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1. The Kidney Donor Profile Index (KDPI) of Marginal Donors Allocated by Standardized Pretransplant Donor Biopsy Assessment: Distribution and Association With Graft Outcomes

Author

Gandolfini, I., Buzio, C., Zanelli, P., Palmisano, A., Cremaschi, E., Vaglio, A., Piotti, G., Melfa, L., La Manna, G., Feliciangeli, G., Cappuccilli, M., Scolari, M.P., Capelli, I., Panicali, L., Baraldi, O., Stefoni, S., Buscaroli, A., Ridolfi, L., D’Errico, A., Cappelli, G., Bonucchi, D., Rubbiani, E., Albertazzi, A., Mehrotra, A., Cravedi, P., and Maggiore, U.

Published
2014
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11. Survival after the diagnosis of de novo malignancy in liver transplant recipients

Author

Taborelli, M, Piselli, P, Ettorre, Gm, Baccarani, U, Burra, P, Lauro, A, Galatioto, L, Rendina, M, Shalaby, S, Petrara, R, Nudo, F, Toti, L, Fantola, G, Cimaglia, C, Agresta, A, Vennarecci, G, Pinna, Ad, Gruttadauria, S, Risaliti, A, Di Leo, A, Rossi, M, Tisone, G, Zamboni, F, Serraino, D, Zanus, G, Zanini, S, Rigotti, P, Schena, Fp, Grandaliano, G, Fiorentino, M, Di Gioia, P, Pellegrini, S, Zanfi, C, Scolari, Mp, Stefoni, S, Todeschini, P, Panicali, L, Valentini, C, Adani, Gl, Lorenzin, D, Colasanti, M, Coco, M, Ettorre, F, Santoro, R, Miglioresi, L, Mennini, G, Casella, A, Fazzolari, L, Sforza, D, Iaria, G, Gazia, C, Belardi, C, D'Offizi, G, Comandini, Uv, Lionetti, R, Montalbano, M, Taibi, C, Piredda, Gb, Michittu, Mb, Murgia, Mg, Onano, B, Fratino, L, Maso, Ld, De Paoli, P, Verdirosi, D, Vaccher, E, Pisani, F, Famulari, A, Delreno, F, Iesari, S, De Luca, L, Iaria, M, Capocasale, E, Cremaschi, E, Sandrini, S, Valerio, F, Mazzucotelli, V, Bossini, N, Setti, G, Veroux, M, Veroux, P, Giuffrida, G, Giaquinta, A, Zerbo, D, Busnach, G, Di Leo, L, Perrino, Ml, Querques, M, Colombo, V, Sghirlanzoni, Mc, Messa, P, Leoni, A, Sparacino, V, Caputo, F, Buscemi, B, Citterio, F, Spagnoletti, G, Salerno, Mp, Favi, E, Segoloni, Gp, Biancone, L, Lavacca, A, Maresca, Mc, Cascone, C, Virgilio, B, Donati, D, Dossi, F, Fontanella, A, Ambrosini, A, and Di Cicco, M.

Published
2019

12. Increased cancer risk in patients undergoing dialysis: A population-based cohort study in North-Eastern Italy

Author

Taborelli, M., Toffolutti, F., Del Zotto, S., Clagnan, E., Furian, L., Piselli, P., Citterio, Franco, Zanier, L., Boscutti, G., Serraino, D., Shalaby, S., Petrara, R., Burra, P., Zanus, G., Zanini, S., Rigotti, P., Rendina, M., Di Leo, A., Schena, F. P., Grandaliano, Giuseppe, Fiorentino, M., Lauro, A., Pinna, A. D., Di Gioia, P., Pellegrini, S., Zanfi, C., Scolari, M. P., Stefoni, S., Todeschini, P., Panicali, L., Valentini, C., Baccarani, U., Risaliti, A., Adani, G. L., Lorenzin, D., Ettorre, G. M., Vennarecci, G., Colasanti, M., Coco, M., Ettorre, F., Santoro, R., Miglioresi, L., Nudo, F., Rossi, M., Mennini, G., Toti, L., Tisone, G., Casella, A., Fazzolari, L., Sforza, D., Iaria, G., Gazia, C., Belardi, C., Cimaglia, C., Agresta, A., D'Offizi, G., Comandini, U. V., Lionetti, R., Montalbano, M., Taibi, C., Fantola, G., Zamboni, F., Piredda, G. B., Michittu, M. B., Murgia, M. G., Onano, B., Fratino, L., Maso, L. D., De Paoli, P., Verdirosi, D., Vaccher, E., Pisani, F., Famulari, A., Delreno, F., Iesari, S., De Luca, L., Iaria, M., Capocasale, E., Cremaschi, E., Sandrini, S., Valerio, F., Mazzucotelli, V., Bossini, N., Setti, G., Veroux, M., Veroux, P., Giaquinta, A., Zerbo, D., Busnach, G., Di Leo, L., Perrino, M. L., Querques, M., Colombo, V., Sghirlanzoni, M. C., Messa, P., Leoni, A., Galatioto, L., Gruttadauria, S., Sparacino, V., Caputo, F., Buscemi, B., Spagnoletti, Gionata, Salerno, Maria Paola, Favi, E., Segoloni, G. P., Biancone, L., Lavacca, A., Maresca, M. C., Cascone, C., Virgilio, B., Donati, D., Dossi, F., Fontanella, A., Ambrosini, A., Di Cicco, M., Citterio F. (ORCID:0000-0003-0489-6337), Grandaliano G. (ORCID:0000-0003-1213-2177), Spagnoletti G. (ORCID:0000-0003-2626-8147), Salerno M. P., Taborelli, M., Toffolutti, F., Del Zotto, S., Clagnan, E., Furian, L., Piselli, P., Citterio, Franco, Zanier, L., Boscutti, G., Serraino, D., Shalaby, S., Petrara, R., Burra, P., Zanus, G., Zanini, S., Rigotti, P., Rendina, M., Di Leo, A., Schena, F. P., Grandaliano, Giuseppe, Fiorentino, M., Lauro, A., Pinna, A. D., Di Gioia, P., Pellegrini, S., Zanfi, C., Scolari, M. P., Stefoni, S., Todeschini, P., Panicali, L., Valentini, C., Baccarani, U., Risaliti, A., Adani, G. L., Lorenzin, D., Ettorre, G. M., Vennarecci, G., Colasanti, M., Coco, M., Ettorre, F., Santoro, R., Miglioresi, L., Nudo, F., Rossi, M., Mennini, G., Toti, L., Tisone, G., Casella, A., Fazzolari, L., Sforza, D., Iaria, G., Gazia, C., Belardi, C., Cimaglia, C., Agresta, A., D'Offizi, G., Comandini, U. V., Lionetti, R., Montalbano, M., Taibi, C., Fantola, G., Zamboni, F., Piredda, G. B., Michittu, M. B., Murgia, M. G., Onano, B., Fratino, L., Maso, L. D., De Paoli, P., Verdirosi, D., Vaccher, E., Pisani, F., Famulari, A., Delreno, F., Iesari, S., De Luca, L., Iaria, M., Capocasale, E., Cremaschi, E., Sandrini, S., Valerio, F., Mazzucotelli, V., Bossini, N., Setti, G., Veroux, M., Veroux, P., Giaquinta, A., Zerbo, D., Busnach, G., Di Leo, L., Perrino, M. L., Querques, M., Colombo, V., Sghirlanzoni, M. C., Messa, P., Leoni, A., Galatioto, L., Gruttadauria, S., Sparacino, V., Caputo, F., Buscemi, B., Spagnoletti, Gionata, Salerno, Maria Paola, Favi, E., Segoloni, G. P., Biancone, L., Lavacca, A., Maresca, M. C., Cascone, C., Virgilio, B., Donati, D., Dossi, F., Fontanella, A., Ambrosini, A., Di Cicco, M., Citterio F. (ORCID:0000-0003-0489-6337), Grandaliano G. (ORCID:0000-0003-1213-2177), Spagnoletti G. (ORCID:0000-0003-2626-8147), and Salerno M. P.

