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6. Influence of immunogenetic background on the outcome of recurrent hepatitis C after liver transplantation

Author

Belli, Luca Saverio, Zavaglia, Claudio, Alberti, Alberto Battista, Poli, Francesca, Rondinara, Gianfranco, Silini, Enrico, Taioli, Emanuela, De Carlis, Luciano, Scalamogna, Mario, Forti, Domenico, Pinzello, Giovambattista, Idèo, Gaetano, Belli, L, Zavaglia, C, Alberti, A, Poli, F, Rondinara, G, Silini, E, Taioli, E, De Carlis, L, Scalamogna, M, Forti, D, Pinzello, G, and Idèo, G

Subjects
Allele, Adult, Male, Hepatology, Histocompatibility Antigens Class I, Histocompatibility Antigens Class II, Middle Aged, Hepatitis C, Liver Transplantation, Immunogenetic, Postoperative Complications, Gene Frequency, Recurrence, Multivariate Analysis, Disease Progression, Immunogenetics, Humans, Female, Postoperative Complication, Multivariate Analysi, Alleles, Human
Abstract

In immunocompetent patients, specific human leukocyte antigen (HLA) class II alleles have been associated with the severity of hepatitis C virus (HCV)-related disease, in particular, HLA-DRBI* 1 I has been found to exert a protective effect. The authors have analyzed the role of HLA class I and II alleles in determining the frequency, timing, and progression of histologically proven recurrent hepatitis C in 89 patients who underwent a liver transplant for HCV-related cirrhosis. In addition, the influence of HLA mismatch between donor and recipient, HCV genotype, and use of steroid pulses was also evaluated. Median patient follow up was 35 months (range 4-119). HLA-DRBI typing was performed by genomic analysis in all cases. Liver biopsies were obtained routinely and at least at yearly intervals. Histologically proven recurrent hepatitis was observed in 46 patients (52%), 10 patients progressing to stage 5-6 fibrosis in most cases within 2 years after transplant. By univariate analysis, 3 variables, HLA-B14, HLA-DRB1*04, and HLA-DRB1 donor/recipient mismatch, showed a significant effect on time to recurrent hepatitis C disease. These parameters were included in a multivariate regression model along with HCV genotype, treatment with steroid pulses and DRB1*11. HLA-B14, HLA-DRBI*04, and HLA-DRBI donor/recipient mismatch were confirmed to provide a significant and independent contribution to the risk of hepatitic disease recurrence. As for the severity of the disease, none of the 10 patients with stage 5-6 hepatitis carried the HLA- DRBI*11 allele, in line with what was observed in nontransplant subjects. Our results suggest that in posttransplant recurrent hepatitis C, immunogenetic factors are relevant in determining HCV infection outcome

Published
2000

7. HLA-DRB1 donor-recipient mismatch affects the outcome of hepatitis C disease recurrence after liver transplantation

Author

Belli, L, Burra, P, Poli, F, Alberti, A, Silini, E, Zavaglia, C, Fagiuoli, S, Prando, D, Espadas De Arias, A, Boninsegna, S, Tinelli, C, Scalamogna, M, De Carlis, L, Pinzello, G, Belli, Luca Saverio, Burra, Patrizia, Poli, Francesca, Alberti, Alberto Battista, Silini, Enrico, Zavaglia, Claudio, Fagiuoli, Stefano, Prando, Daniela, Espadas De Arias, Alejandro, Boninsegna, Sara, Tinelli, Carmine, Scalamogna, Mario, De Carlis, Luciano, Pinzello, Giovambattista, Belli, L, Burra, P, Poli, F, Alberti, A, Silini, E, Zavaglia, C, Fagiuoli, S, Prando, D, Espadas De Arias, A, Boninsegna, S, Tinelli, C, Scalamogna, M, De Carlis, L, Pinzello, G, Belli, Luca Saverio, Burra, Patrizia, Poli, Francesca, Alberti, Alberto Battista, Silini, Enrico, Zavaglia, Claudio, Fagiuoli, Stefano, Prando, Daniela, Espadas De Arias, Alejandro, Boninsegna, Sara, Tinelli, Carmine, Scalamogna, Mario, De Carlis, Luciano, and Pinzello, Giovambattista

