. The two-way interaction between group and SIR-r positive score in the model of LE was significant (χ2 = 6.24, p =.01, df = 1). In the model of CC, the interactions between group and respectively SIS-r positive (χ2 = 5.59, p =.02, df = 1) and negative symptom scores (χ2 = 4.71, p =.03, df = 1) were significant. Stratified analysis showed that, in siblings, decreased LE and CC was significantly associated with increased SIS-r positive scores (LE: B = −0.0049, p =.003, CC: B = −0.0066, p =.01) and that decreased CC was significantly associated with increased SIS-r negative scores (B = −0.012, p =.003). There were no significant interactions between group and SIS-r scores in the models of GE and density. Conclusion: The findings indicate absence of structural network-connectivity alterations in individuals with psychotic disorder and in individuals at higher than average genetic risk for psychotic disorder, in comparison with healthy subjects. The differential subclinical symptom-network connectivity associations in siblings with respect to controls may be a sign of psychosis vulnerability in the siblings.

Published

2019

10. Childhood trauma- and cannabis-associated microstructural white matter changes in patients with psychotic disorder : a longitudinal family-based diffusion imaging study

Author

Domen, Patrick, Michielse, Stijn, Peeters, Sanne, Viechtbauer, Wolfgang, van Os, Jim, Marcelis, Machteld, for Genetic Risk and Outcome of Psychosis (G.R.O.U.P.), Domen, Patrick, Michielse, Stijn, Peeters, Sanne, Viechtbauer, Wolfgang, van Os, Jim, Marcelis, Machteld, and for Genetic Risk and Outcome of Psychosis (G.R.O.U.P.)

Published

2019

11. Microstructural white matter network-connectivity in individuals with psychotic disorder, unaffected siblings and controls

Author

MS Verloskunde, UMC Utrecht, Hersenen-Medisch 1, Brain, for Genetic Risk and Outcome of Psychosis (G.R.O.U.P.), MS Verloskunde, UMC Utrecht, Hersenen-Medisch 1, Brain, and for Genetic Risk and Outcome of Psychosis (G.R.O.U.P.)

Published

2019

12. Childhood trauma- and cannabis-associated microstructural white matter changes in patients with psychotic disorder: a longitudinal family-based diffusion imaging study

Author

Hersenen-Medisch 1, Brain, Onderzoek, Domen, Patrick, Michielse, Stijn, Peeters, Sanne, Viechtbauer, Wolfgang, van Os, Jim, Marcelis, Machteld, for Genetic Risk and Outcome of Psychosis (G.R.O.U.P.), Hersenen-Medisch 1, Brain, Onderzoek, Domen, Patrick, Michielse, Stijn, Peeters, Sanne, Viechtbauer, Wolfgang, van Os, Jim, Marcelis, Machteld, and for Genetic Risk and Outcome of Psychosis (G.R.O.U.P.)

Published

2019

13. Remission criteria and functional outcome in patients with schizophrenia, a longitudinal study

Author

G.R.O.U.P investigators, Mayke Janssens, Neeltje E.M. van Haren, Lindy-Lou Boyette, Henriette D. Heering, Psychiatry, Psychiatrie & Neuropsychologie, RS: MHeNs - R2 - Mental Health, Klinische Psychologie (Psychologie, FMG), Faculteit der Geneeskunde, Other departments, ANS - Amsterdam Neuroscience, and Adult Psychiatry

Subjects

Adult, Male, Pediatrics, medicine.medical_specialty, Longitudinal study, Remission criteria, Research Support, Outcome (game theory), functional outcome, Young Adult, Quality of life, Adaptation, Psychological, Outcome Assessment, Health Care, medicine, Journal Article, Humans, COHORT, Longitudinal Studies, MENTAL-ILLNESS, Non-U.S. Gov't, Research Support, Non-U.S. Gov't, Remission Induction, General Medicine, RECOVERY, medicine.disease, Mental illness, schizophrenia, Psychiatry and Mental health, Schizophrenia, Cohort, Quality of Life, Female, Schizophrenic Psychology, Psychology, Psychopathology, Clinical psychology

Abstract

Background: The Remission in Schizophrenia Working Group (RSWG) has proposed remission criteria for schizophrenia, which were shown to be valid in terms of functional and clinical outcomes. However, studies investigating the association between dynamics in remission status in relation to longitudinal functional and clinical outcome are scarce. Methods: A total of 648 patients were allocated to four change-in-remission groups, i.e. remission/remission, remission/no-remission, no-remission/remission, and no-remission/no-remission. Remission status was based on PANSS ratings. Multilevel linear modelling techniques were used to investigate whether enduring remission was associated with more improvement in functional outcome at follow-up. Further, change in functional and clinical outcome at follow-up measurement was assessed for each remission category separately. Results: Both at baseline and at follow-up, remission status was associated with better functioning. At baseline, patients who subsequently moved out of remission status could be characterized by more severe psychopathology, disabilities, unmet needs and worse quality of life (QoL) compared with patients who continued to be in remission. The stable in-remission group was characterized by significantly better functioning and QoL, both at baseline and follow-up compared with all other remission groups. Nevertheless, QoL increased in all four patient categories. Conclusions: In a large sample of patients with a non-affective psychotic disorder, stable remission or moving into remission over time, based on the RSWG criteria, was associated with a favourable functional outcome and QoL, providing further support for the clinical validity of the RSWG remission criteria. The findings also suggest growing adaptation and self-management over time, despite ongoing difficulties.

Published

2015

14. Reduced specialized processing in psychotic disorder : a graph theoretical analysis of cerebral functional connectivity

Author

Peeters, Sanne C T, Gronenschild, Ed H B M, van Amelsvoort, Therese, van Os, Jim, Marcelis, Machteld, Kahn, Rene, Wiersma, Durk, Bruggeman, Richard, Cahn, Wiepke, de Haan, Lieuwe, Meijer, Carin, Myin-Germeys, Inez, and Genetic Risk and Outcome of Psychosis (G.R.O.U.P.)

Subjects

Brain connectomics, graph theory, psychotic disorders, Journal Article, functional magnetic resonance imaging, siblings

Abstract

BACKGROUND: Previous research has shown that the human brain can be represented as a complex functional network that is characterized by specific topological properties, such as clustering coefficient, characteristic path length, and global/local efficiency. Patients with psychotic disorder may have alterations in these properties with respect to controls, indicating altered efficiency of network organization. This study examined graph theoretical changes in relation to differential genetic risk for the disorder and aimed to identify clinical correlates. METHODS: Anatomical and resting-state MRI brain scans were obtained from 73 patients with psychotic disorder, 83 unaffected siblings, and 72 controls. Topological measures (i.e., clustering coefficient, characteristic path length, and small-worldness) were used as dependent variables in a multilevel random regression analysis to investigate group differences. In addition, associations with (subclinical) psychotic/cognitive symptoms were examined. RESULTS: Patients had a significantly lower clustering coefficient compared to siblings and controls, with no difference between the latter groups. No group differences were observed for characteristic path length and small-worldness. None of the topological properties were associated with (sub)clinical psychotic and cognitive symptoms. CONCLUSIONS: The reduced ability for specialized processing (reflected by a lower clustering coefficient) within highly interconnected brain regions observed in the patient group may indicate state-related network alterations. There was no evidence for an intermediate phenotype and no evidence for psychopathology-related alterations.

Published

2016

15. Interobserver reproducibility in pathologist interpretation of columnar-lined esophagus

Author

Interobserver reproducibility in pathologist interpretation of columnar lined e.s.o.p.h.a.g.u.s. Mastracci L1, 2, Piol N3, 4, Molinaro L5, Pitto F3, Tinelli C6, De Silvestri A6, Fiocca R3, Grillo F3, ABRAM Study G.r.o.u.p. Collaborators Alò P, Al Omoush TM, Asioli S, Buffelli F, Conforti F, Cornaggia M, Cossu S, De Marco L, Fiocca R, Foscolo AM, Fraternali Orcioni G, Ingravallo G, Locatelli F, Luinetti O, Marchio C, Montinari E, Melchiorri L, Messerini L, Migliora P, Pizzi M, Rugge M, Saragoni L, Tamponi E, Tomezzoli A, Trisolini MP, Trombatore M, Vanoli A, Vellone VG, Villanacci V., D'ARMIENTO, FRANCESCO PAOLO, Mastracci L1, Interobserver reproducibility in pathologist interpretation of columnar lined e. s. o. p. h. a. g. u. s., Piol, N3, Molinaro, L5, Pitto, F3, Tinelli, C6, De Silvestri, A6, Fiocca, R3, Grillo, F3, Collaborators Alò P, ABRAM Study G. r. o. u. p., Al Omoush, Tm, Asioli, S, Buffelli, F, Conforti, F, Cornaggia, M, Cossu, S, D'Armiento, FRANCESCO PAOLO, De Marco, L, Fiocca, R, Foscolo, Am, Fraternali Orcioni, G, Ingravallo, G, Locatelli, F, Luinetti, O, Marchio, C, Montinari, E, Melchiorri, L, Messerini, L, Migliora, P, Pizzi, M, Rugge, M, Saragoni, L, Tamponi, E, Tomezzoli, A, Trisolini, Mp, Trombatore, M, Vanoli, A, Vellone, Vg, and Villanacci, V.

Subjects

Adult, medicine.medical_specialty, Barrett’s esophagu, Esophageal Neoplasms, Concordance, Biopsy, Epithelium, Pathology and Forensic Medicine, 03 medical and health sciences, Barrett Esophagus, 0302 clinical medicine, Esophagus, Metaplasia, Histological diagnosi, Interobserver variation, Medicine, Barrett’s esophagus, Humans, Molecular Biology, Aged, medicine.diagnostic_test, business.industry, Medicine (all), Columnar-lined esophagus, Histological diagnosis, Middle Aged, Reproducibility of Results, Intestinal metaplasia, General Medicine, Anatomy, Cell Biology, medicine.disease, Endoscopy, medicine.anatomical_structure, 2734, 030220 oncology & carcinogenesis, Barrett's esophagus, 030211 gastroenterology & hepatology, Radiology, medicine.symptom, business, Kappa, Columnar-lined esophagu

Abstract

Confirmation of endoscopically suspected esophageal metaplasia (ESEM) requires histology, but confusion in the histological definition of columnar-lined esophagus (CLE) is a longstanding problem. The aim of this study is to evaluate interpathologist variability in the interpretation of CLE. Thirty pathologists were invited to review three ten-case sets of CLE biopsies. In the first set, the cases were provided with descriptive endoscopy only; in the second and the third sets, ESEM extent using Prague criteria was provided. Moreover, participants were required to refer to a diagnostic chart for evaluation of the third set. Agreement was statistically assessed using Randolph's free-marginal multirater kappa. While substantial agreement in recognizing columnar epithelium (K = 0.76) was recorded, the overall concordance in clinico-pathological diagnosis was low (K = 0.38). The overall concordance rate improved from the first (K = 0.27) to the second (K = 0.40) and third step (K = 0.46). Agreement was substantial when diagnosing Barrett's esophagus (BE) with intestinal metaplasia or inlet patch (K = 0.65 and K = 0.89), respectively, in the third step, while major problems in interpretation of CLE were observed when only cardia/cardia-oxyntic atrophic-type epithelium was present (K = 0.05-0.29). In conclusion, precise endoscopic description and the use of a diagnostic chart increased consistency in CLE interpretation of esophageal biopsies. Agreement was substantial for some diagnostic categories (BE with intestinal metaplasia and inlet patch) with a well-defined clinical profile. Interpretation of cases with cardia/cardia-oxyntic atrophic-type epithelium, with or without ESEM, was least consistent, which reflects lack of clarity of definition and results in variable management of this entity.

