Your search keyword '"Morelli M.C."' showing total 6 results

1. Nationwide survey of liver transplantation for Primary Sclerosing Cholangitis in Italy

Author

Morelli, M.C., primary, Gambato, M., additional, Martini, S., additional, Carrai, P., additional, Toniutto, P., additional, Giannelli, V., additional, Donato, F., additional, Lenci, I., additional, Pasulo, L., additional, Mazzarelli, C., additional, Ferrarese, A., additional, Rendina, M., additional, Grieco, A., additional, Lanza, A. Galeota, additional, Svegliati-Baroni, G., additional, De Maria, N., additional, Marenco, S., additional, Mameli, L., additional, and Burra, P., additional

Published

2023

2. SARS-CoV-2 infection in liver transplantation is associated with favorable outcomes: an Italian transplant registry study

Author

Rendina, M., primary, Barone, M., additional, Trapani, S., additional, Masiero, L., additional, Trerotoli, P., additional, Puoti, F., additional, Lupo, L.G., additional, Agnes, S., additional, Grieco, A., additional, Andorno, E., additional, Marenco, S., additional, Baccarani, U., additional, Toniutto, P., additional, Carraro, A., additional, Colecchia, A., additional, Cescon, M., additional, Morelli, M.C., additional, Cillo, U., additional, Burra, P., additional, Angeli, P., additional, Colledan, M., additional, Fagiuoli, S., additional, De Carlis, L., additional, Belli, L., additional, De Simone, P., additional, Carrai, P., additional, Di Benedetto, F., additional, De Maria, N., additional, Ettorre, G.M., additional, Giannelli, V., additional, Gruttadauria, S., additional, Volpes, R., additional, Mazzaferro, V., additional, Bhoori, S., additional, Romagnoli, R., additional, Martini, S., additional, Rossi, G., additional, Donato, F., additional, Rossi, M., additional, Ginanni Corradini, S., additional, Spada, M., additional, Maggiore, G., additional, Tisone, G., additional, Lenci, I., additional, Vennarecci, G., additional, Di Costanzo, G.G., additional, Vivarelli, M., additional, Svegliati Baroni, G., additional, Zamboni, F. o, additional, Mameli, L., additional, Tafuri, S., additional, Simone, S., additional, Gesualdo, L., additional, Cardillo, M., additional, and Di Leo, A., additional

Published

2022

3. Prediction models for carbapenem‐resistant Enterobacterales carriage at liver transplantation: A multicenter retrospective study

Author

Maristela Pinheiro Freire, Matteo Rinaldi, Debora Raquel Benedita Terrabuio, Mariane Furtado, Zeno Pasquini, Michele Bartoletti, Tiago Almeida de Oliveira, Nathalia Neves Nunes, Gabriela Takeshigue Lemos, Angelo Maccaro, Antonio Siniscalchi, Cristiana Laici, Matteo Cescon, Luiz Augusto Carneiro D´albuquerque, Maria Cristina Morelli, Alice T. W. Song, Edson Abdala, Pierluigi Viale, Alexandre Dias Porto Chiavegatto Filho, Maddalena Giannella, Freire M.P., Rinaldi M., Terrabuio D.R.B., Furtado M., Pasquini Z., Bartoletti M., de Oliveira T.A., Nunes N.N., Lemos G.T., Maccaro A., Siniscalchi A., Laici C., Cescon M., D'albuquerque L.A.C., Morelli M.C., Song A.T.W., Abdala E., Viale P., Filho A.D.P.C., and Giannella M.

Subjects

prediction model, Transplantation, machine learning, Infectious Diseases, peritonitis prophylaxi, CLIF-SOFA score, carbapenem-resistance