Abstract

Background: In southern Europe, the risk of cancer in patients with end-stage kidney disease receiving dialysis has not been well quantified. The aim of this study was to assess the overall pattern of risk for de novo malignancies (DNMs) among dialysis patients in the Friuli Venezia Giulia region, north-eastern Italy. Methods: A population-based cohort study among 3407 dialysis patients was conducted through a record linkage between local healthcare databases and the cancer registry (1998-2013). Person-years (PYs) were calculated from 30 days after the date of first dialysis to the date of DNM diagnosis, kidney transplant, death, last follow-up or December 31, 2013, whichever came first. The risk of DNM, as compared to the general population, was estimated using standardized incidence ratios (SIRs) and 95% confidence intervals (CIs). Results: During 10,798 PYs, 357 DNMs were diagnosed in 330 dialysis patients. A higher than expected risk of 1.3-fold was found for all DNMs combined (95% CI: 1.15-1.43). The risk was particularly high in younger dialysis patients (SIR = 1.88, 95% CI: 1.42-2.45 for age 40-59 years), and it decreased with age. Moreover, significantly increased DNM risks emerged during the first 3 years since dialysis initiation, especially within the first year (SIR = 8.52, 95% CI: 6.89-10.41). Elevated excess risks were observed for kidney (SIR = 3.18; 95% CI: 2.06-4.69), skin non-melanoma (SIR = 1.81, 95% CI: 1.46-2.22), oral cavity (SIR = 2.42, 95% CI: 1.36-4.00), and Kaposi's sarcoma (SIR = 10.29, 95% CI: 1.25-37.16). Conclusions: The elevated risk for DNM herein documented suggest the need to implement a targeted approach to cancer prevention and control in dialysis patients.

Published
2019

13. Extracorporeal detoxification for hepatic failure using molecular adsorbent recirculating system: depurative efficiency and clinical results in a long-term follow-up

Author

Donati, G, La Manna, G, Cianciolo, G, Grandinetti, V, Carretta, E, Cappuccilli, M, Panicali, L, Iorio, M, Piscaglia, F, Bolondi, L, Colì, L, Stefoni, S, Donati, G, La Manna, G, Cianciolo, G, Grandinetti, V, Carretta, E, Cappuccilli, M, Panicali, L, Iorio, M, Piscaglia, F, Bolondi, L, Colì L, and Stefoni, S

Subjects
Adult, Aged, 80 and over, Male, Extracorporeal Circulation, LIVER FAILURE, Waiting Lists, MARS, Middle Aged, Liver Transplantation, Young Adult, Treatment Outcome, EXTRACORPOREAL DETOXIFICATION, Humans, Female, Sorption Detoxification, EXTRACORPOREAL SUPPORT, Prospective Studies, Liver Failure, Aged
Abstract

Acute liver failure and acute-on-chronic liver failure still show a poor prognosis. The molecular adsorbent recirculating system (MARS) has been extensively used as the most promising detoxifying therapy for patients with these conditions. Sixty-four patients with life-threatening liver failure were selected, and 269 MARS treatments were carried out as a bridge for orthotopic liver transplantation (OLT) or for liver function recovery. All patients were grouped according to the aim of MARS therapy. Group A consisted of 47 patients treated for liver function recovery (median age 59 years, range 23-82). Group B consisted of 11 patients on the waiting list who underwent OLT (median age 47 years, range 32-62). Group C consisted of 6 patients on the waiting list who did not undergo OLT (median age 45.5 years, range 36-54, P = 0.001). MARS depurative efficiency in terms of liver toxins, cytokines, and growth factors was assessed together with the clinical outcome of the patients during a 1-year follow-up. Total bilirubin reduction rate per session (RRs) for each MARS session was 23% (range 17-29); direct bilirubin RRs was 28% (21-35), and indirect bilirubin RRs was 8% (3-21). Ammonia RRs was 34% (12-86). Conjugated cholic acid RRs was 58% (48-61); chenodeoxycholic acid RRs was 34% (18-48). No differences were found between groups. Hepatocyte growth factor (HGF) values on starting MARS were 4.1 ng/mL (1.9-7.9) versus 7.9 ng/mL (3.2-14.1) at MARS end (P

Published
2013

14. Survival of ptfe grafts vs. Tunneled cuffed catheters (tccs) for hemodialysis

Author

Donati, G, Scrivo, A, Cianciolo, G, La Manna, G, Panicali, L, Rucci, P, Marchetti, A, Giampalma, E, Galaverni, Mc, Golfieri, R, Stefoni, S, and Donati G, Scrivo A, Cianciolo G, La Manna G, Panicali L, Rucci P, Marchetti A, Giampalma E, Galaverni MC, Golfieri R, Stefoni S

Subjects
TCCs, Hemodialysis, Prosthetic grafts, Vascular acce, hemodialysis patient, survival, PTFE graft
Published
2013

15. PTFE Grafts Versus Tunneled Cuffed Catheters for Hemodialysis: Which Is the Second Choice When Arteriovenous Fistula Is Not Feasible?