Published

2016

16. Identification of a 3-gene model as a powerful diagnostic tool for the recognition of ALK-negative anaplastic large-cell lymphoma

Author

Agnelli L., Mereu E., Pellegrino E., Limongi T., Kwee I., Bergaggio E., Ponzoni M., Zamò A., Iqbal J., Neri A., Chan W. C., Bertoni F., Inghirami G., Piva R., European T. Cell Lymphoma Study G.r.o.u.p. Barreca A., Cuccuru G., Medico E., Spaccarotella E., Scarfò I., Fornari A., Ferreri C., Novero D., Chilosi M., Facchetti F., Lonardi S., De Chiara A., Fulciniti F., Doglioni C., Todoerti K., Falini B., Tiacci E., Van Loo P., Tousseyn T., De Wolf Peeters C., Geissinger E., Muller Hermelink H. K., Rosenwald A., Piris M. A., Rodriguez M. E., Boi M., PICCALUGA, PIER PAOLO, PILERI, STEFANO, AGOSTINELLI, CLAUDIO, Agnelli L., Mereu E., Pellegrino E., Limongi T., Kwee I., Bergaggio E., Ponzoni M., Zamò A., Iqbal J., Piccaluga P.P., Neri A., Chan W.C., Pileri S., Bertoni F., Inghirami G., Piva R., European T-Cell Lymphoma Study Group. Barreca A., Cuccuru G., Medico E., Spaccarotella E., Scarfò I., Fornari A., Ferreri C., Novero D., Chilosi M., Facchetti F., Lonardi S., De Chiara A., Fulciniti F., Doglioni C., Todoerti K., Agostinelli C., Falini B., Tiacci E., Van Loo P., Tousseyn T., De Wolf-Peeters C., Geissinger E., Muller-Hermelink H.K., Rosenwald A., Piris M.A., Rodriguez M.E., Boi M., Agnelli, L, Mereu, E, Pellegrino, E, Limongi, T, Kwee, I, Bergaggio, E, Ponzoni, Maurilio, Zamo, A, Iqbal, J, Piccaluga, Pp, Neri, A, Chan, Wc, Pileri, S, Bertoni, F, Inghirami, G, Piva, R, European T., Cell Lymphoma Study Grp, and Doglioni, Claudio

Subjects

Lymphoma, Bioinformatics, Adult, Biomarkers, Tumor, Case-Control Studies, Diagnosis, Differential, Gene Expression Profiling, Gene Expression Regulation, Neoplastic, Humans, Lymphoma, Large-Cell, Anaplastic, Microarray Analysis, Models, Statistical, Molecular Diagnostic Techniques, Predictive Value of Tests, Prognosis, Receptor Protein-Tyrosine Kinases, Genes, Neoplasm, Immunology, Biochemistry, Hematology, Cell Biology, GENE-EXPRESSION ANALYSIS, Models, hemic and lymphatic diseases, PERIPHERAL T-CELL, Diagnosis, Anaplastic, Anaplastic lymphoma kinase, Anaplastic Lymphoma Kinase, Anaplastic large-cell lymphoma, Tumor, Not Otherwise Specified, Statistical, CANCER, Large-Cell, NEOPLASMS, Computational biology, ABERRATIONS, PROFILE, CLASSIFICATION, HODGKIN-LYMPHOMA, KINASE, medicine, TRANSLOCATIONS, Neoplastic, business.industry, Microarray analysis techniques, Large cell, medicine.disease, Gene expression profiling, Gene Expression Regulation, Genes, Differential, Neoplasm, Differential diagnosis, business, Biomarkers

Abstract

Anaplastic large-cell lymphomas (ALCLs) are a group of clinically and biologically heterogeneous diseases including the ALK(+) and ALK(-) systemic forms. Whereas ALK(+) ALCLs are molecularly characterized and can be readily diagnosed, specific immunophenotypic or genetic features to define ALK(-) ALCL are missing, and their distinction from other T-cell non-Hodgkin lymphomas (T-NHLs) remains controversial. In the present study, we undertook a transcriptional profiling meta-analysis of 309 cases, including ALCL and other primary T-NHL samples. Pathway discovery and prediction analyses defined a minimum set of genes capable of recognizing ALK(-) ALCL. Application of quantitative RT-PCR in independent datasets from cryopreserved and formalin-fixed paraffin-embedded samples validated a 3-gene model (TNFRSF8, BATF3, and TMOD1) able to successfully separate ALK(-) ALCL from peripheral T-cell lymphoma not otherwise specified, with overall accuracy near 97%. In conclusion, our data justify the possibility of translating quantitative RT-PCR protocols to routine clinical settings as a new approach to objectively dissect T-NHL and to select more appropriate therapeutic protocols. (Blood. 2012;120(6):1274-1281) Anaplastic large-cell lymphomas (ALCLs) are a group of clinically andbiologically heterogeneous diseases including the ALK(+) and ALK(-) systemicforms. Whereas ALK(+) ALCLs are molecularly characterized and can be readilydiagnosed, specific immunophenotypic or genetic features to define ALK(-) ALCLare missing, and their distinction from other T-cell non-Hodgkin lymphomas(T-NHLs) remains controversial. In the present study, we undertook atranscriptional profiling meta-analysis of 309 cases, including ALCL and otherprimary T-NHL samples. Pathway discovery and prediction analyses defined aminimum set of genes capable of recognizing ALK(-) ALCL. Application ofquantitative RT-PCR in independent datasets from cryopreserved and formalin-fixedparaffin-embedded samples validated a 3-gene model (TNFRSF8, BATF3, and TMOD1)able to successfully separate ALK(-) ALCL from peripheral T-cell lymphoma nototherwise specified, with overall accuracy near 97%. In conclusion, our datajustify the possibility of translating quantitative RT-PCR protocols to routineclinical settings as a new approach to objectively dissect T-NHL and to selectmore appropriate therapeutic protocols

Published

2012

17. Consensus on: Screening and therapy of coronary heart disease in diabetic patients

Author

Rivellese AA1, Piatti PM, Italian Intersociety Consensus G.r.o.u.p. Collaborators Piatti PM, Avogaro A, Anfossi G, Ardigo D, de Kreutzenberg SV, Inchiostro S, Rivellese AA, Trovati M, Zambon S, Zavaroni I, Arcangeli A, Lettino M, Mafrici A, Uguccioni M, Bianchi A, Cavallaro V, Monducci I, Cadeddu C, De Luca G, Manzato E., GENTILE, Sandro, Rivellese, ANGELA ALBAROSA, P. M., Piatti, Rivellese, Aa1, Piatti, Pm, Collaborators Piatti PM, Italian Intersociety Consensus G. r. o. u. p., Avogaro, A, Anfossi, G, Ardigo, D, de Kreutzenberg, Sv, Inchiostro, S, Rivellese, Aa, Trovati, M, Zambon, S, Zavaroni, I, Arcangeli, A, Gentile, Sandro, Lettino, M, Mafrici, A, Uguccioni, M, Bianchi, A, Cavallaro, V, Monducci, I, Cadeddu, C, De Luca, G, and Manzato, E.

Subjects

medicine.medical_specialty, Diabetic Cardiomyopathies, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Cardiovascular risk factors, MEDLINE, Coronary heart disease, Diabetes, Cardiovascular risk factors, Medicine (miscellaneous), Coronary Disease, Revascularization, Electrocardiography, Risk Factors, Diabetes mellitus, Myocardial Revascularization, medicine, Humans, Hypoglycemic Agents, Intensive care medicine, Antihypertensive Agents, Hypolipidemic Agents, Nutrition and Dietetics, Framingham Risk Score, medicine.diagnostic_test, business.industry, Diabetes, Evidence-based medicine, medicine.disease, Coronary heart disease, Italy, Echocardiography, Physical therapy, Cardiology and Cardiovascular Medicine, business, Platelet Aggregation Inhibitors

Abstract

The screening and best treatment for coronary heart disease in diabetic patients is still a matter of debate. For this reason the main Italian scientific societies dealing with diabetes and cardiovascular diseases have tried to finalize a document providing shared recommendations based on the available evidence on : 1) how and who to screen for coronary heart disease, 2) methodologies for the characterization of existing coronary heart disease 3) evaluation of the optimal treatment of cardiovascular risk factors and 4) appropriate revascularization procedures. For each of these points, the levels of evidence and strength of recommendations used in the Italian Standard of Care were adopted.

Published

2011

18. Abatacept in children with juvenile idiopathic arthritis: a randomised, double-blind, placebo-controlled withdrawal trial

Author

Ruperto N, Lovell DJ, Quartier P, Paz E, Rubio Pérez N, Silva CA, Abud Mendoza C, Burgos Vargas R, Gerloni V, Melo Gomes JA, Saad Magalhães C, Sztajnbok F, Goldenstein Schainberg C, Scheinberg M, Penades IC, Fischbach M, Orozco J, Hashkes PJ, Hom C, Jung L, Lepore L, Oliveira S, Wallace CA, Sigal LH, Block AJ, Covucci A, Martini A, Giannini EH, Paediatric Rheumatology INternational Trials Organization, Pediatric Rheumatology Collaborative Study G.r.o.u.p. Collaborators Huemer C, Meunier BB, Deslandre CJ, Lemelle I, Mouy R, Prieur AM, Horneff G, Huppertz HI, Foeldvari I, Minden K, Ravelli A, Loy A, Cortis E, Falcini F, Nunez AF, Chavez J, Blanco FJ, Hofer M, Eberhard BA, Kivitz A, Punaro M, Olson N, Gardiner L., ALESSIO, MARIA, Ruperto, N, Lovell, Dj, Quartier, P, Paz, E, Rubio Pérez, N, Silva, Ca, Abud Mendoza, C, Burgos Vargas, R, Gerloni, V, Melo Gomes, Ja, Saad Magalhães, C, Sztajnbok, F, Goldenstein Schainberg, C, Scheinberg, M, Penades, Ic, Fischbach, M, Orozco, J, Hashkes, Pj, Hom, C, Jung, L, Lepore, L, Oliveira, S, Wallace, Ca, Sigal, Lh, Block, Aj, Covucci, A, Martini, A, Giannini, Eh, Paediatric Rheumatology INternational Trials, Organization, Collaborators Huemer C, Pediatric Rheumatology Collaborative Study G. r. o. u. p., Meunier, Bb, Deslandre, Cj, Lemelle, I, Mouy, R, Prieur, Am, Horneff, G, Huppertz, Hi, Foeldvari, I, Minden, K, Ravelli, A, Loy, A, Cortis, E, Falcini, F, Alessio, Maria, Nunez, Af, Chavez, J, Blanco, Fj, Hofer, M, Eberhard, Ba, Kivitz, A, Punaro, M, Olson, N, and Gardiner, L.

Subjects

Male, medicine.medical_specialty, Immunoconjugates, Adolescent, Arthritis, Placebo, Severity of Illness Index, law.invention, Abatacept, Juvenile Arthritis Disease Activity Score, Double-Blind Method, Randomized controlled trial, law, Internal medicine, medicine, Clinical endpoint, Humans, Range of Motion, Articular, Child, Infusions, Intravenous, Tumor Necrosis Factor-alpha, business.industry, General Medicine, medicine.disease, Arthritis, Juvenile, Rheumatology, Surgery, Treatment Outcome, Antirheumatic Agents, Female, business, Juvenile rheumatoid arthritis, medicine.drug

Abstract

Summary Background Some children with juvenile idiopathic arthritis either do not respond, or are intolerant to, treatment with disease-modifying antirheumatic drugs, including anti-tumour necrosis factor (TNF) drugs. We aimed to assess the safety and efficacy of abatacept, a selective T-cell costimulation modulator, in children with juvenile idiopathic arthritis who had failed previous treatments. Methods We did a double-blind, randomised controlled withdrawal trial between February, 2004, and June, 2006. We enrolled 190 patients aged 6–17 years, from 45 centres, who had a history of active juvenile idiopathic arthritis; at least five active joints; and an inadequate response to, or intolerance to, at least one disease-modifying antirheumatic drug. All 190 patients were given 10 mg/kg of abatacept intravenously in the open-label period of 4 months. Of the 170 patients who completed this lead-in course, 47 did not respond to the treatment according to predefined American College of Rheumatology (ACR) paediatric criteria and were excluded. Of the patients who did respond to abatacept, 60 were randomly assigned to receive 10 mg/kg of abatacept at 28-day intervals for 6 months, or until a flare of the arthritis, and 62 were randomly assigned to receive placebo at the same dose and timing. The primary endpoint was time to flare of arthritis. Flare was defined as worsening of 30% or more in at least three of six core variables, with at least 30% improvement in no more than one variable. We analysed all patients who were treated as per protocol. This trial is registered, number NCT00095173. Findings Flares of arthritis occurred in 33 of 62 (53%) patients who were given placebo and 12 of 60 (20%) abatacept patients during the double-blind treatment (p=0·0003). Median time to flare of arthritis was 6 months for patients given placebo (insufficient events to calculate IQR); insufficient events had occurred in the abatacept group for median time to flare to be assessed (p=0·0002). The risk of flare in patients who continued abatacept was less than a third of that for controls during that double-blind period (hazard ratio 0·31, 95% CI 0·16–0·95). During the double-blind period, the frequency of adverse events did not differ in the two treatment groups. Adverse events were recorded in 37 abatacept recipients (62%) and 34 (55%) placebo recipients (p=0·47); only two serious adverse events were reported, both in controls (p=0·50). Interpretation Selective modulation of T-cell costimulation with abatacept is a rational alternative treatment for children with juvenile idiopathic arthritis. Funding Bristol-Myers Squibb.

Published

2008

19. Reduced specialized processing in psychotic disorder: a graph theoretical analysis of cerebral functional connectivity

Author

Brain, Affectieve & Psychotische Med., Peeters, Sanne C T, Gronenschild, Ed H B M, van Amelsvoort, Therese, van Os, Jim, Marcelis, Machteld, Kahn, Rene, Wiersma, Durk, Bruggeman, Richard, Cahn, Wiepke, de Haan, Lieuwe, Meijer, Carin, Myin-Germeys, Inez, Genetic Risk and Outcome of Psychosis (G.R.O.U.P.), Brain, Affectieve & Psychotische Med., Peeters, Sanne C T, Gronenschild, Ed H B M, van Amelsvoort, Therese, van Os, Jim, Marcelis, Machteld, Kahn, Rene, Wiersma, Durk, Bruggeman, Richard, Cahn, Wiepke, de Haan, Lieuwe, Meijer, Carin, Myin-Germeys, Inez, and Genetic Risk and Outcome of Psychosis (G.R.O.U.P.)