Abstract

Background: Carbapenem-resistant Enterobacterales (CRE) colonisation at liver transplantation (LT) increases the risk of CRE infection after LT, which impacts on recipients’ survival. Colonization status usually becomes evident only near LT. Thus, predictive models can be useful to guide antibiotic prophylaxis in endemic centres. Aims: This study aimed to identify risk factors for CRE colonisation at LT in order to build a predictive model. Methods: Retrospective multicentre study including consecutive adult patients who underwent LT, from 2010 to 2019, at two large teaching hospitals. We excluded patients who had CRE infections within 90 days before LT. CRE screening was performed in all patients on the day of LT. Exposure variables were considered within 90 days before LT and included cirrhosis complications, underlying disease, time on the waiting list, MELD and CLIF-SOFA scores, antibiotic use, intensive care unit and hospital stay, and infections. A machine learning model was trained to detect the probability of a patient being colonized with CRE at LT. Results: A total of 1544 patients were analyzed, 116 (7.5%) patients were colonized by CRE at LT. The median time from CRE isolation to LT was 5 days. Use of antibiotics, hepato-renal syndrome, worst CLIF sofa score, and use of beta-lactam/beta-lactamase inhibitor increased the probability of a patient having pre-LT CRE. The proposed algorithm had a sensitivity of 66% and a specificity of 83% with a negative predictive value of 97%. Conclusions: We created a model able to predict CRE colonization at LT based on easy-to-obtain features that could guide antibiotic prophylaxis (Figure presented.).

Published

2022

4. Genetics in Familial Intrahepatic Cholestasis: Clinical Patterns and Development of Liver and Biliary Cancers: A Review of the Literature

Author

Giovanni Vitale, Alessandro Mattiaccio, Amalia Conti, Laura Turco, Marco Seri, Fabio Piscaglia, Maria Cristina Morelli, Vitale G., Mattiaccio A., Conti A., Turco L., Seri M., Piscaglia F., and Morelli M.C.

Subjects

gallbladder cancer, Cancer Research, Oncology, liver transplantation, microbiota, bile acid, next-generation sequencing, progressive familial intrahepatic cholestasis, hepatocellular carcinoma, Alagille syndrome, cholangiocarcinoma, hepatobiliary cancer

Abstract

The family of inherited intrahepatic cholestasis includes autosomal recessive cholestatic rare diseases of childhood involved in bile acids secretion or bile transport defects. Specific genetic pathways potentially cause many otherwise unexplained cholestasis or hepatobiliary tumours in a healthy liver. Lately, next-generation sequencing and whole-exome sequencing have improved the diagnostic procedures of familial intrahepatic cholestasis (FIC), as well as the discovery of several genes responsible for FIC. Moreover, mutations in these genes, even in the heterozygous status, may be responsible for cryptogenic cholestasis in both young and adults. Mutations in FIC genes can influence serum and hepatic levels of bile acids. Experimental studies on the NR1H4 gene have shown that high bile acids concentrations cause excessive production of inflammatory cytokines, resistance to apoptosis, and increased cell regeneration, all risk conditions for developing hepatocellular carcinoma (HCC) and cholangiocarcinoma (CCA). NR1H4 gene encodes farnesoid X-activated receptor having a pivotal role in bile salts synthesis. Moreover, HCC and CCA can emerge in patients with several FIC genes such as ABCB11, ABCB4 and TJP2. Herein, we reviewed the available data on FIC-related hepatobiliary cancers, reporting on genetics to the pathophysiology, the risk factors and the clinical presentation.

Published

2022

5. The power of kindness: curative treatment with metronomic combination in advanced hepatocellular carcinoma

Author

Rita Golfieri, Alessandro Rizzo, Giorgio Frega, Francesco Vasuri, Stefano Brocchi, Andrea Palloni, Stefania De Lorenzo, Maria Cristina Morelli, Alessandro Federico, Giovanni Brandi, Brandi G., Di Federico A., Rizzo A., De Lorenzo S., Vasuri F., Brocchi S., Golfieri R., Morelli M.C., Frega G., and Palloni A.

Subjects

Oncology, Adult, Male, Liver Cancer, Cancer Research, medicine.medical_specialty, Antimetabolites, Antineoplastic, Carcinoma, Hepatocellular, Cyclophosphamide, medicine.medical_treatment, Liver transplantation, Capecitabine, Internal medicine, medicine, Humans, Pharmacology (medical), Pharmacology, Performance status, business.industry, Liver Neoplasms, Patient Acuity, Hepatocellular Carcinoma, medicine.disease, Hepatitis B, Metronomic Chemotherapy, Hepatitis D, digestive system diseases, Hepatocellular carcinoma, Administration, Metronomic, Liver function, alpha-Fetoproteins, business, Progressive disease, medicine.drug