Author

Donati, G, Cianciolo, G, Mauro, R, Rucci, P, Scrivo, A, Marchetti, A, Giampalma, E, Golfieri, R, Panicali, L, Iorio, M, Stella, A, La Manna, G, Stefoni, S, Donati, Gabriele, Cianciolo, Giuseppe, Mauro, Raffaella, Rucci, Paola, Scrivo, Anna, Marchetti, Antonio, Giampalma, Emanuela, Golfieri, Rita, Panicali, Laura, Iorio, Mario, Stella, Andrea, La Manna, Gaetano, and Stefoni, Sergio

Subjects
Aged, 80 and over, Male, Survival, Medicine (all), Biomedical Engineering, Medicine (miscellaneous), Bioengineering, Kaplan-Meier Estimate, Middle Aged, Tunneled cuffed permanent catheter, Biomaterial, Complications, Grafts, Hemodialysis, Tunneled cuffed permanent catheters, Graft, Arteriovenous Shunt, Surgical, Catheters, Indwelling, Renal Dialysis, Renal Dialysi, Humans, Kidney Failure, Chronic, Female, Hemodialysi, Complication, Polytetrafluoroethylene, Aged, Human
Abstract

Vascular access-related complications are still one of the leading causes of morbidity in hemodialysis patients. The aim of this study was to compare polytetrafluoroethylene (PTFE) grafts versus tunneled cuffed permanent catheters (TCCs) in terms of vascular access and patients' survival. An observational study was carried out with a 2-year follow-up. Eighty-seven chronic hemodialysis patients were enrolled: 31 with a PTFE graft as vascular access for hemodialysis versus 56 with a TCC. Patients' mean age was 63.8 ± 14.6 (grafts) versus 73.5 ± 11.3 years (TCCs), P = 0.001. Significantly more patients with TCC had atrial fibrillation than patients with grafts (30.3% versus 6.5%, P = 0.01). In an unadjusted Kaplan-Meier analysis, median TCC survival at 24 months was 5.4 months longer than that of PTFE grafts but not significantly (log-rank test = 1.3, P = ns). In a Cox regression analysis adjusted for age, gender, number of previous vascular accesses, diabetes, atrial fibrillation, smoking, and any complication, this lack of significant difference in survival of the vascular access between TCC and PTFE groups was confirmed and diabetes proved to be an independent risk factor for the survival of both vascular accesses considered (P = 0.02). In an unadjusted Kaplan-Meier analysis, a higher mortality was found in the TCC group than in the PTFE group at 24 months (log-rank test = 10.07, P

Published
2015

16. Un nuovo modello matematico per la HFR profilata

Author

Coli', L, Donati, G, Cianciolo, G, Ursino, M, Ruggieri, G, Baraldi, O, DI NICOLO', P, Panicali, L, Stefoni, S., Colì L, Donati G, Cianciolo G, Ursino M, Ruggieri G, Baraldi O, Di Nicolò P, Panicali L, and Stefoni S.

Subjects
DIALISI PROFILATA, modello matematico, ipotensione intradialitica, HFR
Published
2006

20. Vascular access

Author

McCullough, K. P., primary, Lok, C. E., additional, Fluck, R. J., additional, Spergel, L. M., additional, Andreucci, V. E., additional, Fort, J., additional, Krishnan, M., additional, Fissell, R. B., additional, Kawanishi, H., additional, Saran, R., additional, Port, F. K., additional, Robinson, B. M., additional, Pisoni, R. L., additional, Shinzato, T., additional, Shionoya, Y., additional, Fukui, H., additional, Sasaki, M., additional, Miwa, M., additional, Toma, S., additional, Lin, C.-C., additional, Yang, W.-C., additional, Simone, S., additional, Loverre, A., additional, Cariello, M., additional, Divella, C., additional, Castellano, G., additional, Gesualdo, L., additional, Grandaliano, G., additional, Pertosa, G., additional, Mattei, S., additional, Pignatelli, G., additional, Corradini, M., additional, Stefani, A., additional, Bovino, A., additional, Iannuzzella, F., additional, Vaglio, A., additional, Manari, A., additional, Pasquali, S., additional, Chan, J.-S., additional, Wu, T.-C., additional, Roy-Chaudhury, P., additional, Shih, C.-C., additional, Chen, J.-W., additional, Ponce, P., additional, Scholz, C., additional, Goncalves, P., additional, Grassmann, A., additional, Canaud, B., additional, Marcelli, D., additional, Suzuki, S., additional, Shibata, K., additional, Kuji, T., additional, Kawata, S., additional, Koguchi, N., additional, Nishihara, M., additional, Satta, H., additional, Toya, Y., additional, Umemura, S., additional, Corbett, R., additional, Demicheli, N., additional, Iori, F., additional, Grechy, L., additional, Khiroya, R., additional, Ellis, D., additional, Crane, J., additional, Hamady, M., additional, Gedroyc, W., additional, Duncan, N., additional, Vincent, P., additional, Caro, C., additional, Sarween, N., additional, Price, A., additional, Powers, S., additional, Allen, C., additional, Holland, M., additional, Gupta, I., additional, Baharani, J., additional, Parisotto, M. T., additional, Schoder, V., additional, Kaufmann, P., additional, Miriunis, C., additional, Moura, A., additional, Madureira, J., additional, Alija, P., additional, Fernandes, J., additional, Oliveira, J. G., additional, Lopez, M., additional, Felgueiras, M., additional, Amado, L., additional, Sameiro-Faria, M., additional, Miranda, V., additional, Vieira, M., additional, Santos-Silva, A., additional, Costa, E., additional, David, P., additional, Capurro, F., additional, Brustia, M., additional, De Mauri, A., additional, Ruva, C., additional, Chiarinotti, D., additional, Gravellone, L., additional, De Leo, M., additional, Turkvatan, A., additional, Kirkpantur, A., additional, Mandiroglu, S., additional, Afsar, B., additional, Seloglu, B., additional, Alkis, M., additional, Erkula, S., additional, GURBUZ, H. G., additional, Serin, M., additional, CALIK, Y., additional, Mandiroglu, F., additional, Balci, M., additional, Rikker, C., additional, Juhasz, E., additional, Tornoci, L., additional, Tovarosi, S., additional, Greguschik, J., additional, Rosivall, L., additional, Ibeas, J., additional, Valeriano, J., additional, Vallespin, J., additional, Fortuno, J., additional, Rodriguez-Jornet, A., additional, Cabre, C., additional, Merino, J., additional, Vinuesa, X., additional, Bolos, M., additional, Branera, J., additional, Mateos, A., additional, Jimeno, V., additional, Grau, C., additional, Criado, E., additional, Moya, C., additional, Ramirez, J., additional, Gimenez, A., additional, Garcia, M., additional, Kirmizis, D., additional, Kougioumtzidou, O., additional, Vakianis, P., additional, Bandera, A., additional, Veniero, P., additional, Brunori, G., additional, Dimitrijevic, Z., additional, Cvetkovic, T., additional, Paunovic, K., additional, Stojanovic, M., additional, Ljubenovic, S., additional, Mitic, B., additional, Djordjevic, V., additional, Aicha Henriette, S., additional, Farideh, A., additional, Daniela, B., additional, Zafer, T., additional, Francois, C., additional, Donati, G., additional, Scrivo, A., additional, Cianciolo, G., additional, La Manna, G., additional, Panicali, L., additional, Rucci, P., additional, Marchetti, A., additional, Giampalma, E., additional, Galaverni, M., additional, Golfieri, R., additional, Stefoni, S., additional, Skornyakov, I., additional, Kiselev, N., additional, Rozhdestvenskaya, A., additional, Stolyar, A., additional, Ancarani, P. P. A., additional, Devoto, E., additional, Dardano, G. G. D., additional, Coskun yavuz, Y., additional, Selcuk, N. Y., additional, Guney, I., additional, Altintepe, L., additional, Gerasimovska, V., additional, Gerasimovska-Kitanovska, B., additional, Persic, V., additional, Buturovic-Ponikvar, J., additional, Arnol, M., additional, Ponikvar, R., additional, Conti, N., additional, Scrivano, J., additional, Pettorini, L., additional, Giuliani, A., additional, Punzo, G., additional, Mene, P., additional, Pirozzi, N., additional, Kocyigit, I., additional, Unal, A., additional, Guney, A., additional, Mavili, E., additional, Deniz, K., additional, Sipahioglu, M., additional, Eroglu, E., additional, Tokgoz, B., additional, Oymak, O., additional, Gunal, A., additional, Boubaker, K., additional, Kaaroud, H., additional, Kheder, A., additional, Vidal, M., additional, Amengual, M. J., additional, Orellana, R., additional, Sanfeliu, I., additional, Marquina, D., additional, Xirinachs, M., additional, Sanchez, E., additional, Rey, M., additional, Strozecki, P., additional, Flisinski, M., additional, Kapala, A., additional, Manitius, J., additional, Gerasimovska-Kitanovska, B. D., additional, Sikole, A., additional, Weber, E., additional, Adrych, D., additional, Wolyniec, W., additional, Liberek, T., additional, Rutkowski, B., additional, Oguchi, K., additional, Nakahara, T., additional, Okamoto, M., additional, Iwabuchi, H., additional, Asano, M., additional, Rap, O., additional, Ruiz-Valverde, M., additional, Rodriguez-Murillo, J. A., additional, Mallafre-Anduig, J. M., additional, Zeid, M. M., additional, Deghady, A. A., additional, Elshair, H. S., additional, Elkholy, N. A., additional, Panagoutsos, S., additional, Devetzis, V., additional, Roumeliotis, A., additional, Kantartzi, K., additional, Mourvati, E., additional, Vargemezis, V., additional, Passadakis, P., additional, Kang, S. H., additional, Jung, S. Y., additional, Lee, S. H., additional, Cho, K. H., additional, Park, J. W., additional, Yoon, K. W., additional, and Do, J. Y., additional