Published

2016

20. Health-related quality of life and treatment preferences in adolescents with type 1 diabetes. The VIPKIDS study

Author

Cherubini V, Gesuita R, Bonfanti R, Frongia AP, Iafusco D, Iannilli A, Lombardo F, Rabbone I, Sabbion A, Salvatoni A, Scaramuzza A, Schiaffini R, Sulli N, Toni S, Tumini S, Mosca A, Carle F, VIPKIDS Study G.r.o.u.p., FRANZESE, ADRIANA, Cherubini, V, Gesuita, R, Bonfanti, R, Franzese, Adriana, Frongia, Ap, Iafusco, D, Iannilli, A, Lombardo, F, Rabbone, I, Sabbion, A, Salvatoni, A, Scaramuzza, A, Schiaffini, R, Sulli, N, Toni, S, Tumini, S, Mosca, A, Carle, F, VIPKIDS Study, G. r. o. u. p., Franzese, A, Iafusco, Dario, and VIPKIDS Study, Group

Subjects

Male, medicine.medical_specialty, Pediatrics, Activities of daily living, Adolescent, Health Status, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, MEDLINE, Infusions, Subcutaneous, Insulin Infusion Systems, Endocrinology, Quality of life, CSII Quality of life Diabetes in childhood. Devices Psychological aspects, Surveys and Questionnaires, Diabetes mellitus, Devices, Diabetes in childhood, Psychological aspects, Internal Medicine, medicine, Humans, Insulin, Child, Health related quality of life, Type 1 diabetes, business.industry, Reproducibility of Results, Patient Preference, General Medicine, medicine.disease, humanities, Diabetes Mellitus, Type 1, Quality of Life, Physical therapy, Female, Observational study, business

Abstract

A multi-centre, observational, cross-sectional study was carried out to determine whether the healthrelated quality of life (HRQOL) of adolescents with type 1 diabetes is affected by different insulin treatment systems, and which features of HRQOL are impacted by the respective insulin treatment. The study regarded 577 adolescents, aged 10–17 years, with type 1 diabetes treated with continuous subcutaneous insulin infusion (CSII) (n = 306) or multiple daily injections (MDI) (n = 271). The Insulin Delivery System Rating Questionnaire was validated in Italian and was self-completed by the subjects during a routine visit to the centres. Subjects were compared following the domains of the questionnaire. Good HRQOL was seen in subjects treated with either MDI or CSII. Significant differences were not found in the domains for general diabetes, including diabetes worries, social burden and psychological well-being. Multiple quantile regression analysis showed that CSII confers significant advantages in terms of HRQOL with improvements in treatment satisfaction, perceived clinical efficacy and reduction in treatment interference with daily activities.This favourable impact was more evident in subjects reporting lower HRQOL scores, suggesting that CSII may be especially useful for individuals perceiving a poor HRQOL. Analysis of the domains indicated that CSII was associated with a higher HRQOL than MDI. Life-course HRQOL evaluation using a standardised questionnaire can ensure better chronic disease management. This is particularly important when providing individualized care for adolescents, as they become increasingly responsible for managing their diabetes.

Published

2014

21. In the last 15 years, survival in Italian children (0-14 years) is increased to 12%. [Negli ultimi 15 anni la sopravvivenza per tumore nei bambini italiani di età 0-14 anni è aumentata del 12%]

Author

Fusco, M, Trama, A, Buzzoni, C, AIRTUM Working G.r.o.u.p. Collaborators: Autelitano, M, Bizzoco, S, Vercelli, M, Borciani, E, Candela, G, Cocchioni, M, Cremone, L, Crocetti, E, Crosignani, P, Cusimano, R, Dei Tos, A, Falcini, F, Federico, M, Ferretti, S, Gennaro, V, Giacomin, A, Gola, G, La Rosa, F, Madeddu, A, Magoni, M, Mangone, L, Maspero, S, Mazzoleni, G, Melcarne, A, Merletti, F, Michiara, M, Minerba, S, Pannozzo, F, Piffer, S, Ponz de Leon, M, Quarta, F, Ricci, P, Russo, A, Sampietro, G, Sciacca, S, Sechi, O, Serraino, D, Sutera Sardo, A, Tisano, F, Traina, A, Tumino, R, Usala, M, VITALE, Francesco, Vitarelli, S, Zanetti, R., Fusco, M, Trama, A, Buzzoni, C, AIRTUM Working Group. Collaborators: Autelitano, M, Bizzoco, S, Vercelli, M, Borciani, E, Candela, G, Cocchioni, M, Cremone, L, Crocetti, E, Crosignani, P, Cusimano, R, Dei Tos, A, Falcini, F, Federico, M, Ferretti, S, Gennaro, V, Giacomin, A, Gola, G, La Rosa, F, Madeddu, A, Magoni, M, Mangone, L, Maspero, S, Mazzoleni, G, Melcarne, A, Merletti, F, Michiara, M, Minerba, S, Pannozzo, F, Piffer, S, Ponz de Leon, M, Quarta, F, Ricci, P, Russo, A, Sampietro, G, Sciacca, S, Sechi, O, Serraino, D, Sutera Sardo, A, Tisano, F, Traina, A, Tumino, R, Usala, M, Vitale, F, Vitarelli, S, and Zanetti, R.

Subjects

descriptive study, children survival, Settore MED/42 - Igiene Generale E Applicata, survival

Published

2014

22. DOORS syndrome: Phenotype, genotype and comparison with Coffin-Siris syndrome

Author

Campeau PM, Hennekam RC, the DOORS Syndrome collaborative g.r.o.u.p., BILO, LEONILDA, Campeau, Pm, Hennekam, Rc, the DOORS Syndrome collaborative, g. r. o. u. p., and Bilo, Leonilda

Abstract

DOORS syndrome (Deafness, Onychodystrophy, Osteodystrophy, mental Retardation, Seizures) is characterized mainly by sensorineural deafness, shortened terminal phalanges with small nails of hands and feet, intellectual deficiency, and seizures. Half of the patients with all clinical features have mutations in TBC1D24. We review here the manifestations of patients clinically diagnosed with DOORS syndrome. In this cohort of 32 families (36 patients) we detected 13 individuals from 10 families with TBC1D24 mutations. Subsequent whole exome sequencing in the cohort showed the same de novoSMARCB1 mutation (c.1130G>A), known to cause Coffin-Siris syndrome, in two patients. Distinguishing features include retinal anomalies, Dandy-Walker malformation, scoliosis, rocker bottom feet, respiratory difficulties and absence of seizures, and 2-oxoglutaric aciduria in the patients with the SMARCB1 mutation. We briefly discuss the heterogeneity of the DOORS syndrome phenotype and the differential diagnosis of this condition.

Published

2014

23. Brain-derived neurotrophic factor/FK506-binding protein 5 genotype by childhood trauma interactions do not impact on hippocampal volume and cognitive performance

Author

Dennis Hernaus, Ruud van Winkel, Ed Gronenschild, Petra Habets, Gunter Kenis, Machteld Marcelis, Jim van Os, Inez Myin-Germeys, Dina Collip, for Genetic Risk and Outcome in Psychosis (G.R.O.U.P.), Potash, James Bennett, Promovendi MHN, Psychiatrie & Neuropsychologie, Ondersteunend personeel MHN, and RS: MHeNs - R2 - Mental Health

Subjects

Male, Hippocampal formation, Neuropsychological Tests, Bioinformatics, Hippocampus, 0302 clinical medicine, Cognition, Neurotrophic factors, Risk Factors, Medicine and Health Sciences, Young adult, Multidisciplinary, Organ Size, Magnetic Resonance Imaging, Medicine, Female, Epigenetics, FKBP5, rs6265, Research Article, Adult, medicine.medical_specialty, Genotype, Science, Neuroimaging, Biology, Polymorphism, Single Nucleotide, Tacrolimus Binding Proteins, Molecular Genetics, 03 medical and health sciences, Young Adult, Mental Health and Psychiatry, medicine, Genetics, Humans, Effects of sleep deprivation on cognitive performance, Psychiatry, Brain-derived neurotrophic factor, Brain-Derived Neurotrophic Factor, Biology and Life Sciences, Human Genetics, 030227 psychiatry, Psychotic Disorders, Schizophrenia, Cognitive Science, Tomography, X-Ray Computed, 030217 neurology & neurosurgery, Neuroscience

Abstract

In the development of psychotic symptoms, environmental and genetic factors may both play a role. The reported association between childhood trauma and psychotic symptoms could therefore be moderated by single nucleotide polymorphisms (SNPs) associated with the stress response, such as FK506-binding protein 5 (FKBP5) and brain-derived neurotrophic factor (BDNF). Recent studies investigating childhood trauma by SNP interactions have inconsistently found the hippocampus to be a potential target underlying these interactions. Therefore, more detailed modelling of these effects, using appropriate covariates, is required. We examined whether BDNF/FKBP5 and childhood trauma interactions affected two proxies of hippocampal integrity: (i) hippocampal volume and (ii) cognitive performance on a block design (BD) and delayed auditory verbal task (AVLT). We also investigated whether the putative interaction was different for patients with a psychotic disorder (n = 89) compared to their non-psychotic siblings (n = 95), in order to elicit possible group-specific protective/vulnerability effects. SNPs were rs9296158, rs4713916, rs992105, rs3800373 (FKBP5) and rs6265 (BDNF). In the combined sample, no BDNF/FKBP5 by childhood trauma interactions were apparent for either outcome, and BDNF/FKBP5 by childhood trauma interactions were not different for patients and siblings. The omission of drug use and alcohol consumption sometimes yielded false positives, greatly affected explained error and influenced p-values. The consistent absence of any significant BDNF/FKBP5 by childhood trauma interactions on assessments of hippocampal integrity suggests that the effect of these interactions on psychotic symptoms is not mediated by hippocampal integrity. The importance of appropriate statistical designs and inclusion of relevant covariates should be carefully considered. ispartof: PLoS One vol:9 issue:3 ispartof: location:United States status: published

Published

2013

24. About 1,400 new cancer diagnosis in Italian children (0-14 years) are attended every year (7,000 in 5 years) [Ogni anno sono previste circa 1.400 nuove diagnosi di tumori maligni nei bambini italiani di età 0-14 anni (7.000 nel quinquennio)]

Author

Crocetti, E, Rondelli, R, Dal Maso, L, AIRTUM Working G.r.o.u.p. Collaborators: Autelitano, M, Bizzoco, S, Vercelli, M, Borciani, E, Buzzoni, C, Candela, G, Cocchioni, M, Cremone, L, Crosignani, P, Cusimano, R, Dei Tos, A, Falcini, F, Federico, M, Ferretti, S, Fusco, M, Gennaro, V, Giacomin, A, Gola, G, La Rosa, F, Madeddu, A, Magoni, M, Mangone, L, Maspero, S, Mazzoleni, G, Melcarne, A, Merletti, F, Michiara, M, Minerba, S, Pannozzo, F, Piffer, S, Ponz de Leon, M, Quarta, F, Ricci, P, Russo, A, Sampietro, G, Sciacca, S, Sechi, O, Serraino, D, Sutera Sardo, A, Tisano, Traina, A, Tumino, R, Usala, M, VITALE, Francesco, Vitarelli, S, Zanetti, R., Crocetti, E, Rondelli, R, Dal Maso, L, AIRTUM Working Group. Collaborators: Autelitano, M, Bizzoco, S, Vercelli, M, Borciani, E, Buzzoni, C, Candela, G, Cocchioni, M, Cremone, L, Crosignani, P, Cusimano, R, Dei Tos, A, Falcini, F, Federico, M, Ferretti, S, Fusco, M, Gennaro, V, Giacomin, A, Gola, G, La Rosa, F, Madeddu, A, Magoni, M, Mangone, L, Maspero, S, Mazzoleni, G, Melcarne, A, Merletti, F, Michiara, M, Minerba, S, Pannozzo, F, Piffer, S, Ponz de Leon, M, Quarta, F, Ricci, P, Russo, A, Sampietro, G, Sciacca, S, Sechi, O, Serraino, D, Sutera Sardo, A, Tisano, Traina, A, Tumino, R, Usala, M, Vitale, F, Vitarelli, S, and Zanetti, R.

Subjects

cancer incidence, cancer in italian children, Settore MED/42 - Igiene Generale E Applicata, cancer in children

Published

2013

25. The SUBITO-DE study: sexual dysfunction in newly diagnosed type 2 diabetes male patients

Author

Corona G1, Giorda CB, Cucinotta D, Guida P, Nada E, SUBITO DE study g.r.o.u.p. CollaboratorsAglialoro A, Albanese V, Albano S, Antonangelo C, Baccetti F, Bulzomì R, Calatola P, Capano F, Clemente G, Corigliano G, Corona G, De Fazio C, De Francesco C, De Joannon U, Del Buono A, Fontana L, Fornengo R, Fraticelli E, Gaviglio D, GENTILE, Sandro, Giorgianni L, GUARINO, Giuseppina, Iannarelli R, Improta L, Improta M, Leotta S, Magro G, Maiani L, Mingardi R, Morviducci L, Nosso G, Nuzzi A, Ocelli C, Paciotti V, Pata P, Rampini PA, Rovere M, Sabbatini A, Sciarrafia M, Sciarretta F, Sforza A, Starnone V, Testori G, Trevisan F, Turco S, Viviani G, Zavaroni D., Corona, G1, Giorda, Cb, Cucinotta, D, Guida, P, Nada, E, CollaboratorsAglialoro A, SUBITO DE study g. r. o. u. p., Albanese, V, Albano, S, Antonangelo, C, Baccetti, F, Bulzomì, R, Calatola, P, Capano, F, Clemente, G, Corigliano, G, Corona, G, De Fazio, C, De Francesco, C, De Joannon, U, Del Buono, A, Fontana, L, Fornengo, R, Fraticelli, E, Gaviglio, D, Gentile, Sandro, Giorgianni, L, Guarino, Giuseppina, Iannarelli, R, Improta, L, Improta, M, Leotta, S, Magro, G, Maiani, L, Mingardi, R, Morviducci, L, Nosso, G, Nuzzi, A, Ocelli, C, Paciotti, V, Pata, P, Rampini, Pa, Rovere, M, Sabbatini, A, Sciarrafia, M, Sciarretta, F, Sforza, A, Starnone, V, Testori, G, Trevisan, F, Turco, S, Viviani, G, and Zavaroni, D.