Abstract

Background & Aims: This study extends our previously reported observations that various immunological factors are associated with the occurrence of histologically proven recurrent hepatitis C. The two specific issues investigated were to confirm the associations of MHC alleles and donor/recipient mismatch with the occurrence of recurrent hepatitis C in an independent cohort of newly transplanted patients and to look for immunologic and nonimmunologic variables affecting the severity of the recurrent disease. Methods: Two separate cohorts of consecutive patients were studied: a look-back cohort (LC) of 120 patients and a cohort for studying the disease progression (CSDP) of 190 patients. Protocol liver biopsies were obtained at least 1, 3, 5, 7, and 10 years after liver transplantation (LT). Results: A fully mismatched donor/recipient pair at the DRB1 locus was confirmed to be associated with both the recurrence of histologic hepatitis in the LC (59% vs 23%, P = .0002) and its progression beyond stage 3 in the CSPD (71.4% vs 39.3%, P = .0003). Relevant immunologic and nonimmunologic variables were included into a multivariate Cox proportional model and three variables, namely, donor age, full HLA-DRB1 donor-recipient mismatch, and HLA B14, resulted in independent risk factors for the development of severe fibrosis. Conclusion: This study provides evidence that DRB1 donor-recipient mismatch affects both the occurrence and progression of recurrent hepatitis C disease. This information is clinically relevant as it may help to better allocate organs and to recognize patients at risk for progression so that specific interventions can be implemented. © 2006 by the American Gastroenterological Association Institute

Published
2006

8. Sequence variation in the hypervariable region 1 of hepatitis C virus and posttransplantation recurrent hepatitis

Author

Silini, E, Belli, L, Brambilla, S, Foti, L, Gritti, M, Lisa, A, Alberti, A, Vinci, M, De Carlis, L, Rondinara, G, Pinzello, G, Silini, Enrico, Belli, Luca, Brambilla, Sabrina, Foti, Luciana, GRITTI, MARIA CHIARA, Lisa, Antonella, Alberti, Alberto Battista, Vinci, Marilina, De Carlis, Luciano, Rondinara, Gianfranco, Pinzello, Giovanbattista, Silini, E, Belli, L, Brambilla, S, Foti, L, Gritti, M, Lisa, A, Alberti, A, Vinci, M, De Carlis, L, Rondinara, G, Pinzello, G, Silini, Enrico, Belli, Luca, Brambilla, Sabrina, Foti, Luciana, GRITTI, MARIA CHIARA, Lisa, Antonella, Alberti, Alberto Battista, Vinci, Marilina, De Carlis, Luciano, Rondinara, Gianfranco, and Pinzello, Giovanbattista

Abstract

Hepatitis C virus (HCV) shows remarkable genetic variation in both populations and individuals, in whom it circulates as quasispecies (QS). Sequence variation within an infected host has adaptive significance and reflects the modes and intensity of selection mechanisms operating on the virus. We investigated the sequence diversity of hypervariable region 1 of HCV in liver transplant recipients and correlated it with the recurrence of hepatitis. Twenty-six patients were considered during a 2-year period; all had graft reinfection, and 14 patients developed hepatitis recurrence. Cloned sequences were obtained from sera collected before or within 1 month after orthotopic liver transplantation (OLT) and at 3 and 24 months thereafter. Sequence diversity within single sera and over consecutive samples was analyzed quantitatively by matrix comparison and phylogenetic analysis. Propagation of viral QS in the graft was markedly dependent on individual factors. Viral QS in post-OLT sera were less complex and evolved slower compared with immunocompetent subjects with chronic hepatitis. Sequence variation was greater during the first 3 months post-OLT than during the remaining period. Genetic diversity within single samples was not related to hepatitis recurrence or other clinical features. Conversely, sequence diversity over consecutive samples was reduced in patients who experienced hepatitis recurrence, in particular, in those infected with genotype 1b and with an HLA-DR mismatched graft. Selection of viral sequences was markedly impaired in liver transplant recipients and tended to be greater early after OLT. Reduced sequence turnover correlated negatively with the outcome of graft reinfection

Published
2003

9. Combined therapy with interferon and low-dose ribavirin in posttransplantation recurrent hepatitis C: A pragmatic study

Author

Alberti, A, Belli, L, Airoldi, A, De Carlis, L, Rondinara, G, Minola, E, Vangeli, M, Cernuschi, A, D'Amico, M, Forti, D, Pinzello, G, Alberti, Alberto Battista, Belli, Luca Saverio, Airoldi, Aldo, De Carlis, Luciano, Rondinara, Gianfranco, Minola, Ernesto, Vangeli, Marcello, Cernuschi, Alessandra, D'Amico, Maria, Forti, Domenico, Pinzello, Giovambattista, Alberti, A, Belli, L, Airoldi, A, De Carlis, L, Rondinara, G, Minola, E, Vangeli, M, Cernuschi, A, D'Amico, M, Forti, D, Pinzello, G, Alberti, Alberto Battista, Belli, Luca Saverio, Airoldi, Aldo, De Carlis, Luciano, Rondinara, Gianfranco, Minola, Ernesto, Vangeli, Marcello, Cernuschi, Alessandra, D'Amico, Maria, Forti, Domenico, and Pinzello, Giovambattista