Published
2013
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24. De Novo Malignancies after Organ Transplantation: Focus on Viral Infections

Author

Piselli, P1, Busnach, G, Fratino, L, Citterio, F, Ettorre, Gm, De Paoli, P, Serraino, D, Dal Maso, L, Di Maso, M, Zucchetto, A, Agresta, A, Cimaglia, C, Puro, V, Ippolito, G, Miglioresi, L, Vennarecci, G, Santoro, R, Famulari, A, Delreno, F, Grandaliano, G, Fiorentino, M, Stefoni, S, Todeschini, P, Panicali, L, Valentini, C, Valerio, F, Bossini, N, Setti, G, Michittu, Mb, Murgia, Mg, Onano, B, Veroux, Pierfrancesco, Giuffrida, G, Giaquinta, A, Zerbo, D, Di Leo, L, Perrino, Ml, Colombo, V, Sghirlanzoni, Mc, Leoni, A, Buscemi, B, Lazzarin, M, Zanini, S, Spagnoletti, G, Salerno, Mp, Favi, E, De Luca, L, Lavacca, A, Cascone, C, Virgilio, B, Dossi, F, Fontanella, A, Ambrosini, A, Di Cicco, M., Piselli P, Busnach G, Fratino L, Citterio F, Ettorre GM, De Paoli P, Serraino D, Todeschini P, and Immunosuppression and Cancer Study Group

Subjects
SOLID ORGAN TRANSPLANT, Herpesvirus 4, Human, medicine.medical_specialty, Skin Neoplasms, Settore MED/18 - CHIRURGIA GENERALE, medicine.medical_treatment, Lymphoproliferative disorders, cancer risk, medicine.disease_cause, Biochemistry, Organ transplantation, Virus, medicine, Humans, Sarcoma, Kaposi, Molecular Biology, solid organ transplantation, Immunosuppression Therapy, business.industry, ORGAN, Cancer, Kaposi sarcoma, Immunosuppression, KAPOSI'S SARCOMA, General Medicine, renal transplantation, medicine.disease, iatrogenic immunosuppression, Kidney Transplantation, neoplasia, VIRAL INFECTIONS, Herpesvirus 8, Human, Immunology, Molecular Medicine, POST-TRANSPLANT MALIGNANCY, Sarcoma, viral infection, Carcinogenesis, business, Oncovirus
Abstract

Organ transplantation is an increasingly used medical procedure for treating otherwise fatal end stage organ diseases with 107,000 transplants performed worldwide in 2010. Newly developed anti-rejection drugs greatly helped to prolong long-term survival of both the individual and the transplanted organ, and they facilitate the diffusion of organ transplantation. Presently, 5-year patient survival rates are around 90% after kidney transplant and 70% after liver transplant. However, the prolonged chronic use of immunosuppressive drugs is well known to increase the risks of opportunistic diseases, particularly infections and virus-related malignancies. Although transplant recipients experience a nearly 2-fold elevated risk for all types of de-novo cancers, persistent infections with oncogenic viruses - such as Kaposi sarcoma herpes virus, high-risk human papillomaviruses, and Epstein-Barr virus - are associated with up to 100-fold increased cancer risks. This review, focusing on kidney and liver transplants, highlights updated evidences linking iatrogenic immunosuppression, persistent infections with oncogenic viruses and cancer risk. The implicit capacity of oncogenic viruses to immortalise infected cells by disrupting the cell-cycle control can lead, in a setting of induced lowered immune surveillance, to tumorigenesis and this ability is thought to closely correlate with cumulative exposure to immunosuppressive drugs. Mechanisms underlying the relationship between viral infections, immunosuppressive drugs and the risk of skin cancers, post-transplant lymphoproliferative disorders, Kaposi sarcoma, cervical and other ano-genital cancers are reviewed in details.