Subjects

Male, Depression, Hypogonadism, Comorbidity, Middle Aged, Prognosis, Cross-Sectional Studies, Diabetes Mellitus, Type 2, Erectile Dysfunction, Risk Factors, Humans, Testosterone, Longitudinal Studies, Prospective Studies, Follow-Up Studies

Abstract

No data on the prevalence of erectile dysfunction (ED) in subjects with newly diagnosed Type 2 diabetes mellitus (T2DM) are currently available.The aim of the present study was to estimate the prevalence of ED and its associated causes in a sample of male patients with recently diagnosed DM (24 months) attending a diabetes care center.The study comprised two phases: a cross-sectional analysis and a longitudinal reassessment of the data collected during the first phase. During the first phase, 1503 subjects (mean age 58.7±8.9 yr) from 27 centers were interviewed: 666 (43.3%) reported experiencing ED, 499 of which (mean age 58.8±8.8 yr) agreed to participate in the study (final enrolment rate, 33.3%). Concurrent morbidities were hypertension (55.3%), dyslipidemia (39.5%), and coronary heart disease (7.8%); chronic complications were neuropathy (8.9%), nephropathy (12.6%) and retinopathy (7.6%) in about one third of the sample at enrolment.Overall, about 20% of the patients reported having used ED drugs, but more than 50% had abandoned therapy because of the drug's ineffectiveness or high cost. The prevalence of hypogonadism was 46.9% (total testosterone level, 3.5 ng/ml). Some 20% of patients reported symptoms suggestive of depression.The present study provides data showing a high prevalence of ED, hypogonadism and depressive symptoms among male patients with newly diagnosed T2DM. Further analysis of the data will elucidate the specific determinants of such conditions and their longitudinal significance.

Published

2013

26. GADA titer-related risk for organ-specific autoimmunity in LADA subjects subdivided according to gender (NIRAD study 6)

Author

Zampetti S, Capizzi M, Spoletini M, Campagna G, Leto G, Cipolloni L, Tiberti C, Bosi E, Falorni A, Buzzetti R, NIRAD Study G.r.o.u.p. Collaborators Arpi ML, Bracaglia D, Capuano G, Carro S, Cocco L, Ciccarone AM, Cossu E, De Cosmo S, Dei Cas A, De Simone G, Giordano C, Giorgino F, Laviola L, Mantovani E, Poma C, Meloncelli I, Morano S, Morviducci L, Pontiroli AE, Pozzilli P, Rotella C, Songini M, Cau V, Spallone V, Tatti P., GENTILE, Sandro, Zampetti, S, Capizzi, M, Spoletini, M, Campagna, G, Leto, G, Cipolloni, L, Tiberti, C, Bosi, E, Falorni, A, Buzzetti, R, Collaborators Arpi ML, NIRAD Study G. r. o. u. p., Bracaglia, D, Capuano, G, Carro, S, Cocco, L, Ciccarone, Am, Cossu, E, De Cosmo, S, Dei Cas, A, De Simone, G, Gentile, Sandro, Giordano, C, Giorgino, F, Laviola, L, Mantovani, E, Poma, C, Meloncelli, I, Morano, S, Morviducci, L, Pontiroli, Ae, Pozzilli, P, Rotella, C, Songini, M, Cau, V, Spallone, V, and Tatti, P.

Subjects

Male, Tissue transglutaminase, Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Thyroid Gland, Autoimmunity, Type 2 diabetes, medicine.disease_cause, Biochemistry, LADA, Settore MED/13 - Endocrinologia, Endocrinology, Risk Factors, Seroepidemiologic Studies, Insulin-Secreting Cells, Age of Onset, biology, Glutamate Decarboxylase, Middle Aged, anti-TPO, Titer, Female, Antibody, Adult, medicine.medical_specialty, tiroidite cronica, anti-21-idrossilasi, Context (language use), organ-specific autoimmunity, GADA, Thyroid peroxidase, Internal medicine, Diabetes mellitus, medicine, Humans, Diabete autoimmune latente dell'adulto, Morbo di Addison, Sex Distribution, Autoantibodies, business.industry, Biochemistry (medical), medicine.disease, Diabetes Mellitus, Type 1, Diabetes Mellitus, Type 2, Immunology, biology.protein, business

Abstract

Latent autoimmune diabetes in adults (LADA) includes a heterogeneous population wherein, based on glutamic acid decarboxylase antibody (GADA) titer, different subgroups of subjects can be identified. OBJECTIVE: The aim of the present study was to evaluate GADA titer-related risk for β-cell and other organ-specific autoimmunity in LADA subjects. METHODS: Adult-onset autoimmune diabetes subjects (n=236) and type 2 diabetes (T2DM) subjects (n=450) were characterized for protein tyrosine phosphatase (IA-2IC and IA-2(256-760)), zinc transporter 8 (ZnT8), thyroid peroxidase, (TPO), steroid 21-hydroxylase (21-OH), tissue transglutaminase (tTG), and antiparietal cell (APC) antibodies. RESULTS: High GADA titer compared to low GADA titer showed a significantly higher prevalence of IA-2IC, IA-2(256-760), ZnT8, TPO, and APC antibodies (P≤0.04 for all comparison). 21-OH antibodies were detected in 3.4% of high GADA titer. A significant decreasing trend was observed from high GADA to low GADA and to T2DM subjects for IA-2(256-760), ZnT8, TPO, tTG, and APC antibodies (P for trend≤0.001). TPO was the only antibody showing a different prevalence between gender; low GADA titer and T2DM female patients had a higher frequency of TPO antibody compared to males (P=0.0004 and P=0.0006, respectively), where the presence of high GADA titer conferred an odds ratio of 8.6 for TPO compared to low GADA titer. After subdividing high and low GADA titer subjects according to the number of antibodies, we observed that 73.3% of high GADA titer subjects were positive for at least one or more antibodies, compared to 38.3% of low GADA titer (P

Published

2012

27. Intravenous immunoglobulin versus intravenous methylprednisolone for chronic inflammatory demyelinating polyradiculoneuropathy: a randomised controlled trial

Author

Nobile Orazio E, Cocito D, Jann S, Uncini A, Beghi E, Messina P, Antonini G, Fazio R, Gallia F, Schenone A, Francia A, Pareyson D, SANTORO, LUCIO, Tamburin S, Macchia R, Cavaletti G, Giannini F, Sabatelli M, for the IMC Trial G.r.o.u.p., Cavaletti, G, Nobile Orazio, E, Cocito, D, Jann, S, Uncini, A, Beghi, E, Messina, P, Antonini, G, Fazio, R, Gallia, F, Schenone, A, Francia, A, Pareyson, D, Santoro, Lucio, Tamburin, S, Macchia, R, Giannini, F, Sabatelli, M, and for the IMC Trial, G. r. o. u. p.

Subjects

Adult, Male, chronic inflammatory demyelinating polyradiculoneuropathy, Intravenous Immunoglobulin (IVIg), intravenous methylprednisolone, Treatment Outcome, clinical trial, CIDP, Placebo, Methylprednisolone, Severity of Illness Index, Follow-Up Studie, law.invention, Young Adult, Double-Blind Method, Randomized controlled trial, Recurrence, Modified Rankin Scale, law, medicine, Infusions, Intravenou, intravenous immunoglobin versus intravenous methilprednisolone, Adverse effect, Aged, Aged, 80 and over, business.industry, Polyradiculoneuropathy, Middle Aged, medicine.disease, Discontinuation, Anti-Inflammatory Agent, Settore MED/26 - NEUROLOGIA, Polyradiculoneuropathy, Chronic Inflammatory Demyelinating, Tolerability, Immunoglobulins, Intravenou, Anesthesia, Female, Neurology (clinical), business, Human, medicine.drug

Abstract

Summary Background Intravenous immunoglobulin (IVIg) and corticosteroids are effective as initial treatment in patients with chronic inflammatory demyelinating polyradiculoneuropathy (CIDP), but little is known about the comparative risk–benefit profile of their long-term use in this disease. We compared the efficacy and tolerability of 6-month therapy with IVIg versus that with intravenous methylprednisolone. Methods We did a multicentre, randomised, double-blind, placebo controlled, parallel-group study in patients with CIDP. We assessed efficacy and tolerability of IVIg (0·5 g/kg per day for 4 consecutive days) and intravenous methylprednisolone (0·5 g in 250 mL sodium chloride solution per day for 4 consecutive days) given every month for 6 months. Eligible patients had to be in an active or stationary phase of the disease. Allocation to treatment was centrally managed with a computer-generated, 1:1 randomisation scheme with a sequential block size of four. All patients and assessors were unaware of the treatment assignment. After therapy discontinuation, patients were followed up for 6 months to assess relapses. The primary outcome was the difference in the number of patients discontinuing either therapy owing to inefficacy or intolerance. Secondary endpoints included the difference in the proportion of patients experiencing adverse events or worsening after therapy discontinuation. This study is registered with EUDRACT, number 2005-001136-76. Findings 45 patients (24 IVIg, 21 intravenous methylprednisolone) completed the study; one was excluded for inappropriate inclusion. More patients stopped methylprednisolone (11 [52%] of 21) than IVIg (three [13%] of 24; relative risk 0·54, 95% CI 0·34–0·87; p=0·0085). When adjusted for sex, age, disease duration, comorbidity, modified Rankin scale and ONLS scores at enrolment, and previous treatment with IVIg and steroids, the difference between the two groups remained significant (odds ratio 7·7, 95% CI 1·7–33·9; p=0·0070). Reasons for discontinuation were lack of efficacy (eight in the methylprednisolone group vs three in the IVIg group), adverse events (one in the methylprednisolone group), or voluntary withdrawal (two in the methylprednisolone group). Two patients on IVIg died during follow-up after the 6-month assessment. The proportion of patients with adverse events did not differ between the intravenous methylprednisolone group (14 [67%] of 21) and the IVIg group (11 [46%] of 24; p=0·1606). After therapy discontinuation, more patients on IVIg worsened and required further therapy (eight [38%] of 21) than did those on methylprednisolone (none of ten; p=0·0317). Interpretation Treatment of CIDP with IVIg for 6 months was less frequently discontinued because of inefficacy, adverse events, or intolerance than was treatment with intravenous methylprednisolone. The longer-term effects of these treatments on the course of CIDP need to be addressed in future studies. Funding Kedrion.

Published

2012

28. Categorisation of complications and validation of the Clavien score for percutaneous nephrolithotomy

Author

de la Rosette JJ, Opondo D, Daels FP, Giusti G, Serrano A, Kandasami SV, Wolf JS Jr, Grabe M, Gravas S, CROES PCNL Study G.r.o.u.p. Hendrikx A, Tefekli A, Yamaguchi A, Breda A, D'Addessi A, Crisci A, Kural AR, Serrano Pascual A, Hoznek A, Gross A, Skolarikos A, Timoney A, De Lisa A, Celia A, Frattini A, Smith A, Mandal A, Rippa A, van Cleynenbreugel B, Silva B, Onal B, Turna B, Wong C, Saussine C, Klingler C, Pacik D, Bolton D, Tolley D, Assimos D, Montanari E, Liatsikos E, Cauda F, Gopalakrishnan G, Ibarlucea Gonzalez G, Labate G, Bianchi G, Preminger G, Bueno Chomon G, Guisti G, Razvi H, Walfridsson H, Shah H, Lingeman J, Kums J, de la Rosette J, Rassweiler J, Stolzenburg JU, Gutierrez J, Rioja J, Amón Sesmero J, Valdivia Uria JG, Sangam K, Lopez Garcia JA, Nutahara K, Kijvikai K, Szymanski K, Shi L, Cormio L, Desai M, Lopes T, Garofalo M, Pearle M, Sofer M, Grasso M, Louie M, Luke M, Melekos M, Boja MR, Botoca M, Duvdevani M, Gupta N, Buchholz N, Osther P, Alken P, Olbert P, Vijverberg P, Geavlete P, Saba P, Kapoor R, Venkatesh R, Nadler R, Scarpa R, Guven S, Pal SK, Nakada S, Wolf S. Jr, Erdogru T, Averch T, Bucuras V, Xue W, Boellaard W, Strijbos W, Zhang X, Sun Y., DE SIO, Marco, de la Rosette, Jj, Opondo, D, Daels, Fp, Giusti, G, Serrano, A, Kandasami, Sv, Wolf JS, Jr, Grabe, M, Gravas, S, Hendrikx A, CROES PCNL Study G. r. o. u. p., Tefekli, A, Yamaguchi, A, Breda, A, D'Addessi, A, Crisci, A, Kural, Ar, Serrano Pascual, A, Hoznek, A, Gross, A, Skolarikos, A, Timoney, A, De Lisa, A, Celia, A, Frattini, A, Smith, A, Mandal, A, Rippa, A, van Cleynenbreugel, B, Silva, B, Onal, B, Turna, B, Wong, C, Saussine, C, Klingler, C, Pacik, D, Bolton, D, Tolley, D, Assimos, D, Montanari, E, Liatsikos, E, Cauda, F, Gopalakrishnan, G, Ibarlucea Gonzalez, G, Labate, G, Bianchi, G, Preminger, G, Bueno Chomon, G, Guisti, G, Razvi, H, Walfridsson, H, Shah, H, Lingeman, J, Kums, J, de la Rosette, J, Rassweiler, J, Stolzenburg, Ju, Gutierrez, J, Rioja, J, Amón Sesmero, J, Valdivia Uria, Jg, Sangam, K, Lopez Garcia, Ja, Nutahara, K, Kijvikai, K, Szymanski, K, Shi, L, Cormio, L, Desai, M, Lopes, T, DE SIO, Marco, Garofalo, M, Pearle, M, Sofer, M, Grasso, M, Louie, M, Luke, M, Melekos, M, Boja, Mr, Botoca, M, Duvdevani, M, Gupta, N, Buchholz, N, Osther, P, Alken, P, Olbert, P, Vijverberg, P, Geavlete, P, Saba, P, Kapoor, R, Venkatesh, R, Nadler, R, Scarpa, R, Guven, S, Pal, Sk, Nakada, S, Wolf S., Jr, Erdogru, T, Averch, T, Bucuras, V, Xue, W, Boellaard, W, Strijbos, W, Zhang, X, and Sun, Y.

