Marino L
University of Palermo
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Annals of Internal Medicine | 1992
Rosa Giovanna Simonetti; Calogero Cammà; Felice Fiorello; Mario Cottone; Maria Rapicetta; Marino L; Germana Fiorentino; A. Craxì; A.R. Ciccaglione; Roberto Giuseppetti; Tommaso Stroffolini; Luigi Pagliaro
OBJECTIVE To determine whether chronic hepatitis C virus (HCV) infection is an independent risk factor for hepatocellular carcinoma and whether it increases the cirrhosis-related risk for hepatocellular carcinoma. DESIGN Two pair-matched case-control studies. SETTING A referral-based hospital. PATIENTS In study I, 212 patients with hepatocellular carcinoma (197 of whom had known underlying cirrhosis) were compared with controls who had chronic nonhepatic diseases. In study II, the 197 patients with hepatocellular carcinoma and cirrhosis were compared with 197 pair-matched controls who had cirrhosis but not hepatocellular carcinoma. MEASUREMENTS Levels of antibody to HCV (anti-HCV), hepatitis B surface antigen (HBsAg), and antibody to hepatitis B core antigen (anti-HBc) were assayed, and alcohol abuse was assessed by history. MAIN RESULTS In study I, 151 patients (71%) with hepatocellular carcinoma were anti-HCV positive compared with 11 controls (5%) with chronic nonhepatic diseases (odds ratio, 42; 95% CI, 22 to 95). Multivariate analysis showed that anti-HCV was an independent risk factor for hepatocellular carcinoma (odds ratio, 69; CI, 15 to 308). The analysis also showed that HBsAg (odds ratio, 8.7; CI, 1.5 to 50) and anti-HBc (odds ratio, 4.2 (CI, 1.7 to 11) were risk factors for hepatocellular carcinoma. No statistically significant interaction was found between anti-HCV and the markers of HBV infection. In study II, 146 patients (74%) with hepatocellular carcinoma and cirrhosis were anti-HCV positive compared with 122 patients (62%) with cirrhosis alone (odds ratio, 1.8; CI, 1.1 to 2.8). Multivariate analysis confirmed that anti-HCV (odds ratio, 2.0; CI, 1.3 to 32) and HBsAg (odds ratio, 2.0; CI, 1.0 to 4.2) were independent risk factors for hepatocellular carcinoma. CONCLUSIONS Hepatitis C virus infection is a risk factor for hepatocellular carcinoma, apparently by inducing cirrhosis and, to a lesser extent, by enhancing the risk in patients with cirrhosis. Hepatitis C virus infection acts independently of HBV infection (another risk factor) and of alcohol abuse, age, or gender.
Gut | 1993
Giuseppe Provenzano; Orazia Diquattro; A. Craxì; P.L. Almasio; G.B. Pinzello; Marino L; Germana Fiorentino; Fortunato Rinaldi; Luigi Pagliaro
Primary biliary cirrhosis is characterised by the presence of antimitochondrial antibodies which are directed against components of mitochondrial dehydrogenase complexes. The specificity of antimitochondrial antibodies for primary biliary cirrhosis as detected by immunoblotting was investigated. Commercially available preparations of pyruvate and oxo-glutarate dehydrogenases and beef-heart mitochondria were used as source of antigens. Sera from 47 primary biliary cirrhosis patients (46 of whom were antimitochondrial antibody positive by immunofluorescence), 16 non-primary biliary cirrhosis patients (antimitochondrial antibody positive by immunofluorescence), 23 liver-kidney microsomal antibody positive chronic active hepatitis patients, and 32 patients with connective tissue diseases were examined. Of the 47 subjects with primary biliary cirrhosis, 43 (91%) and 13 (28%) tested positive by immunoblotting for pyruvate and oxo-glutarate dehydrogenase, respectively. Only three primary biliary cirrhosis patients were negative for both antigens, including the only one shown to be antimitochondrial antibody negative by immunofluorescence. The other two patients were positive by immunoblotting with beef-heart mitochondria. In contrast, only three of 16 (19%) non-primary biliary cirrhosis patients who were antimitochondrial antibody positive by immunofluorescence tested positive by immunoblotting (for both pyruvate dehydrogenase and beef-heart mitochondria). None of the 23 liver-kidney microsomal antibody positive and the 32 patients with rheumatic diseases were positive by immunoblotting with any antigen. Our data show that immunoblotting with commercially available oxo-acid dehydrogenases is a reproducible method for the detection of antimitochondrial antibodies highly specific for primary biliary cirrhosis.
Hepatology | 1994
Silvio Magrin; A. Craxì; Carmelo Fabiano; Rosa Giovanna Simonetti; Germana Fiorentino; Marino L; Orazia Diquattro; Vito Di Marco; Oreste Loiacono; Riccardo Volpes; Piero Luigi Almasio; Mickey S. Urdea; Paul Neuwald; Ray Sanchez-Pescador; Jill Detmer; Judith C. Wilber; Luigi Pagliaro
Journal of Hepatology | 1996
Silvio Magrin; A. Craxì; Carmelo Fabiano; Marino L; Germana Fiorentino; Oreste Lo Iacono; Riccardo Volpes; Vito Di Marco; Piero Luigi Almasio; Alessandra Vaccaro; Mickey S. Urdea; Judith C. Wilber; Celestino Bonoura; Fabrizio Gianguzza; Vincenza Capursi; Salvatore Filiberti; Lieven Stuyver; Luigi Pagliaro
Journal of Medical Virology | 1992
Silvio Magrin; A. Craxì; Carmelo Fabiano; G. Fiorentino; Marino L; P.L. Almasio; G. Pinzello; U. Palazzo; M. Vitale; Aurelio Maggio; G. Bucca; Fabrizio Gianguzza; V. Shyamala; Jang Han; Luigi Pagliaro
The Lancet | 1991
A. Craxì; Germana Fiorentino; VitoDi Marco; Marino L; Silvio Magrin; Carmelo Fabriano; Luigi Pagliaro
Progress in Clinical and Biological Research | 1993
A. Craxì; Di Marco; Lo Iacono O; P.L. Almasio; Carmelo Fabiano; Germana Fiorentino; Marino L; Silvio Magrin; G.B. Pinzello; Sammarco S
The Italian journal of gastroenterology | 1991
A. Craxì; P.L. Almasio; Di Marco; Silvio Magrin; Raffaele Bruno; C. Cammà; Germana Fiorentino; Lo Jacono O; Marino L; U. Palazzo
Allergologia Et Immunopathologia | 1991
Giuseppe Provenzano; Marino L; A. Craxì
Bollettino dell'Istituto sieroterapico milanese | 1988
A. Craxì; Marino L; Aragona E; Patti C