Abstract

Recurrent hepatitis C is a common problem after liver transplantation that can progress to liver cirrhosis of the graft. Preliminary reports of combination treatment with interferon (IFN) and ribavirin have been promising, but long-term follow-up data are not yet available. We report our experience with 1 year of combination therapy with IFN (3 million units thrice weekly) and low-dose ribavirin (600 mg/d), followed by long-term ribavirin monotherapy in 18 patients with moderate to severe recurrent hepatitis C and a median follow-up of 32 months after the completion of combined therapy. All patients were followed up clinically and histologically at regular intervals. Overall, in an intention-to-treat analysis, 15 patients had normal alanine aminotransferase levels (biochemical end-treatment response [ETR], 83%), and 8 patients were also hepatitis C virus RNA negative in serum (virological ETR, 44%) at the end of combined treatment. At last follow-up after the completion of combined therapy (median, 32 months; range, 18 to 73 months), 13 patients were biochemical responders (biochemical long term-sustained response [LT-SR], 72%), and 5 patients also maintained viral clearance (virological LT-SR, 27%). Comparison of liver biopsy specimens before and after 12 months of combined therapy showed improvement in grading scores of at least two points in the majority of the patients (73%). Notably, a trend toward fibrotic progression was only noted in nonresponders. Regarding side effects, despite the low dose of ribavirn, almost half the patients developed hemolytic anemia requiring dose reductions. In addition, long-term ribavirin monotherapy was not associated with iron accumulation. We conclude that combined therapy with low-dose ribavirin followed by long-term ribavirin monotherapy can be recommended because it favorably modifies the natural history of recurrent hepatitis C in most patients and possibly halts histological disease progression without causing iron accumula

Published
2001

10. Influence of immunogenetic background on the outcome of recurrent hepatitis C after liver transplantation

Author

Belli, L, Zavaglia, C, Alberti, A, Poli, F, Rondinara, G, Silini, E, Taioli, E, De Carlis, L, Scalamogna, M, Forti, D, Pinzello, G, Idèo, G, Belli, Luca Saverio, Zavaglia, Claudio, Alberti, Alberto Battista, Poli, Francesca, Rondinara, Gianfranco, Silini, Enrico, Taioli, Emanuela, De Carlis, Luciano, Scalamogna, Mario, Forti, Domenico, Pinzello, Giovambattista, Idèo, Gaetano, Belli, L, Zavaglia, C, Alberti, A, Poli, F, Rondinara, G, Silini, E, Taioli, E, De Carlis, L, Scalamogna, M, Forti, D, Pinzello, G, Idèo, G, Belli, Luca Saverio, Zavaglia, Claudio, Alberti, Alberto Battista, Poli, Francesca, Rondinara, Gianfranco, Silini, Enrico, Taioli, Emanuela, De Carlis, Luciano, Scalamogna, Mario, Forti, Domenico, Pinzello, Giovambattista, and Idèo, Gaetano

Abstract

In immunocompetent patients, specific human leukocyte antigen (HLA) class II alleles have been associated with the severity of hepatitis C virus (HCV)-related disease, in particular, HLA-DRBI* 1 I has been found to exert a protective effect. The authors have analyzed the role of HLA class I and II alleles in determining the frequency, timing, and progression of histologically proven recurrent hepatitis C in 89 patients who underwent a liver transplant for HCV-related cirrhosis. In addition, the influence of HLA mismatch between donor and recipient, HCV genotype, and use of steroid pulses was also evaluated. Median patient follow up was 35 months (range 4-119). HLA-DRBI typing was performed by genomic analysis in all cases. Liver biopsies were obtained routinely and at least at yearly intervals. Histologically proven recurrent hepatitis was observed in 46 patients (52%), 10 patients progressing to stage 5-6 fibrosis in most cases within 2 years after transplant. By univariate analysis, 3 variables, HLA-B14, HLA-DRB1*04, and HLA-DRB1 donor/recipient mismatch, showed a significant effect on time to recurrent hepatitis C disease. These parameters were included in a multivariate regression model along with HCV genotype, treatment with steroid pulses and DRB1*11. HLA-B14, HLA-DRBI*04, and HLA-DRBI donor/recipient mismatch were confirmed to provide a significant and independent contribution to the risk of hepatitic disease recurrence. As for the severity of the disease, none of the 10 patients with stage 5-6 hepatitis carried the HLA- DRBI*11 allele, in line with what was observed in nontransplant subjects. Our results suggest that in posttransplant recurrent hepatitis C, immunogenetic factors are relevant in determining HCV infection outcome

Published
2000

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