Abstract

BACKGROUND: Although widely used, the validity and reliability of the Clavien classification of postoperative complications have not been tested in urologic procedures, such as percutaneous nephrolithotomy (PCNL). OBJECTIVE: To validate the Clavien score and categorise complications of PCNL. DESIGN, SETTING, AND PARTICIPANTS: Data for 528 patients with complications after PCNL were used to create a set of 70 unique complication-management combinations. Clinical case summaries for each complication-management combination were compiled in a survey distributed to 98 urologists, who rated each combination using the Clavien classification. OUTCOME MEASUREMENTS AND STATISTICAL ANALYSIS: Interrater agreement for Clavien scores was estimated using Fleiss' kappa (κ). The relationship between Clavien score and the duration of postoperative hospital stay was analysed using multivariate nonlinear regression models that adjusted for operating time, preoperative urine microbial culture, presence of staghorn stone, and use of postoperative nephrostomy tube. RESULTS AND LIMITATIONS: Overall interrater agreement in grading postoperative complications was moderate (κ=0.457; p

Published

2012

29. Aminoterminal natriuretic peptides and cardiovascular risk in an Italian male adult cohort

Author

BARBATO, ANTONIO, IACONE, ROBERTO, IPPOLITO, RENATO, STRAZZULLO, PASQUALE, Sciarretta S, Marchitti S, Di Castro S, Stanzione R, Cotugno M, Palmieri L, Calvieri C, Battistoni A, Volpe M, Rubattu S, Olivetti Heart Study Research G.r.o.u.p., Barbato, Antonio, Sciarretta, S, Marchitti, S, Iacone, Roberto, Di Castro, S, Stanzione, R, Cotugno, M, Ippolito, Renato, Palmieri, L, Calvieri, C, Battistoni, A, Volpe, M, Strazzullo, Pasquale, Rubattu, S, and Olivetti Heart Study Research, G. r. o. u. p.

Subjects

Adult, Male, medicine.medical_specialty, cohort, Study research, Risk Assessment, Sensitivity and Specificity, Cohort Studies, Cardiovascular prevention, Internal medicine, Epidemiology, Natriuretic Peptide, Brain, medicine, Humans, risk, Aged, Aged, 80 and over, business.industry, cardiovascular, natriuretic peptides, cardiovascular prevention, cardiovascular risk, Medical school, Middle Aged, peptide, Peptide Fragments, Endocrinology, Italy, ROC Curve, Cardiovascular Diseases, Family medicine, Cohort, Aminoterminal, natriuretic, Cardiology and Cardiovascular Medicine, business, Algorithms, Atrial Natriuretic Factor, Biomarkers, Cohort study

Abstract

adult cohort☆,☆☆ Antonio Barbato , Sebastiano Sciarretta , Simona Marchitti , Roberto Iacone , Sara Di Castro , Rosita Stanzione , Maria Cotugno , Renato Ippolito , Luigi Palmieri , Camilla Calvieri , Allegra Battistoni , Massimo Volpe , Pasquale Strazzullo , Speranza Rubattu b,c,⁎ and On behalf of the Olivetti Heart Study Research Group a Department of Clinical and Experimental Medicine, Federico II University of Naples Medical School, Naples, Italy b IRCCS Neuromed, Pozzilli (Is) Italy c Department of Cardiology, School of Medicine and Psychology, University Sapienza of Rome, Ospedale S. Andrea, Rome, Italy d Department of Cerebro and Cardiovascular Diseases Epidemiology, Istituto Superiore di Sanita, Rome, Italy

Published

2011

30. Prevalence of hypovitaminosis D and factors associated with vitamin D deficiency and morbidity among HIV-infected patients enrolled in a large Italian cohort

Author

Vescini F, Cozzi Lepri A, Maggiolo F, De Luca A, Cassola G, Vullo V, Carosi G, Antinori A, Tozzi V, Monforte AD, Icona Foundation Study G.r.o.u.p. Moroni M, Angarano G, Cauda R, Di Perri G, Galli M, Iardino R, Ippolito G, Lazzarin A, Perno CF, Von Schlosser F, Ammassari A, Andreoni M, Balotta C, Bonfanti P, Bonora S, Capobianchi MR, Castagna A, Ceccherini Silberstein F, Gargiulo M, Gervasoni C, Girardi E, Lichtner M, Lo Caputo S, Madeddu G, Marcotullio S, Monno L, Murri R, Mussini C, Puoti M, Torti C, Fanti I, Formenti T, Montroni M, Giacometti A, Costantini A, Riva A, Tirelli U, Martellotta F, Ladisa N, Suter F, Cristini G, Minardi C, Bertelli D, Quirino T, Abeli C, Manconi PE, Piano P, Vecchiet J, Falasca K, Carnevale G, Lorenzotti S, Sighinolfi L, Leoncini F, Mazzotta F, Pozzi M, Viscoli G, Alessandrini A, Piscopo R, Mazzarello G, Mastroianni C, Belvisi V, Molteni C, Chiodera A, Castelli P, Rizzardini G, Ridolfo AL, Foschi A, Salpietro S, Merli S, Carenzi L, Moioli MC, Cicconi P, Esposito R, Gori A, Pastore V, Abrescia N, Chirianni A, De Marco M, Ferrari C, Borghi R, Baldelli F, Belfiori B, Parruti G, Sozio F, Magnani G, Ursitti MA, Emilia R, Arlotti M, Ortolani P, Antonucci G, Narciso P, Zaccarelli M, Gallo L, Acinapura R, De Longis P, Ceccarelli L, Libertone R, Trotta MP, Miccoli A, Cattelan AM, Mura MS, Caramello P, Orofino GC, Sciandra M, Raise E, Ebo F, Pellizzer G, Buonfrate D., BORDERI, MARCO, RE, MARIA CARLA, VIALE, PIERLUIGI, VERUCCHI, GABRIELLA, PIERGENTILI, BENEDETTA, Vescini F, Cozzi-Lepri A, Borderi M, Re MC, Maggiolo F, De Luca A, Cassola G, Vullo V, Carosi G, Antinori A, Tozzi V, Monforte AD, Icona Foundation Study Group.Moroni M, Angarano G, Cauda R, Di Perri G, Galli M, Iardino R, Ippolito G, Lazzarin A, Perno CF, Viale PL, Von Schlosser F, Ammassari A, Andreoni M, Balotta C, Bonfanti P, Bonora S, Capobianchi MR, Castagna A, Ceccherini-Silberstein F, Gargiulo M, Gervasoni C, Girardi E, Lichtner M, Lo Caputo S, Madeddu G, Marcotullio S, Monno L, Murri R, Mussini C, Puoti M, Torti C, Fanti I, Formenti T, Montroni M, Giacometti A, Costantini A, Riva A, Tirelli U, Martellotta F, Ladisa N, Suter F, Verucchi G, Piergentili B, Cristini G, Minardi C, Bertelli D, Quirino T, Abeli C, Manconi PE, Piano P, Vecchiet J, Falasca K, Carnevale G, Lorenzotti S, Sighinolfi L, Leoncini F, Mazzotta F, Pozzi M, Viscoli G, Alessandrini A, Piscopo R, Mazzarello G, Mastroianni C, Belvisi V, Molteni C, Chiodera A, Castelli P, Rizzardini G, Ridolfo AL, Foschi A, Salpietro S, Merli S, Carenzi L, Moioli MC, Cicconi P, Esposito R, Gori A, Pastore V, Abrescia N, Chirianni A, De Marco M, Ferrari C, Borghi R, Baldelli F, Belfiori B, Parruti G, Sozio F, Magnani G, Ursitti MA, Emilia R, Arlotti M, Ortolani P, Antonucci G, Narciso P, Zaccarelli M, Gallo L, Acinapura R, De Longis P, Ceccarelli L, Libertone R, Trotta MP, Miccoli A, Cattelan AM, Mura MS, Caramello P, Orofino GC, Sciandra M, Raise E, Ebo F, Pellizzer G, Buonfrate D., Vescini, F, Cozzi Lepri, A, Borderi, M, Re, M, Maggiolo, F, De Luca, A, Cassola, G, Vullo, V, Carosi, G, Antinori, A, Tozzi, V, Monforte, A, Gori, A, Vescini, Fabio, Cozzi lepri, Alessandro, Borderi, Marco, Re, Maria Carla, Maggiolo, Franco, De Luca, Andrea, Cassola, Giovanni, Vullo, Vincenzo, Carosi, Giampiero, Antinori, Andrea, Tozzi, Valerio, Monforte, Antonella D'arminio, Icona Foundation Study, Group, and Castagna, Antonella

Subjects

Male, HIV Infections, vitamin D, Logistic regression, Risk Factors, Cardiovascular Disease, Prevalence, HIV Infection, Pharmacology (medical), Renal Insufficiency, Chronic, Vitamin D, Young adult, education.field_of_study, hiv infection, prognosis, vitamin d deficiency and insufficiency, Diabetes Mellitu, Middle Aged, Prognosis, Infectious Diseases, Anti-Retroviral Agents, Italy, Cardiovascular Diseases, Combination, Cohort, Linear Model, Drug Therapy, Combination, Female, Seasons, prognosi, Adult, Africa, Aged, Central America, Diabetes Mellitus, Drug Therapy, Humans, Linear Models, South America, Vitamin D Deficiency, Young Adult, Human, medicine.medical_specialty, Population, Infectious Disease, Settore MED/17 - MALATTIE INFETTIVE, vitamin D deficiency, Internal medicine, medicine, Vitamin D and neurology, Renal Insufficiency, Chronic, education, Survival analysis, business.industry, Risk Factor, Hypovitaminosis D, HIV, Odds ratio, medicine.disease, vitamin D deficiency and insufficiency, Immunology, Anti-Retroviral Agent, Season, business

Abstract

Background: A high prevalence of hypovitaminosis D (hypD) in HIV-infected patients has been reported, but reasons are unclear. Methods: The 25 hydroxy vitamin D (vitD) concentration was measured in a sample of HIV-positive patients from Italy enrolled in the Icona Foundation Study. The change in absolute levels of vitD pre/post combination antiretroviral treatment was modelled by linear regression controlling for confounders and seasonality. Factors associated with hypD were identified using logistic regression analysis, and survival analysis was employed to evaluate the prognostic value of vitD concentration to predict severe diseases (diabetes, cardiovascular, renal), AIDS, and death. RESULTS:: We studied 810 patients contributing 1408 vitD measures. Median age was 36 years (range: 20-69). VitD insufficiency (30-75 nmol/L) and deficiency (

Published

2011

31. Acute myeloid leukemia in Italian patients with multiple sclerosis treated with mitoxantrone

Author

Martinelli V, Cocco E, Capra R, Salemi G, Gallo P, Capobianco M, Pesci I, Ghezzi A, Pozzilli C, Lugaresi A, Bellantonio P, Amato MP, Grimaldi LM, Trojano M, Mancardi GL, Bergamaschi R, Gasperini C, Rodegher M, Straffi L, Ponzio M, Comi G, Italian Mitoxantrone G.r.o.u.p. COLLABORATORS: Radaelli M, Esposito F, Moiola L, Colombo B, Rossi P, Marrosu MG, Frau J, Lorefice L, Coghe G, Savettieri G, Ragonese P, Cusimano V, Perini P, Rinaldi F, Vidali A, Bertolotto A, Malucchi S, Di Sapio A, Montanari E, Guareschi A, Rizzo A, Zaffaroni M, Baldini S, De Rossi N, Cordioli C, Rasia S, Salvetti M, Buttinelli C, Ausili Cefaro L, De Luca G, Tommaso D, Farina D, Fantozzi R, Ruggieri S, Hakiki B, Zipoli V, Portaccio E, Bartolozzi ML, Scandellari C, Stecchi S, Marchello LP, Palmeri B, Vitello G, Iaffaldano P, Lucchese G, Dattola V, Buccafusca M, Sola P, Simone AM, Barreca F, Patti F, Laisa P, Cavalla P, Masera S, Tavazzi E, Galgani S, Sacco R, Provinciali L, Maura D, LUS, Giacomo, Alfieri G, Ticca A, Piras ML, Maimone D, Bianca M, Iudice A, Giro ME, Galeotti M, Florio C, Spitalieri P, La Mantia L, Motti L, Rottoli MR, Granella F, Solaro C, Scarpini E, Servillo G, Cavalletti G., TEDESCHI, Gioacchino, Martinelli, V, Cocco, E, Capra, R, Salemi, G, Gallo, P, Capobianco, M, Pesci, I, Ghezzi, A, Pozzilli, C, Lugaresi, A, Bellantonio, P, Amato, Mp, Grimaldi, Lm, Trojano, M, Mancardi, Gl, Bergamaschi, R, Gasperini, C, Rodegher, M, Straffi, L, Ponzio, M, Comi, G, COLLABORATORS: Radaelli M, Italian Mitoxantrone G. r. o. u. p., Esposito, F, Moiola, L, Colombo, B, Rossi, P, Marrosu, Mg, Frau, J, Lorefice, L, Coghe, G, Savettieri, G, Ragonese, P, Cusimano, V, Perini, P, Rinaldi, F, Vidali, A, Bertolotto, A, Malucchi, S, Di Sapio, A, Montanari, E, Guareschi, A, Rizzo, A, Zaffaroni, M, Baldini, S, De Rossi, N, Cordioli, C, Rasia, S, Salvetti, M, Buttinelli, C, Ausili Cefaro, L, De Luca, G, Tommaso, D, Farina, D, Fantozzi, R, Ruggieri, S, Hakiki, B, Zipoli, V, Portaccio, E, Bartolozzi, Ml, Scandellari, C, Stecchi, S, Marchello, Lp, Palmeri, B, Vitello, G, Iaffaldano, P, Lucchese, G, Dattola, V, Buccafusca, M, Sola, P, Simone, Am, Barreca, F, Patti, F, Laisa, P, Cavalla, P, Masera, S, Tavazzi, E, Galgani, S, Tedeschi, Gioacchino, Sacco, R, Provinciali, L, Maura, D, Lus, Giacomo, Alfieri, G, Ticca, A, Piras, Ml, Maimone, D, Bianca, M, Iudice, A, Giro, Me, Galeotti, M, Florio, C, Spitalieri, P, La Mantia, L, Motti, L, Rottoli, Mr, Granella, F, Solaro, C, Scarpini, E, Servillo, G, and Cavalletti, G.