25. Native kidney function after renal transplantation combined with other solid organs in preemptive patients

Author

Maria Cappuccilli, Elisa Persici, Sergio Stefoni, Paola Todeschini, G. Mosconi, G. Liviano D’Arcangelo, Laura Panicali, Diletta Conte, Vania Cuna, Irene Capelli, Mosconi G, Panicali L, Persici E, Conte D, Cappuccilli ML, Cuna V, Capelli I, Todeschini P, D'Arcangelo GL, and Stefoni S.

Subjects
Adult, Male, medicine.medical_specialty, Urology, Renal function, Kidney Function Tests, Nephropathy, chemistry.chemical_compound, Native Kidney Function, Renal Transplantation, medicine, Polycystic kidney disease, Humans, Kidney transplantation, Combined Solid Organ Transplantation, Transplantation, Kidney, Creatinine, Polycystic Kidney Diseases, business.industry, Organ Transplantation, Middle Aged, medicine.disease, Kidney Transplantation, Surgery, Liver Transplantation, Preemptive Patients, medicine.anatomical_structure, chemistry, Heart Transplantation, Kidney Failure, Chronic, Female, Kidney Diseases, business, Kidney disease, Glomerular Filtration Rate
Abstract

Kidney transplantations combined with other solid organs are progressively increasing in number. There are no guidelines regarding the nephrologic indications for combined transplantations, namely liver-kidney (LKT), or heart-kidney (HKT), in preemptive patients with chronic kidney failure who are not on regular dialysis therapy. The objective of this study was to assess the functional contribution of the native kidneys after preemptive kidney transplantation combined with other solid organs. From 2004, 9 patients (aged 50.3 +/- 8.5 years) with chronic kidney failure (creatinine 2.5 +/- 1.0 mg/dL) caused by polycystic kidney disease (n = 4), vascular nephropathy (n = 2), interstitial nephropathy (n = 1), glomerulonephritis (n = 1), or end-stage kidney disease (n = 1), underwent combined transplantations (8 LKT, 1 HKT). A scintigraphic functional study (Tc-99DMSA or Tc-99mMAG3), was performed at 4 +/- 3 months after transplantation to evaluate the functional contribution of both the native kidneys and the graft. All patients were given immunosuppressive drugs, including a calcineurin inhibitor (tacrolimus/or cyclosporine). At the time of scintigraphy, renal function in all patients was 1.3 +/- 0.3 mg/dL. The functional contribution of the transplanted kidneys was on average 77 +/- 18%. Only in 1 patient was the contribution of the graft

Published
2010

26. Donor-specific anti-HLA antibodies after bone-graft transplantation. Impact on a subsequent renal transplantation: a case report

Author

Olga Baraldi, Serena Corsini, Andrea Buscaroli, Concetta Fantinati, Giovanni Mosconi, P Zanelli, Sergio Stefoni, A Bassi, Maria Cappuccilli, Giorgio Feliciangeli, Laura Panicali, Maddalena Veronesi, Mosconi G, Baraldi O, Fantinati C, Panicali L, Veronesi M, Cappuccilli ML, Corsini S, Zanelli P, Bassi A, Buscaroli A, Feliciangeli G, and Stefoni S.

Subjects
Adult, Male, Pathology, medicine.medical_specialty, Waiting Lists, HLA TYPING, Human leukocyte antigen, Hyperimmunization, ANTI-HLA ANTIBODIES, Antigen, medicine, Humans, Kidney transplantation, Transplantation, Osteosarcoma, Bone Transplantation, biology, RENAL TRANSPLANT, business.industry, Histocompatibility Testing, Panel reactive antibody, Bone prosthesis, medicine.disease, Flow Cytometry, Kidney Transplantation, HYPERIMMUNIZATION, Immunology, biology.protein, Kidney Failure, Chronic, Surgery, Antibody, Cisplatin, business, BONE-GRAFT TRANSPLANTATION
Abstract

Immunological evaluation by panel-reactive antibody (PRA) and determination of anti-HLA specificity are important phases in the evaluation of patients awaiting kidney transplantation. The main causes of immunization are previous solid organ transplantation, hemotransfusion, and pregnancy. It is also possible that immunogenicity can be triggered by vascularized tissue grafts. Immune induction by cryopreserved bone prostheses is not yet understood. A 19-year-old patient with osteosarcoma had undergone resection of the left proximal tibia with reconstruction using human bone in 1997. The donor HLA typing was as follows: A3, A29 (19); B44 (12), Bw4; DR13 (6), DR7, DR52, DR53. The patient was subsequently enrolled onto the waiting list for cadaveric donor kidney transplantation due to chronic kidney failure caused by cisplatin toxicity. Pretransplantation immunological screening using the complement-dependent cytotoxicity (CDC) technique revealed a PRA of 63%. IgG antibody specificities were detected against class I and class II donor antigens, specifically anti-A3, B44, DR7 antibodies, using flow cytometry (Tepnel Luminex). Further immunological studies using single HLA specificity analysis (LSA Class I degrees -II degrees , Tepnel-Luminex) showed direct antibodies against all donor antigen specificities. This case showed immune induction after the implantation of bone prosthesis in a kidney transplant candidate, underlining the importance of the availability of HLA typing data of donors of a human prosthesis.

Published
2009

27. Epatopatia e trapianto renale: esperienza a medio-lungo termine

Author

MOSCONI, GIOVANNI, LIVIANO D'ARCANGELO, GIOVANNI, BUSCAROLI, ANDREA, CRISTINO, STEFANIA, PANICALI, LAURA, SIRRI, MASSIMO, SCOLARI, MARIA, STEFONI, SERGIO, Mosconi G, Liviano D’Arcangelo G, Buscaroli A, Cristino S, Panicali L, Sirri M, Scolari MP, and Stefoni S

Published
2007

29. Il Trapianto Combinato Rene-Fegato: esperienza monocentrica a lungo termine

Author

MOSCONI, GIOVANNI, CRISTINO, STEFANIA, PANICALI, LAURA, CAROLI, PAOLA, SIRRI, MASSIMO, FELICIANGELI, GIORGIO, FAENZA, ALESSANDRO, PINNA, ANTONIO DANIELE, SCOLARI, MARIA, STEFONI, SERGIO, Mosconi G, Cristino S, Panicali L, Caroli P, Sirri M, Feliciangeli G, Faenza A, Pinna AD, Scolari MP, and Stefoni S.