Abstract

The administration of approved systemic treatments for advanced hepatocellular carcinoma (HCC) is limited to patients with preserved liver function (Child-Pugh A/B7) and performance status. Conversely, metronomic chemotherapy can be safely administered to patients with poor clinical conditions and severe liver impairment. The metronomic schedule demonstrated to exert different anticancer mechanisms compared to that of the same agent administered at its standard schedule, including immune stimulation and the inhibition of angiogenesis and vasculogenesis. Nevertheless, metronomic chemotherapy is a nearly neglected option for the treatment of advanced HCC patients, even among those who cannot afford standard treatments. Herein, we report the case of a 40-year-old patient affected by HBV-HDV-related cirrhosis who was diagnosed with advanced HCC. The severe liver impairment (Child-Pugh B9) did not allow to administer first-line treatment with tyrosine kinase inhibitors so that the patient received metronomic capecitabine as upfront therapy. Due to the suspect of progressive disease at the first radiologic assessment, metronomic cyclophosphamide was added to capecitabine aiming to enhance its efficacy. After 4 months of treatment, complete tumor response, alpha-fetoprotein (AFP) normalization and the recovery of a Child-Pugh A were achieved. The patient was then able to undergo liver transplantation, and, after 18 months from the diagnosis, he is still free of disease recurrence. This experience emphasizes the reliability of metronomic capecitabine as a well-tolerated and effective treatment when patient's conditions prevent the administration of standard first-line treatments. In fact, metronomic capecitabine demonstrated its effectiveness in advanced HCC in retrospective and prospective analyses, leading to median progression-free survival and overall survival of, respectively, 6.03 and 14.47 months in phase II single-arm trial. Moreover, in consideration of the raising interest in immune-checkpoint inhibition in HCC, we believe that the immunomodulating effects of metronomic chemotherapy, either capecitabine or cyclophosphamide, warrant future trials exploring its combination with immunotherapy.

Published

2022

6. Improved Survival after Transarterial Radioembolisation for Hepatocellular Carcinoma Gives the Procedure Added Value

Author

Cristina Mosconi, Alberta Cappelli, Cinzia Pettinato, Maria Adriana Cocozza, Giulio Vara, Eleonora Terzi, Maria Cristina Morelli, Elisa Lodi Rizzini, Matteo Renzulli, Francesco Modestino, Matteo Serenari, Rachele Bonfiglioli, Letizia Calderoni, Elena Tabacchi, Matteo Cescon, Alessio Giuseppe Morganti, Franco Trevisani, Fabio Piscaglia, Stefano Fanti, Lidia Strigari, Alessandro Cucchetti, Rita Golfieri, Mosconi C., Cappelli A., Pettinato C., Cocozza M.A., Vara G., Terzi E., Morelli M.C., Lodi Rizzini E., Renzulli M., Modestino F., Serenari M., Bonfiglioli R., Calderoni L., Tabacchi E., Cescon M., Morganti A.G., Trevisani F., Piscaglia F., Fanti S., Strigari L., Cucchetti A., and Golfieri R.

Subjects

radioembolization, hepatocellular carcinoma, HCC, General Medicine

Abstract

Background: Transarterial Radioembolisation (TARE) requires multidisciplinary experience and skill to be effective. The aim of this study was to identify determinants of survival in patients with hepatocellular carcinoma (HCC), focusing on learning curves, technical advancements, patient selection and subsequent therapies. Methods: From 2005 to 2020, 253 patients were treated. TARE results achieved in an initial period (2005–2011) were compared to those obtained in a more recent period (2012–2020). To isolate the effect of the treatment period, differences between the two periods were balanced using “entropy balance”. Results: Of the 253 patients, 68 were treated before 2012 and 185 after 2012. In the second period, patients had an Eastern Cooperative Oncology Group (ECOG) Performance Status (PS) score of 1 (p = 0.025) less frequently, less liver involvement (p = 0.006) and a lesser degree of vascular invasion (p = 0.019). The median overall survival (OS) of patients treated before 2012 was 11.2 months and that of patients treated beginning in 2012 was 25.7 months. After reweighting to isolate the effect of the treatment period, the median OS of patients before 2012 increased to 16 months. Conclusions: Better patient selection, refinement of technique and adoption of personalised dosimetry improved survival after TARE. Conversely, sorafenib after TARE did not impact life expectancy.

Published

2022