Published

2011

32. URBAN GEOCHEMICAL STUDIES IN EUROPE

Author

Demetriades A., Birke M., Locutura J., Bel lan A. B., Duris M., EuroGeoSurveys Geochemistry Expert G.r.o.u.p. members of the EuroGeoSurveys Geochemistry Expert Group, Austria: Albert Schedl, Heinz Reitner, Edith Haslinger, Peter Filzmoser, Belgium: Walter De Vos, Bosnia, Herzegovina: Hazim Hrvatovic, Neven Miosic, Ferid Skopljak, Natalija Samardzic, Bulgaria: Valeri Trendavilov, Croatia: Josip Halamić, Ajka Šorša, Stjepan Husnjak, Czech Republic: Miloslav Duris, Cyprus: Zomenia Zomeni, Denmark: Vibeke Ernstsen, Estonia: Jaan Kivisilla, Walter Petersell, Finland: Timo Tarvainen, Mikael Eklund, France: Ignace Salpeteur, F. Y. R. O. M. : Trajce Stafilov, Germany: Manfred Birke, Rainer Hoffmann, Jens Utermann, Hellas: Alecos Demetriades, Hungary: Gyozo Jordan, Ubul Fugedi, Laszlo Kuti, Ireland: Patrick O’Connor, Fionnuala Ni Mhairtin, Vincent Gallagher, Italy: Benedetto De Vivo, Annamaria Lima, Stefano Albanese, Domenico Cicchella, Paolo Valera, Latvia: Aivars Gilucis, Lithuania: Virgilija Gregorauskiene, Luxembourg: Robert Maquil, Netherlands, The: Gerben Mol, Norway: Clemens Reimann, Rolf Tore Ottesen, Tore Volden, Ola A. Eggen, Arnold Arnoldussen, Poland: Anna Pasieczna, Aleksandra Dusza, Paweł Kwecko, Portugal: Maria Joao Batista, Cátia Prazeres, Serbia: Aleksandra Gulan, Dragana Vidojević, Slovakia: Igor Slaninka, Peter Sefcik, Daniela Mackovych, Silvester Pramuka, Slovenia: Mateja Gosar, Spain: Juan Locutura, Alejandro Bel lan, Sweden: Madelen Andersson, Kaj Lax, Switzerland: Peter Hayoz, Reto Giulio Meuli, Ukraine: Boris I. Malyuk, Volodymyr Klos, United Kingdom: Dee Flight, Andreas Scheib, Mick Strutt, Paul McDonnell, DINELLI, ENRICO, Demetriades A., Birke M., Locutura J., Bel-lan A.B., Duris M. and EuroGeoSurveys Geochemistry Expert Group. members of the EuroGeoSurveys Geochemistry Expert Group, Austria: Albert Schedl, Heinz Reitner, Edith Haslinger, Peter Filzmoser, Belgium: Walter De Vo, Bosnia & Herzegovina: Hazim Hrvatovic, Neven Miosic, Ferid Skopljak, Natalija Samardzic, Bulgaria: Valeri Trendavilov, Croatia: Josip Halamić, Ajka Šorša, Stjepan Husnjak, Czech Republic: Miloslav Duri, Cyprus: Zomenia Zomeni, Denmark: Vibeke Ernstsen, Estonia: Jaan Kivisilla, Walter Petersell, Finland: Timo Tarvainen, Mikael Eklund, France: Ignace Salpeteur, F.Y.R.O.M.: Trajce Stafilov, Germany: Manfred Birke, Rainer Hoffmann, Jens Utermann, Hellas: Alecos Demetriade, Hungary: Gyozo Jordan, Ubul Fugedi, Laszlo Kuti, Ireland: Patrick O’Connor, Fionnuala Ni Mhairtin, Vincent Gallagher, Italy: Benedetto De Vivo, Annamaria Lima, Stefano Albanese, Enrico Dinelli, Domenico Cicchella, Paolo Valera, Latvia: Aivars Giluci, Lithuania: Virgilija Gregorauskiene, Luxembourg: Robert Maquil, Netherlands, The: Gerben Mol, Norway: Clemens Reimann, Rolf Tore Ottesen, Tore Volden, Ola A. Eggen, Arnold Arnoldussen, Poland: Anna Pasieczna, Aleksandra Dusza, Paweł Kwecko, Portugal: Maria Joao Batista, Cátia Prazere, Serbia: Aleksandra Gulan, Dragana Vidojević, Slovakia: Igor Slaninka, Peter Sefcik, Daniela Mackovych, Silvester Pramuka, Slovenia: Mateja Gosar, Spain: Juan Locutura, Alejandro Bel-lan, Sweden: Madelen Andersson, Kaj Lax, Switzerland: Peter Hayoz, Reto Giulio Meuli, Ukraine: Boris I. Malyuk, Volodymyr Klo, and United Kingdom: Dee Flight, Andreas Scheib, Mick Strutt, Paul McDonnell.

Subjects

CONTAMINATION, EUROPE, toxic chemical element, dust, urban geochemistry, soil

Abstract

Urban soil is generally contaminated to a variable degree depending on its proximity to contamination sources. Traffic is one of the main sources of urban contamination; lead (Pb) from the use of leaded petrol, zinc (Zn) and cadmium (Cd) from tyre wear, antimony (Sb) from break pads, and the platinum group elements (PGEs) from the wear of catalytic converters, are some typical elements that often reach high concentrations in the urban environment. Lead was also a key ingredient in white paint, and in towns with a high proportion of white wooden houses very high concentrations were found in soil. Crematoria can or have emitted mercury (Hg). Coal and heavy oil fired municipal power and heating stations emit sulphur (S), silver (Ag), vanadium (V), bromine (Br) and barium (Ba). The use of impregnated wood may have resulted in high concentrations of arsenic (As), especially in kindergartens (nursery schools) and playgrounds. Building materials (plaster and paint) may also contain high concentrations of organic contaminants, especially polychlorinated biphenyls (PCBs), which again end up in urban soil. Coal and wood burning, the use of diesel fuel, and the production of coke, all lead to the emission of polycyclic aromatic hydrocarbons (PAHs). There exist countless other sources of local contamination in towns, and there is thus every reason to be concerned about the quality of the urban environment, and the suitability of soil for sensitive land uses, such as schools, playgrounds, parks and vegetable gardens. Contaminated urban soil may contaminate indoor dust and, therefore, to an increased human exposure to toxic chemicals. Consequently, the distribution of toxic contaminants in urban soil needs to be documented and known by city administration to avoid costly mistakes in land use planning, and further spreading of highly contaminated materials. The EuroGeoSurveys ‘Geochemistry’ Expert Group during the compilation of a proposal to the Directors for a European wide urban geochemistry project, using a harmonised sampling and analytical methodology, it discovered that many urban geochemical studies have been performed in Europe by National Geological Surveys, which are not known to the wider geoscientific community. Since, the results of these studies are directly related to our quality of life, the EuroGeoSurveys ‘Geo chemistry’ Expert Group decided to publish at least one case study from each country in a book,which will be available in the second half of 2010. A concise description of some of these studies will be given in this paper.

Published

2010

33. Geochemical atlases of Europe produced by the EuroGeoSurveys Geochemistry Expert Group: state of progress and potential uses

Author

DEMETRIADES A., REIMANN C., BIRKE M., SALMINEN R., DE VOS W., TARVAINEN, T., THE EUROGEOSURVEYS GEOCHEMISTRY EXPERT G.R.O.U.P. members of the EuroGeoSurveys Geochemistry Expert Group, Austria: Albert Schedl, Heinz Reitner, Edith Haslinger, Peter Filzmoser, Belgium: Walter De Vos, Bosnia, Herzegovina: Hazim Hrvatovic, Neven Miosic, Ferid Skopljak, Natalija Samardzic, Bulgaria: Valeri Trendavilov, Croatia: Josip Halami, 263, Ajka Šorša, Stjepan Husnjak, Czech Republic: Miloslav Duris, Cyprus: Zomenia Zomeni, Denmark: Vibeke Ernstsen, Estonia: Jaan Kivisilla, Walter Petersell, Finland: Timo Tarvainen, Mikael Eklund, France: Ignace Salpeteur, F. Y. R. O. M. : Trajce Stafilov, Germany: Manfred Birke, Rainer Hoffmann, Jens Utermann, Hellas: Alecos Demetriades, Hungary: Gyozo Jordan, Ubul Fugedi, Laszlo Kuti, Ireland: Patrick O’Connor, Fionnuala Ni Mhairtin, Vincent Gallagher, Italy: Benedetto De Vivo, Annamaria Lima, Stefano Albanese, Domenico Cicchella, Paolo Valera, Latvia: Aivars Gilucis, Lithuania: Virgilija Gregorauskiene, Luxembourg: Robert Maquil, Netherlands, The: Gerben Mol, Norway: Clemens Reimann, Rolf Tore Ottesen, Tore Volden, Ola A. Eggen, Arnold Arnoldussen, Poland: Anna Pasieczna, Aleksandra Dusza, Pawe, #322, Kwecko, Portugal: Maria Joao Batista, Cátia Prazeres, Serbia: Aleksandra Gulan, Dragana Vidojevi, Slovakia: Igor Slaninka, Peter Sefcik, Daniela Mackovych, Silvester Pramuka, Slovenia: Mateja Gosar, Spain: Juan Locutura, Alejandro Bel lan, Sweden: Madelen Andersson, Kaj Lax, Switzerland: Peter Hayoz, Reto Giulio Meuli, Ukraine: Boris I. Malyuk, Volodymyr Klos, United Kingdom: Dee Flight, Andreas Scheib, Mick Strutt, Paul McDonnell, DINELLI, ENRICO, DEMETRIADES A., REIMANN C., BIRKE M., SALMINEN R., DE VOS W., TARVAINEN, T. and THE EUROGEOSURVEYS GEOCHEMISTRY EXPERT GROUP. members of the EuroGeoSurveys Geochemistry Expert Group, Austria: Albert Schedl, Heinz Reitner, Edith Haslinger, Peter Filzmoser, Belgium: Walter De Vo, Bosnia & Herzegovina: Hazim Hrvatovic, Neven Miosic, Ferid Skopljak, Natalija Samardzic, Bulgaria: Valeri Trendavilov, Croatia: Josip Halami&#263, Ajka Šorša, Stjepan Husnjak, Czech Republic: Miloslav Duri, Cyprus: Zomenia Zomeni, Denmark: Vibeke Ernstsen, Estonia: Jaan Kivisilla, Walter Petersell, Finland: Timo Tarvainen, Mikael Eklund, France: Ignace Salpeteur, F.Y.R.O.M.: Trajce Stafilov, Germany: Manfred Birke, Rainer Hoffmann, Jens Utermann, Hellas: Alecos Demetriade, Hungary: Gyozo Jordan, Ubul Fugedi, Laszlo Kuti, Ireland: Patrick O’Connor, Fionnuala Ni Mhairtin, Vincent Gallagher, Italy: Benedetto De Vivo, Annamaria Lima, Stefano Albanese, Enrico Dinelli, Domenico Cicchella, Paolo Valera, Latvia: Aivars Giluci, Lithuania: Virgilija Gregorauskiene, Luxembourg: Robert Maquil, Netherlands, The: Gerben Mol, Norway: Clemens Reimann, Rolf Tore Ottesen, Tore Volden, Ola A. Eggen, Arnold Arnoldussen, Poland: Anna Pasieczna, Aleksandra Dusza, Pawe&#322, Kwecko, Portugal: Maria Joao Batista, Cátia Prazere, Serbia: Aleksandra Gulan, Dragana Vidojevi&#263, Slovakia: Igor Slaninka, Peter Sefcik, Daniela Mackovych, Silvester Pramuka, Slovenia: Mateja Gosar, Spain: Juan Locutura, Alejandro Bel-lan, Sweden: Madelen Andersson, Kaj Lax, Switzerland: Peter Hayoz, Reto Giulio Meuli, Ukraine: Boris I. Malyuk, Volodymyr Klo, and United Kingdom: Dee Flight, Andreas Scheib, Mick Strutt, Paul McDonnell.

Subjects

EUROPE, harmonisation of method, stream water, GROUND WATER, REACH, INSPIRE, geochemical atlas, overbank sediment, bottled water, floodplain sediment, soil

Abstract

An ‘Atlas’is a collection of maps usually published in a book form. A ‘Geochemical Atlas’is a thematic special purpose atlas with maps describing the geographical distribution of chemical elements and other physico-chemical parameters in different natural sample media, such as stream sediment, overbank or floodplain sediment, stream water, ground water, soil, plants, etc. Because our standard of living and health depend closely on the chemistry of near-surface materials, such atlases that provide data on the state of our environment are important for policy and decision makers, but also for researchers and citizens alike. The EuroGeoSurveys Geochemistry Expert Group is dedicated to provide harmonised multi-purpose geochemical data bases, and has already published the Geochemical Atlas of Europe, and is in the process of preparing the Atlas of Ground water eochemistry of Europe, and the Atlas of Agricultural and Grazing Land Soils. An important aspect is that all raw data, quality control information, statistics, maps and interpretation texts are freely available for downloading through the internet.