Published
2007

31. Genetic variability and cardiovascular risk in renal transplant recipients

Author

CAPPUCCILLI, MARIA, LA MANNA, GAETANO, COMAI, GIORGIA, PANICALI, LAURA, CONTE, DILETTA, LANCI, NICOLE, CORSINI, SERENA, CIANCIOLO, GIUSEPPE, SCOLARI, MARIA, STEFONI, SERGIO, Cappuccilli ML, La Manna G, Comai G, Panicali L, Conte D, Lanci N, Corsini S, Cianciolo G, Scolari MP, and Stefoni S

Published
2007

32. Delayed Graft Function (DGF) e Trapianto Renale: studio dei principali fattori di rischio

Author

COMAI, GIORGIA, LA MANNA, GAETANO, SCOLARI, MARIA, D'ADDIO, FRANCESCA, CRISTINO, STEFANIA, NASTASI, VALENTINA, PANICALI, LAURA, MOSCONI, GIOVANNI, STEFONI, SERGIO, Comai G, La Manna G, Scolari MP, D’Addio F, Cristino S, Nastasi V, Panicali L, Mosconi G, and Stefoni S.

Subjects
DELAYED GRAFT FUNCTION, TRAPIANTO RENALE, FATTORI DI RISCHIO
Published
2006

33. A new mathematical model for profiled-HFR

Author

COLI', LUIGI, URSINO, MAURO, MAGOSSO, ELISA, DONATI, GABRIELE, CIANCIOLO, GIUSEPPE, PANICALI, LAURA, RUGGERI, GIOVANNI, NASTASI, VALENTINA, PICCARI, MATTEO, CANNARILE, DANIELA CECILIA, STEFONI, SERGIO, Capriotti P, Di Nicolò P, Bergamini C, Colì L, Ursino M, Magosso E, Capriotti P, Donati G, Cianciolo G, Panicali L, Ruggeri G, Nastasi V, Piccari M, Di Nicolò P, Cannarile D, Bergamini C, and Stefoni S

Subjects
PROFILER, DIALYSIS HYPOTENSION, HFR
Published
2006

34. Anticoagulation therapy for the prevention of hemodialysis tunneled cuffed catheters (TCC) thrombosis

Author

Luigi Coli, Matteo Piccari, Valentina Nastasi, Francesco Gozzetti, Giuseppe Cianciolo, Giorgia Comai, Sergio Stefoni, Gabriele Donati, Daniela Cecilia Cannarile, Laura Panicali, C. Raimondi, Coli L, Donati G, Cianciolo G, Raimondi C, Comai G, Panicali L, Nastasi V, Cannarile DC, Gozzetti F, Piccari M, and Stefoni S.

Subjects
Male, HEMODIALYSIS, Time Factors, medicine.medical_treatment, Treatment outcome, 030232 urology & nephrology, Administration, Oral, Blood Pressure, 030204 cardiovascular system & hematology, Renal Veins, 0302 clinical medicine, Catheters, Indwelling, Renal Artery, TUNNELED CUFFED CATHETERS, PREVENTION, THROMBOSIS, WARFARIN THERAPY, Oral anticoagulation, Aged, 80 and over, Follow up studies, Heparin, Middle Aged, Thrombosis, Combined Modality Therapy, Treatment Outcome, Nephrology, Female, Hemodialysis, medicine.drug, medicine.medical_specialty, Ticlopidine, Warfarin therapy, Renal Circulation, 03 medical and health sciences, Fibrinolytic Agents, Renal Dialysis, medicine, Humans, International Normalized Ratio, Aged, business.industry, Anticoagulants, Heparin, Low-Molecular-Weight, medicine.disease, Survival Analysis, Surgery, Kidney Failure, Chronic, Warfarin, business, Biomarkers, Follow-Up Studies
Abstract

Background Chronic oral anticoagulation is currently used to avoid thrombosis and the malfunction of tunneled cuffed catheters (TCCs) for hemodialysis (HD). The aim of the study was to assess the efficacy of early warfarin administration, after TCC placement, in comparison to its administration after the first thrombosis or malfunction event of the TCC. Patients and methods One hundred and forty-four chronic dialysis patients, who underwent TCC placement between June 2001 and June 2005, were randomized into two groups: 81 patients, group A, started oral anticoagulation 12 hr after the TCC placement (target international normalized ratio (INR) 1.8–2.5), in association with ticlopidine 250 mg/die; 63 patients, group B, started warfarin after the first thrombosis/malfunction episode (target INR 1.8–2.5) in association with ticlopidine 250 mg/die. The efficacy of oral anticoagulation therapy in preventing TCC thrombotic complications was evaluated in a 12-month follow-up period, after TCC placement, in terms of: a) the number of patients with thrombotic-malfunction events; b) the number of thrombotic-malfunction events with urokinase infusion (events/patient/year); c) intradialytic blood flow rate (BFR, ml/min); d) negative blood pressure (BP) from the arterial line of the TCC (AP, mmHg); e) positive BP, in the extracorporeal circuit from the venous line (VP, mmHg); and f) bleeding complications. Results Ten patients (12%) in group A showed TCC thrombosis/malfunction vs. 33 patients (52%) in group B (pConclusions Early warfarin therapy allows a significant reduction in TCC thrombotic complications and an improvement in both arterial and venous fluxes in comparison with the same therapy administered after the first TCC thrombotic/malfunction event. This therapy did not induce any bleeding complications in the patients included in the study.

Published
2006

35. Rigetto ed espressione di geni 'housekeeping' nel Trapianto di Rene

Author

ORTOLANI, MICHELA, LANCI, NICOLE, CAPPUCCILLI, MARIA, LA MANNA, GAETANO, MOSCONI, GIOVANNI, PANICALI, LAURA, CIAVATTI, ALESSANDRO, SCOLARI, MARIA, STEFONI, SERGIO, Ortolani M, Lanci N, Cappuccilli ML, La Manna G, Mosconi G, Panicali L, Ciavatti A, Scolari MP, and Stefoni S.

Subjects
RIGETTO ACUTO, TRAPIANTO RENALE, ESPRESSIONE GENICA, GENI HOUSEKEEPING
Published
2006

36. [Choice and management of anticoagulation during CRRT].