Published

2010

34. Improving the diagnostic accuracy of depression in older persons: the Depression in the Aged Female National Evaluation cluster randomized trial

Author

Lattanzio F, Di Bari M, Sgadari A, Baccini M, Ercolani S, Senin U, Bernabei R, Marchionni N, Cherubini A, Depression in the Aged Female National Evaluation Study G.r.o.u.p., RENGO, FRANCO, Lattanzio, F, Di Bari, M, Sgadari, A, Baccini, M, Ercolani, S, Rengo, Franco, Senin, U, Bernabei, R, Marchionni, N, Cherubini, A, and Depression in the Aged Female National Evaluation Study, G. r. o. u. p.

Abstract

OBJECTIVES: To evaluate whether a training intervention can improve the ability of geriatricians to recognize depression in older persons. DESIGN: Multicenter, cluster randomized clinical trial. SETTING: Fourteen geriatric outpatient clinics in Italy, each representing the unit of randomization. PARTICIPANTS: After training, a total of 1,914 outpatients aged 65 years and older in both arms, not on antidepressant at entry, were blindly evaluated by the clinic geriatrician, in charge of routine clinical management, and by a field researcher, who formally diagnosed depression by the Diagnostic and Statistical Manual of Mental Disorders, Fourth Edition (DSM-IV), taken as the criterion standard. INTERVENTION: After randomization, geriatricians belonging to the intervention arm were assigned to receive a residential 3-day educational program on depression. Those in the control arm received a generic course on disease management in elderly people. MEASUREMENTS: Sensitivity and specificity of the diagnosis of depression made by geriatricians, compared with the DSM-IV diagnosis. RESULTS: Sensitivity and specificity were significantly higher in trained than in untrained geriatricians (49 vs 35% and 91 vs 88%, respectively; P=.002 in marginal regression models). Effectiveness of training was confirmed, adjusting for age, sex, and cognitive performance (P=.02). CONCLUSION: The ability of geriatricians to diagnose depression in older outpatients can be improved with a specific training intervention. Improvement of diagnostic performance might translate into more-appropriate clinical management.

Published

2009

35. Predictability of sustained virological response to pegylated interferon alpha-2b Plus ribavirin therapy by week-8 viral response in HIV-positive patients with chronic hepatitis C virus infection

Author

Angeli E, Mainini A, Cargnel A, Uberti Foppa C, Orani A, Carbone R, Andreoni M, Schiavini M, Giorgi R, Rizzardini G, Gubertini G, ICoS 2 G.r.o.u.p. Azzini M, Mian P, Pristerà R, Quirino T, Sagnelli E, Pizzigallo E, Dalessandro M, Ghinelli F, Sighinolfi L, Leoncini F, Ambu S, Cancellieri C, Di Cesare S, Pagano G, Dodi F, Di Biagio A, Cassola G, Piscopo R, Benedetti M, Moroni M, Milazzo L, Lazzarin A, D'Arminio Monforte A, Bongiovanni M, Ferrari C, Degli Antoni A, Alberici F, Sacchini D, Menichetti F, Polidori M, Magnani G, Ursitti MA, Antonucci G, Rosati S, Narciso P, Bellagamba R, Babudieri S, Maida I, Grossi P, Tambini R., SAGNELLI, Caterina, Angeli, E, Mainini, A, Cargnel, A, Uberti Foppa, C, Orani, A, Carbone, R, Andreoni, M, Schiavini, M, Giorgi, R, Rizzardini, G, Gubertini, G, Azzini M, ICoS 2 G. r. o. u. p., Mian, P, Pristerà, R, Quirino, T, Sagnelli, E, Pizzigallo, E, Dalessandro, M, Ghinelli, F, Sighinolfi, L, Leoncini, F, Ambu, S, Cancellieri, C, Di Cesare, S, Pagano, G, Dodi, F, Di Biagio, A, Cassola, G, Piscopo, R, Benedetti, M, Moroni, M, Milazzo, L, Lazzarin, A, Sagnelli, Caterina, D'Arminio Monforte, A, Bongiovanni, M, Ferrari, C, Degli Antoni, A, Alberici, F, Sacchini, D, Menichetti, F, Polidori, M, Magnani, G, Ursitti, Ma, Antonucci, G, Rosati, S, Narciso, P, Bellagamba, R, Babudieri, S, Maida, I, Grossi, P, and Tambini, R.

Abstract

Chronic hepatitis C is frequent and aggressive in HIV-positive patients. Identification of early predictors of response to anti-HCV therapy is needed for a lower rate of response and higher discontinuations, compared to HCV mono-infected subjects. The aim of our study was to evaluate the predictive value of virological response (VR) at week 4-8-12 of Pegylated interferon alpha-2b (PEG-IFN) plus ribavirin (RBV) on sustained virological response (SVR) in HIV-HCV co-infected patients. 100 patients were treated with PEG-IFN (1.5 mcg/Kg/w) plus RBV (> or =10.6 mg/kg/d) and randomized for 24-48 or 48-72 weeks, respectively for genotype 2-3 and 1-4, in case of response (HCV-RNA PCR negativity) at the end of standard therapy (24 weeks for genotype 2-3, 48 weeks for genotype 1-4). Transcription-Mediated Amplification (TMA) assay for HCV-RNA was also applied. 27 patients reached end-of-treatment response (9 genotype 1-4, 18 genotype 2-3), 21 achieved SVR (8 genotype 1-4, 13 genotype 2-3). 35 patients dropped, 15 due to side-effects. SVR was statistically related to lower baseline HCV-RNA and to VR at week 4-8-12, with PPV 64%, 53% and 58%, and NPV 81%, 96% and 88%, respectively. In 27 patients, TMA was performed and confirmed standard PCR, except in two cases of relapse, who were PCR negative but TMA positive at week-12. In conclusion, VR at week 8 showed the highest NPV on SVR (96%). The study of viral kinetics requires further investigations in HIV-positive patients to guarantee a cost-effective therapy and to guide individually the duration of treatment. In this setting, TMA might be useful.

Published

2009

36. The Italian AICE-Genetics hemophilia A database: results and correlation with clinical phenotype

Author

MARGAGLIONE M., CASTAMAN G., MORFINI M., ROCINO A., SANTAGOSTINO E., TAGARIELLO G., TAGLIAFERRI A.R., ZANON E., BICOCCHI M. P., CASTALDO, GIUSEPPE, PEYVANDI F., SANTACROCE R., TORRICELLI F., GRANDONE E., MANNUCCI P.M., AICE GENETICS STUDY G.R.O.U.P., Margaglione, M., Castaman, G., Morfini, M., Rocino, A., Santagostino, E., Tagariello, G., Tagliaferri, A. R., Zanon, E., Bicocchi, M. P., Castaldo, Giuseppe, Peyvandi, F., Santacroce, R., Torricelli, F., Grandone, E., Mannucci, P. M., and AICE GENETICS STUDY, G. R. O. U. P.

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Genotype, Genetic counseling, Nonsense mutation, DNA Mutational Analysis, Biology, computer.software_genre, Hemophilia A, Denaturing high performance liquid chromatography, hemic and lymphatic diseases, Internal medicine, Databases, Genetic, medicine, Coagulopathy, Missense mutation, Humans, Registries, Codon, Chromatography, High Pressure Liquid, Genetics, Hematology, Factor VIII, Database, Blood Coagulation Factor Inhibitors, Models, Genetic, Point mutation, medicine.disease, Null allele, Introns, Phenotype, Italy, frequency, Mutation, computer, F8C gene mutation

Abstract

Background The high mutational heterogeneity of hemophilia A is a challenge for the provision of genetic services. We plan to identify the mutation in patients with hemophilia A in order to create a confidential national database of mutations for the optimization of genetic services in Italy. Design and Methods The factor VIII gene ( F8 ) was analyzed in 1296 unrelated patients with hemophilia A using screening methods for intron 22 and 1 inversions and rare mutations (denaturing high performance liquid chromatography, conformation sensitive gel electrophoresis) and/or direct sequencing. Results F8 mutations were identified in 874 (89%), 146 (89%), and 133 (94%) families with severe, moderate, or mild hemophilia A, respectively. Mutations predicting a null allele were responsible for 80%, 15%, and less than 1% of cases of severe, moderate, or mild hemophilia A, respectively. About 40% of missense and nonsense mutations occurred at a CpG site, arginines being most frequently affected. Of the small deletions or insertions, 29% occurred at one of two stretches of adenines, codons 1191–1194 (8As) and 1439–1441 (9As). Overall, these “hotspots” accounted for 31% of the point mutations in the patients with hemophilia A. Inhibitors developed in 22% of the patients with severe hemophilia A, 8% of those with moderate disease and in 4% of patients with mild hemophilia A. Patients who had severe hemophilia A and mutations predicting a null allele developed inhibitors more frequently (22 to 67%) than patients with missense mutations (5%). Conclusions We report a wide spectrum of mutations in a large national database. The type of mutation was a strong predictor of the clinical phenotype. This database is expected to considerably improve the genetic counselling and medical care of families with hemophilia A in Italy.

Published

2008

37. The association of telomere length with paternal history of premature myocardial infarction in the European Atherosclerosis Research Study II

Author

Salpea KD, Nicaud V, Tiret L, Talmud PJ, Humphries SE, EARS II g.r.o.u.p., FARINARO, EDUARDO, Salpea, Kd, Nicaud, V, Tiret, L, Talmud, Pj, Humphries, Se, EARS II, g. r. o. u. p., and Farinaro, Eduardo

Published

2008

38. Survey of European programmes for the epidemiological surveillance of congenital toxoplasmosis

Author

Bénard A, Petersen E, Salamon R, Chêne G, Gilbert R, Salmi LR, European Toxo Prevention Study G.r.o.u.p., BUFFOLANO, WILMA, Bénard, A, Petersen, E, Salamon, R, Chêne, G, Gilbert, R, Salmi, Lr, Buffolano, Wilma, and European Toxo Prevention Study, G. r. o. u. p.

Published

2008

39. IGG practice guidelines on germ cell tumor in adult male patients

Author

De Giorgi U, Nicolai N, Tana S, Tavolini IM, Palazzi S, Bracarda S, Tedeschi L, Frassineti L, Da Pozzo L, Pastorino U, Emiliani E, Marangolo M, Pizzocaro G, Rosti G, Salvioni R, Italian Germ cell cancer G.r.o.u.p., PALMIERI, GIOVANNELLA, De Giorgi, U, Nicolai, N, Tana, S, Tavolini, Im, Palazzi, S, Bracarda, S, Tedeschi, L, Palmieri, Giovannella, Frassineti, L, Da Pozzo, L, Pastorino, U, Emiliani, E, Marangolo, M, Pizzocaro, G, Rosti, G, Salvioni, R, and Italian Germ cell cancer, G. r. o. u. p.

Published

2008

40. Effectiveness of health education on Toxoplasma-related knowledge, behaviour, and risk of seroconversion in pregnancy

Author

Gollub EL, Leroy V, Gilbert R, Chêne G, Wallon M, European Toxoprevention Study G.r.o.u.p., BUFFOLANO, WILMA, Gollub, El, Leroy, V, Gilbert, R, Chêne, G, Wallon, M, Buffolano, Wilma, and European Toxoprevention Study, G. r. o. u. p.

Published

2008

41. Red flags for multiple system atrophy

Author

Köllensperger M, Geser F, Seppi K, Stampfer Kountchev M, Sawires M, Scherfler C, Boesch S, Mueller J, Koukouni V, Quinn N, Pellecchia MT, Schimke N, Dodel R, Oertel W, Dupont E, Østergaard K, Daniels C, Deuschl G, Gurevich T, Giladi N, Coelho M, Sampaio C, Nilsson C, Widner H, Sorbo FD, Albanese A, Cardozo A, Tolosa E, Abele M, Klockgether T, Kamm C, Gasser T, Djaldetti R, Colosimo C, Meco G, Schrag A, Poewe W, Wenning GK, European MSA Study G.r.o.u.p., BARONE, PAOLO, Köllensperger, M, Geser, F, Seppi, K, Stampfer Kountchev, M, Sawires, M, Scherfler, C, Boesch, S, Mueller, J, Koukouni, V, Quinn, N, Pellecchia, Mt, Barone, Paolo, Schimke, N, Dodel, R, Oertel, W, Dupont, E, Østergaard, K, Daniels, C, Deuschl, G, Gurevich, T, Giladi, N, Coelho, M, Sampaio, C, Nilsson, C, Widner, H, Sorbo, Fd, Albanese, A, Cardozo, A, Tolosa, E, Abele, M, Klockgether, T, Kamm, C, Gasser, T, Djaldetti, R, Colosimo, C, Meco, G, Schrag, A, Poewe, W, Wenning, Gk, and European MSA Study, G. r. o. u. p.

Published

2008

42. Detection of growth hormone abuse in sport. Powrie JK, Bassett EE, Rosen T, Jørgensen JO, Napoli R, Sacca L, Christiansen JS, Bengtsson BA, Sönksen PH; GH-2000 Project Study Group

Author

Powrie JK, Bassett EE, Rosen T, Jørgensen JO, Christiansen JS, Bengtsson BA, Sönksen PH, GH 2000 Project Study G.r.o.u.p., NAPOLI, RAFFAELE, SACCA', LUIGI, Powrie, Jk, Bassett, Ee, Rosen, T, Jørgensen, Jo, Napoli, Raffaele, Sacca', Luigi, Christiansen, J, Bengtsson, Ba, Sönksen, Ph, and GH 2000 Project Study, G. r. o. u. p.