Author

Ricci D, Panicali L, Cavallari G, Facchini MG, and Mancini E

Subjects
Anticoagulants adverse effects, Buffers, Citric Acid adverse effects, Hemorrhage chemically induced, Hemorrhage prevention & control, Heparin administration & dosage, Humans, Water-Electrolyte Balance, Acute Kidney Injury therapy, Anticoagulants administration & dosage, Blood Coagulation, Citric Acid administration & dosage, Renal Replacement Therapy methods
Abstract

Continuous renal replacement therapies (CRRT) are widely used in the treatment of acute kidney injury. Several causes, related to the treatment itself or to the patient's condition, determine the coagulation of the extracorporeal circuit. These interruptions (or down-time) have a negative impact on the effectiveness of the treatment in terms of solute clearance and fluid balance. Historically, the choice of anticoagulant has fallen on unfractionated heparin because it is cheap and easy to use. Today, the use of citrate is recommended in most instances because of its high efficacy and safety. Several studies demonstrate the superiority of citrate in terms of filter survival. The reduction of down-time results in a reduction of the delta between the prescribed dialysis dose and the dose that is actually administered (ml/Kg/hour of collected effluent). The literature also agrees that there is a reduction in the incidence of major bleeding events when citrate is used instead of heparin, although there is no impact on mortality rates. Some technical and clinical complexities, secondary to citrate action both as anticoagulant and buffer, still exist in the use of regional citrate anticoagulation. However, complications due to citrate use, such as acid-base balance disorders and hypocalcaemia, are rare and easily reversible. There is not much data about the costs and benefits of using citrate instead of heparin; according to the experience within our own Unit, we have observed a reduction in costs when the data is normalized for 35 ml of effluent administered. Appropriate protocols, accurate surveillance and the automated management of regional citrate anticoagulation thanks to dedicated software make this technique safe and effective., (Copyright by Società Italiana di Nefrologia SIN, Rome, Italy.)

Published
2019

37. [Hemodialysis and cardiovascular outcome].

Author

Panicali L, Brigante F, and Mancini E

Subjects
Arrhythmias, Cardiac etiology, Cardiovascular Diseases prevention & control, Hemodiafiltration, Hemodynamics, Humans, Hypotension etiology, Kidney Failure, Chronic physiopathology, Risk Factors, Treatment Outcome, Cardiovascular Diseases etiology, Kidney Failure, Chronic blood, Renal Dialysis adverse effects
Abstract

Hemodialysis patients often present multiple comorbidities and have a high mortality rate (15-20% per year), mostly due to cardiovascular events. Besides predisposing pathological conditions related to uremia (heart failure, coronary heart disease, left ventricular hypertrophy, arrhythmias), they also have specific risk factors linked to the hemodialysis (HD) treatment in itself: chronic inflammation, fluid overload, autonomic nervous system dysfunction, arterovenous fistula. These factors may affect the hemodynamic compensatory systems (vascular refilling, arteriolar and venous tone, autonomic nervous system response) to fluid removal, with high risk of intra-dialysis hypotension (IDH) episodes or arrhythmic events. IDH is recognized as associated to a negative long term outcome, due to the repeated episodes of organ hypoperfusion with ischemic damage to heart, brain and gut. Over the years, dialysis technology has greatly improved, with the development of continuous and noninvasive monitoring systems, able to control some hemodynamic parameters affecting blood pressure (mainly blood volume and body temperature), with positive results in terms of hemodynamic instability during HD. Furthermore, recent studies suggest that hemodiafiltration may reduce the risk of IDH and cardiovascular mortality, compared with conventional HD. Diabetic and/or old patients, as well as those with a previous cardiovascular event, are the first patients who should receive the new treatment options. Overall, the HD prescription needs to be tailored to each patient's need, to improve the hemodynamic tolerance to treatment and the cardiovascular outcome., (Copyright by Società Italiana di Nefrologia SIN, Rome, Italy.)

Published
2017

38. Citrate Anticoagulation during Continuous Renal Replacement Therapy.

Author

Ricci D, Panicali L, Facchini MG, and Mancini E

Subjects
Equipment and Supplies, Humans, Renal Replacement Therapy instrumentation, Anticoagulants therapeutic use, Citrates therapeutic use, Renal Replacement Therapy methods
Abstract

During extracorporeal dialysis, some anticoagulation strategy is necessary to prevent the coagulation of blood. Heparin has historically been used as an anticoagulant because of its efficacy combined with low cost. However, a variable incidence of hemorrhagic complications (5-30%) has been documented in patients undergoing continuous renal replacement therapy (CRRT) with heparin as an anticoagulant. Citrate has anticoagulation properties secondary to its ability to chelate calcium, which is necessary for the coagulation cascade. Citrate may thus be used in a regional anticoagulation (RCA), limited to the extracorporeal circuit of CRRT, to avoid systemic anticoagulation. Recent meta-analysis confirmed the advantage of RCA over heparin in terms of incidence of bleeding during CRRT. Moreover, an increase in filter lifespan is documented, with a secondary advantage in reaching the prescribed dialysis dose. In our experience, we could confirm this positive effect. In fact, with a progressive increase in the proportion of CRRT with citrate as RCA, we obtained a reduction in the number of filters used for every 72 h of treatment (from 2.4 in 2011 to 1.3 in 2015), and most importantly, a reduction in the difference between the prescribed and delivered dialysis doses (from 22 to 7%). Citrate has an intense effect on the acid-base balance as well, if fully metabolized through the Krebs cycle, due to the production of bicarbonate. Even more severely ill patients, such as those with liver dysfunction, may be treated with RCA without severe complications, because modern machines for CRRT are equipped with simple systems that are able to manage the citrate infusion and control the calcium levels, with minimal risks of metabolic derangements., (© 2017 S. Karger AG, Basel.)

Published
2017
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39. PTFE grafts versus tunneled cuffed catheters for hemodialysis: which is the second choice when arteriovenous fistula is not feasible?