Abstract

Objective: To develop a test for GH abuse in sport.Design: A double blind placebo controlled study of one month's GH administration to 102 healthy non-competing but trained subjects. Blood levels of nine markers of GH action were measured throughout the study and for 56 days after cessation of GH administration. Blood samples were also taken from 813 elite athletes both in and out of competition.Results: GH caused a significant change in the nine measured blood markers. Men were more sensitive to the effects of GH than women. IGF-I and N-terminal extension peptide of procollagen type III were selected to construct formulae which gave optimal discrimination between the GH and placebo groups. Adjustments were made to account for the fall in IGF-I and P-III-P with age and the altered distribution seen in elite athletes. Using a cut-off specificity of 1: 10,000 these formulae would allow the detection of up to 86% of men and 60% of women abusing GH at the doses used in this study.Conclusions: We report a methodology that will allow the detection of GH abuse. This will provide the basis of a robust and enforceable test identifying those who are already cheating and provide a deterrent to those who may be tempted to do so.

Published

2007

43. CARE OF GIRLS AND WOMEN WITH TURNER SYNDROME: A GUIDLINE OF THE TURNER SYNDROME STUDY GROUP

Author

TURNER SYNDROME STUDY G.R.O.U.P. Bondy CA, Turner Sindrome Study Group: Turner Sindrome Consensus Study Group: Neus Baena, V. K. Bakalov, B. B. Biesecker, J. C. Carel, G. Conway, M. Davenport, C. Disteche, M. F. Karnis, J. A. Germak, C. H. Gravholt, J. Foodim, D. Gunther, O. Hovatta, A. M. Kappelgard, W. Kiess, K. Landin Wilhelmsen, A. Lin, B. Lippe, M. Loscalzo, K. Lynch, M. M. M. Mazzocco, E. McCauley, P. McDonough, S. M. P. F. de Muinck Keizer Schrama, R. W. Naeraa, C. Quigley, R. Rosenfield, D. Rosing, J. Ross, D. Roulot, K. Rubin, P. Saenger, P. Schmidt, M. Silberbach, V. Sybert, D. L. Van Dyke, A. Zinn, MAZZANTI, LAURA, TURNER SYNDROME STUDY GROUP. Bondy CA and Turner Sindrome Study Group: Turner Sindrome Consensus Study Group: Neus Baena, V. K. Bakalov, B.B. Biesecker, J.C. Carel, G.Conway, M. Davenport, C. Disteche, M. F. Karni, J. A. Germak, C.H. Gravholt, J. Foodim, D. Gunther, O. Hovatta, A.M. Kappelgard, W. Kie, K. Landin-Wilhelmsen, A. Lin, B. Lippe, M. Loscalzo, K. Lynch, L. Mazzanti, M. M. M. Mazzocco, E. McCauley, P. McDonough, S.M.P.F. de Muinck Keizer-Schrama, R. W. Naeraa, C. Quigley, R. Rosenfield, D. Rosing, J. Ro, D. Roulot, K. Rubin, P. Saenger, P. Schmidt, M. Silberbach, V. Sybert, D. L. Van Dyke, and A. Zinn.

Subjects

Adult, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, media_common.quotation_subject, Clinical Biochemistry, MEDLINE, Turner Syndrome, Biochemistry, Bone and Bones, Child health, Presentation, Cognition, Neonatal Screening, Endocrinology, Multidisciplinary approach, Prenatal Diagnosis, Internal medicine, Turner syndrome, Good evidence, medicine, Humans, Child, media_common, Web site, business.industry, Liver Diseases, Estrogen Replacement Therapy, Puberty, Biochemistry (medical), Infant, Newborn, Guideline, medicine.disease, Fertility, Cardiovascular Diseases, Female, business, GROWTH-HORMONE TREATMENT, SEX-CHROMOSOME ABNORMALITIES, LERI-WEILL DYSCHONDROSTEOSIS, CARDIOVASCULAR RISK-FACTORS, CONGENITAL HEART-DISEASE, RANDOMIZED DOSE-RESPONSE, PULMONARY VENOUS RETURN, POPULATION-BASED COHORT, BONE-MINERAL DENSITY, QUALITY-OF-LIFE

Abstract

Objectives: The objective of this work is to provide updated guidelines for the evaluation and treatment of girls and women with Turner syndrome (TS). Participants: The Turner Syndrome Consensus Study Group is a multidisciplinary panel of experts with relevant clinical and research experience with TS that met in Bethesda, Maryland, April 2006. The meeting was supported by the National Institute of Child Health and unrestricted educational grants from pharmaceutical companies. Evidence: The study group used peer-reviewed published information to form its principal recommendations. Expert opinion was used where good evidence was lacking. Consensus: The study group met for 3 d to discuss key issues. Breakout groups focused on genetic, cardiological, auxological, psychological, gynecological, and general medical concerns and drafted recommendations for presentation to the whole group. Draft reports were available for additional comment on the meeting web site. Synthesis of the section reports and final revisions were reviewed by e-mail and approved by whole-group consensus. Conclusions:Wesuggest that parents receiving a prenatal diagnosis of TS be advised of the broad phenotypic spectrum and the good quality of life observed in TS in recent years. We recommend that magnetic resonance angiography be used in addition to echocardiography to evaluate the cardiovascular system and suggest that patients with defined cardiovascular defects be cautioned in regard to pregnancy and certain types of exercise. We recommend that puberty should not be delayed to promote statural growth. We suggest a comprehensive educational evaluation in early childhood to identify potential attention-deficit or nonverbal learning disorders. We suggest that caregivers address the prospect of premature ovarian failure in an open and sensitive manner and emphasize the critical importance of estrogen treatment for feminization and for bone health during the adult years. All individuals with TS require continued monitoring of hearing and thyroid function throughout the lifespan. We suggest that adults with TS be monitored for aortic enlargement, hypertension, diabetes, and dyslipidemia. (J Clin Endocrinol Metab 92: 10–25, 2007) TURNER SYNDROME (TS) affects approximately one in 2500 live-born females (1). This disorder presents the clinician with a challenging array of genetic, developmental, endocrine, cardiovascular, psychosocial, and reproductive issues. There have been important advances in each of these arenas since publication of the previous recommendations for the care of girls and women with TS (2). This paper is based on the proceedings of a multidisciplinary international conference sponsored by the National Institute of Child Health and Human Development (NICHD) in April 2006. Discussions at this conference and the ensuing recommendations have been based upon recent, peer-reviewed scientific publications. However, there are very few TS studies that would qualify as guidance for evidence-based recommendations, and hence

Published

2007

44. Progression of multiple system atrophy (MSA): a prospective natural history study by the European MSA Study Group (EMSA SG)

Author

Geser F, Wenning GK, Seppi K, Stampfer Kountchev M, Scherfler C, Sawires M, Frick C, Ndayisaba JP, Ulmer H, Pellecchia MT, Kim HT, Hooker J, Quinn NP, Cardozo A, Tolosa E, Abele M, Klockgether T, Østergaard K, Dupont E, Schimke N, Eggert KM, Oertel W, Djaldetti R, Poewe W, the European MSA Study G.r.o.u.p., BARONE, PAOLO, Geser, F, Wenning, Gk, Seppi, K, Stampfer Kountchev, M, Scherfler, C, Sawires, M, Frick, C, Ndayisaba, Jp, Ulmer, H, Pellecchia, Mt, Barone, Paolo, Kim, Ht, Hooker, J, Quinn, Np, Cardozo, A, Tolosa, E, Abele, M, Klockgether, T, Østergaard, K, Dupont, E, Schimke, N, Eggert, Km, Oertel, W, Djaldetti, R, Poewe, W, and the European MSA Study, G. r. o. u. p.

Published

2006

45. Mutational analysis of the PINK1 gene in early-onset parkinsonism in Europe and North Africa

Author

IBANEZ P, LESAGE S, LOHMANN E, THOBOIS S, BORG M, AGID Y, DURR, A, BRICE A, FRENCH PARKINSON'S DISEASE GENETICS STUDY G.R.O.U.P., DE MICHELE, GIUSEPPE, Ibanez, P, Lesage, S, Lohmann, E, Thobois, S, DE MICHELE, Giuseppe, Borg, M, Agid, Y, Durr, A, Brice, A, and FRENCH PARKINSON'S DISEASE GENETICS STUDY, G. R. O. U. P.

Published

2006

46. The Beckwith-Wiedemann Syndrome: genetic and epigenetic defects in bipartite cluster of imprintend genes

Author

DELLA CASA, ROBERTO, SEBASTIO G., MELIS D., MAJO F., TENCONI R., SILENGO M., RINALDI M. M., SPARAGO A., CERRATO F., RICCIO A. END ITALIAN BWS STUDY G.R.O.U.P., DELLA CASA, Roberto, Sebastio, G., Melis, D., Majo, F., Tenconi, R., Silengo, M., Rinaldi, M. M., Sparago, A., Cerrato, F., and Riccio, A. END ITALIAN BWS STUDY G. R. O. U. P.

Published

2005

47. Quality of life and disability assessment in neuropathy: a multicentre study

Author

Padua L, Schenone A, Aprile I, Benedetti L, Caliandro P, Tonali P, Orazio EN, Italian NEUROPA Study G.r.o.u.p., SANTORO, LUCIO, Padua, L, Schenone, A, Aprile, I, Benedetti, L, Caliandro, P, Tonali, P, Orazio, En, Italian NEUROPA Study, G. r. o. u. p., and Santoro, Lucio

Published

2005

48. A randomised factorial trial of sequential doxorubicin and CMF vs CMF and chemotherapy alone vs chemotherapy followed by goserelin plus tamoxifen as adjuvant treatment of node-positive breast cancer

Author

DE PLACIDO, SABINO, DE LAURENTIIS, MICHELINO, LAURIA, ROSSELLA, PETRELLA, GIUSEPPE, LIMITE, GENNARO, COSTANZO, RAFFAELE, DE LENA M, LORUSSO V, PARADISO A, D'APRILE M, PISTILLUCCI G, FARRIS A, SAROBBA MG, PALAZZO S, MANZIONE L, ADAMO V, PALMERI S, FERRAU F, PAGLIARULO C, BIANCO AR, GOCSI COOPERATIVE G.R.O.U.P., DE PLACIDO, Sabino, DE LAURENTIIS, Michelino, DE LENA, M, Lorusso, V, Paradiso, A, D'Aprile, M, Pistillucci, G, Farris, A, Sarobba, Mg, Palazzo, S, Manzione, L, Adamo, V, Palmeri, S, Ferrau, F, Lauria, Rossella, Pagliarulo, C, Petrella, Giuseppe, Limite, Gennaro, Costanzo, Raffaele, Bianco, Ar, and GOCSI COOPERATIVE, G. R. O. U. P.

Abstract

The sequential doxorubicin --> CMF (CMF=cyclophosphamide, methotrexate, fluorouracil) regimen has never been compared to CMF in a randomised trial. The role of adding goserelin and tamoxifen after chemotherapy is unclear. In all, 466 premenopausal node-positive patients were randomised to: (a) CMF x 6 cycles (CMF); (b) doxorubicin x 4 cycles followed by CMF x 6 cycles (A --> CMF); (c) CMF x 6 cycles followed by goserelin plus tamoxifen x 2 years (CMF --> GT); and (d) doxorubicin x 4 cycles followed by CMF x 6 cycles followed by goserelin plus tamoxifen x 2 years (A --> CMF --> GT). The study used a 2 x 2 factorial experimental design to assess: (1) the effect of the chemotherapy regimens (CMF vs A --> CMF or arms a+c vs b+d) and (2) the effect of adding GT after chemotherapy (arms a+b vs c+d). At a median follow-up of 72 months, A --> CMF as compared to CMF significantly improved disease-free survival (DFS) with a multivariate hazard ratio (HR)=0.740 (95\% confidence interval (CI): 0.556-0.986; P=0.040) and produced a nonsignificant improvement of overall survival (OS) (HR=0.764; 95\% CI: 0.489-1.193). The addition of GT after chemotherapy significantly improved DFS (HR=0.74; 95\% CI: 0.555-0.987; P=0.040), with a nonsignificant improvement of OS (HR=0.84; 95\% CI: 0.54-1.32). A --> CMF is superior to CMF. Adding GT after chemotherapy is beneficial for premenopausal node-positive patients..

Published

2005

49. Prevalence, risk factors and cardiovascular comorbidity of symptomatic peripheral arterial disease in Italy

Author

BREVETTI G, OLIVA G, SILVESTRO A, SCOPACASA F, PERIPHERAL ARTERIOPATHY AND CARDIOVASCULAR EVENTS PACE STUDY G.R.O.U.P., CHIARIELLO, MASSIMO, Brevetti, G, Oliva, G, Silvestro, A, Scopacasa, F, Chiariello, Massimo, and PERIPHERAL ARTERIOPATHY AND CARDIOVASCULAR EVENTS PACE STUDY, G. R. O. U. P.

Published

2004

50. Inflammatory bowel disease and hospital treatment in Italy: the RING multi-centre study

Author

SONCINI M, TRIOSSI O, LEO P, MAGNI G. ON BEHALF OF THE RING STUDY G.R.O.U.P. CATTEDRA DI GASTROENTEROLOGIA, II UNIVERSITA' DI NAPOLI DEL VECCHIO BLANCO C, FEDERICO, Alessandro, Soncini, M, Triossi, O, Leo, P, CATTEDRA DI GASTROENTEROLOGIA, MAGNI G. ON BEHALF OF THE RING STUDY G. R. O. U. P., II UNIVERSITA' DI NAPOLI DEL VECCHIO BLANCO, C, and Federico, Alessandro

Published

2004