Author

Donati G, Cianciolo G, Mauro R, Rucci P, Scrivo A, Marchetti A, Giampalma E, Golfieri R, Panicali L, Iorio M, Stella A, La Manna G, and Stefoni S

Subjects
Aged, Aged, 80 and over, Arteriovenous Shunt, Surgical, Female, Humans, Kaplan-Meier Estimate, Male, Middle Aged, Catheters, Indwelling, Kidney Failure, Chronic therapy, Polytetrafluoroethylene chemistry, Renal Dialysis instrumentation
Abstract

Vascular access-related complications are still one of the leading causes of morbidity in hemodialysis patients. The aim of this study was to compare polytetrafluoroethylene (PTFE) grafts versus tunneled cuffed permanent catheters (TCCs) in terms of vascular access and patients' survival. An observational study was carried out with a 2-year follow-up. Eighty-seven chronic hemodialysis patients were enrolled: 31 with a PTFE graft as vascular access for hemodialysis versus 56 with a TCC. Patients' mean age was 63.8 ± 14.6 (grafts) versus 73.5 ± 11.3 years (TCCs), P = 0.001. Significantly more patients with TCC had atrial fibrillation than patients with grafts (30.3% versus 6.5%, P = 0.01). In an unadjusted Kaplan-Meier analysis, median TCC survival at 24 months was 5.4 months longer than that of PTFE grafts but not significantly (log-rank test = 1.3, P = ns). In a Cox regression analysis adjusted for age, gender, number of previous vascular accesses, diabetes, atrial fibrillation, smoking, and any complication, this lack of significant difference in survival of the vascular access between TCC and PTFE groups was confirmed and diabetes proved to be an independent risk factor for the survival of both vascular accesses considered (P = 0.02). In an unadjusted Kaplan-Meier analysis, a higher mortality was found in the TCC group than in the PTFE group at 24 months (log-rank test = 10.07, P < 0.01). The adjusted Cox regression analysis showed that patients with TCC had a 3.2 times higher risk of death than patients with PTFE grafts. When an arteriovenous fistula (AVF) is not possible, PTFE grafts can be considered the vascular access of second choice, whereas TCCs can be used when an AVF or PTFE graft are not feasible or as a bridge to AVF or PTFE graft creation., (Copyright © 2014 International Center for Artificial Organs and Transplantation and Wiley Periodicals, Inc.)

Published
2015
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40. Extracorporeal detoxification for hepatic failure using molecular adsorbent recirculating system: depurative efficiency and clinical results in a long-term follow-up.

Author

Donati G, La Manna G, Cianciolo G, Grandinetti V, Carretta E, Cappuccilli M, Panicali L, Iorio M, Piscaglia F, Bolondi L, Colì L, and Stefoni S

Subjects
Adult, Aged, Aged, 80 and over, Female, Humans, Liver Transplantation, Male, Middle Aged, Prospective Studies, Treatment Outcome, Waiting Lists, Young Adult, Extracorporeal Circulation methods, Liver Failure therapy, Sorption Detoxification methods
Abstract

Acute liver failure and acute-on-chronic liver failure still show a poor prognosis. The molecular adsorbent recirculating system (MARS) has been extensively used as the most promising detoxifying therapy for patients with these conditions. Sixty-four patients with life-threatening liver failure were selected, and 269 MARS treatments were carried out as a bridge for orthotopic liver transplantation (OLT) or for liver function recovery. All patients were grouped according to the aim of MARS therapy. Group A consisted of 47 patients treated for liver function recovery (median age 59 years, range 23-82). Group B consisted of 11 patients on the waiting list who underwent OLT (median age 47 years, range 32-62). Group C consisted of 6 patients on the waiting list who did not undergo OLT (median age 45.5 years, range 36-54, P = 0.001). MARS depurative efficiency in terms of liver toxins, cytokines, and growth factors was assessed together with the clinical outcome of the patients during a 1-year follow-up. Total bilirubin reduction rate per session (RRs) for each MARS session was 23% (range 17-29); direct bilirubin RRs was 28% (21-35), and indirect bilirubin RRs was 8% (3-21). Ammonia RRs was 34% (12-86). Conjugated cholic acid RRs was 58% (48-61); chenodeoxycholic acid RRs was 34% (18-48). No differences were found between groups. Hepatocyte growth factor (HGF) values on starting MARS were 4.1 ng/mL (1.9-7.9) versus 7.9 ng/mL (3.2-14.1) at MARS end (P < 0.01). Cox regression analysis to determine the risk factors predicting patient outcomes showed that age, male gender, and Sequential Organ Failure Assessment score (but not Model for End-stage Liver Disease score) were factors predicting death, whereas the number of MARS sessions and the ΔHGF proved protective factors. Kaplan-Meier survival analysis was also used; after 12 months, 21.3% of patients in Group A survived, while 90.9% were alive in Group B and 16.7% in Group C (log rank = 0.002). In conclusion, MARS was clinically well tolerated by all patients and significantly reduced hepatic toxins. Better survival rates were linked to an OLT program, but patients' clinical characteristics on starting MARS therapy were the main factors predicting survival. The role of HGF should be evaluated in larger clinical trials., (© 2013 Wiley Periodicals, Inc. and International Center for Artificial Organs and Transplantation.)

Published
2014
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41. [Preventing and reducing comorbidity in candidates for kidney transplantation for the improvement of post-operative results].

Author

Mosconi G, Mosconi G, Scolari MP, Feliciangeli G, Liviano D'Arcangelo G, Baraldi O, Fantinati C, Cristino S, Conte D, Lanci N, Panicali L, and Stefoni S

Subjects
Algorithms, Cardiovascular Diseases epidemiology, Cardiovascular Diseases prevention & control, Communicable Diseases epidemiology, Comorbidity, Humans, Immune System Diseases epidemiology, Immune System Diseases prevention & control, Italy epidemiology, Kidney Failure, Chronic surgery, Monitoring, Physiologic, Neoplasms epidemiology, Neoplasms prevention & control, Osteoarthritis epidemiology, Osteoarthritis prevention & control, Practice Guidelines as Topic, Risk Factors, Tissue and Organ Procurement, Kidney Failure, Chronic complications, Kidney Transplantation mortality, Waiting Lists
Abstract

The correct and constant management of transplant waiting lists is necessary for the optimal utilization of the limited number of organs available for transplantation. The guidelines regarding placement on transplant waiting lists (absolute and relative contraindications) are well documented, even though they are in constant development. The criteria for the monitoring of patients on waiting lists, however, are not so well defined; this aspect is subject to careful evaluation on account of the widening of the criteria for transplantation suitability, the increase in the average age of patients, a rise in the number of enrolments and, as a result, prolonged waiting time (in Italy, the average time spent on a waiting list is 37 months). During the waiting period, a greater risk of clinically significant comorbidities and mortality, above all from cardiovascular events, has been noted (the annual mortality is 5-7% in the US, 1.3% in Italy). An in-depth clinical and instrumental study of patients with chronic renal failure is necessary when screening eligible candidates for transplant programs, individualizing therapeutic strategies, and identifying patients for whom the risks outweigh the potential benefits. Clinical and instrumental monitoring, as well as adequate treatment of comorbidities during the waiting period, can help improve the post-transplant outcome. This work examines the study algorithms and monitoring procedures for patients on kidney transplant waiting lists.

Published
2009

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