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1. Enhancing human islet xenotransplant survival and function in diabetic immunocompetent mice through LRH-1/NR5A2 pharmacological activation.

Author

Cobo-Vuilleumier, N., Lorenzo, P. I., Vazquez, E. Martin, Noriega, L. López, Nano, R., Piemonti, L., Martín, F., and Gauthier, B. R.

Abstract

The intricate etiology of type 1 diabetes mellitus (T1D), characterized by harmful interactions between the immune system and insulin-producing beta cells, has hindered the development of effective therapies including human islet transplantation, which requires strong immunosuppressants that impair beta cell survival and function. As such alternative immunomodulating therapies are required for successful transplantation. The discovery that pharmacological activation of the nuclear receptor LRH-1/NR5A2 can reverse hyperglycemia inmousemodels of T1D by altering, and not suppressing the autoimmune attack, prompted us to investigate whether LRH-1/NR5A2 activation could improve human islet function/survival after xenotransplantation in immunocompetent mice. Human islets were transplanted under the kidney capsule of streptozotocin (STZ)-induced diabetic mice, and treatment with BL001 (LRH-1/NR5A2 agonist) or vehicle was administered one week post-transplant. Our study, encompassing 3 independent experiments with 3 different islet donors, revealed that mice treated for 8 weeks with BL001 exhibited lower blood glucose levels correlating with improved mouse survival rates as compared to vehicle-treated controls. Human C-peptide was detectable in BL001-treated mice at both 4 and 8 weeks indicating functional islet beta cells. Accordingly, in mice treated with BL001 for 8 weeks, the beta cell mass was preserved, while a significant decrease in alpha cells was observed compared to mice treatedwith BL001 for only 4 weeks. In contrast, vehicle-treated mice exhibited a reduction in insulin-expressing cells at 8 weeks compared to those at 4 weeks. These results suggest that BL001 significantly enhances the survival, engraftment, and functionality of human islets in a STZ-induced diabetic mouse model. [ABSTRACT FROM AUTHOR]

Published
2024
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4. Targeting CXCR1/2 Does Not Improve Insulin Secretion After Pancreatic Islet Transplantation: A Phase 3, Double-Blind, Randomized, Placebo-Controlled Trial in Type 1 Diabetes

Author

Maffi P., Lundgren T., Tufveson G., Rafael E., Shaw J. A. M., Liew A., Saudek F., Witkowski P., Golab K., Bertuzzi F., Gustafsson B., Daffonchio L., Ruffini P. A., Piemonti L., Nano R., Mercalli A., Lampasona V., Magistretti P., Sordi V., Antonio S., Antonioli B., Galuzzi M., Tosca M. C., De Carlis L., Colussi G., Korsgren O., Pollard H., Maffi, Paola, Lundgren, Torbjörn, Tufveson, Gunnar, Rafael, Ehab, Shaw, James A M, Liew, Aaron, Saudek, Frantisek, Witkowski, Piotr, Golab, Karolina, Bertuzzi, Federico, Gustafsson, Bengt, Daffonchio, Luisa, Ruffini, Pier Adelchi, Piemonti, Lorenzo, Maffi, P, Lundgren, T, Tufveson, G, Rafael, E, Shaw, J, Liew, A, Saudek, F, Witkowski, P, Golab, K, Bertuzzi, F, Gustafsson, B, Daffonchio, L, Ruffini, P, Piemonti, L, Nano, R, Mercalli, A, Lampasona, V, Magistretti, P, Sordi, V, Antonio, S, Antonioli, B, Galuzzi, M, Tosca, M, De Carlis, L, Colussi, G, Korsgren, O, and Pollard, H

Subjects
Male, Time Factors, Endocrinology, Diabetes and Metabolism, Islets of Langerhans Transplantation, Placebo-controlled study, Gastroenterology, Receptors, Interleukin-8B, Receptors, Interleukin-8A, law.invention, Placebos, 0302 clinical medicine, Randomized controlled trial, law, Insulin Secretion, Postoperative Period, 030212 general & internal medicine, Sulfonamides, geography.geographical_feature_category, Clinical Care/Education/Nutrition/Psychosocial Research, Area under the curve, Middle Aged, Islet, Combined Modality Therapy, Female, Immunosuppressive Agents, Adult, medicine.medical_specialty, Adolescent, 030209 endocrinology & metabolism, Placebo, Drug Administration Schedule, Young Adult, Islets of Langerhans, 03 medical and health sciences, Double-Blind Method, Internal medicine, CXCR1/2, insulin secretion, pancreatic islet transplantation, Internal Medicine, medicine, Humans, Aged, Advanced and Specialized Nursing, geography, Type 1 diabetes, business.industry, medicine.disease, Transplantation, Diabetes Mellitus, Type 1, Pancreatic islet transplantation, business
Abstract

OBJECTIVE Reparixin is an inhibitor of CXCR1/2 chemokine receptor shown to be an effective anti-inflammatory adjuvant in a pilot clinical trial in allotransplant recipients. RESEARCH DESIGN AND METHODS A phase 3, multicenter, randomized, double-blind, parallel-assignment study (NCT01817959) was conducted in recipients of islet allotransplants randomized (2:1) to reparixin or placebo in addition to immunosuppression. Primary outcome was the area under the curve (AUC) for C-peptide during the mixed-meal tolerance test at day 75 ± 5 after the first and day 365 ± 14 after the last transplant. Secondary end points included insulin independence and standard measures of glycemic control. RESULTS The intention-to-treat analysis did not show a significant difference in C-peptide AUC at both day 75 (27 on reparixin vs. 18 on placebo, P = 0.99) and day 365 (24 on reparixin vs. 15 on placebo, P = 0.71). There was no statistically significant difference between treatment groups at any time point for any secondary variable. Analysis of patient subsets showed a trend for a higher percentage of subjects retaining insulin independence for 1 year after a single islet infusion in patients receiving reparixin as compared with patients receiving placebo (26.7% vs. 0%, P = 0.09) when antithymocyte globulin was used as induction immunosuppression. CONCLUSIONS In this first double-blind randomized trial, islet transplantation data obtained with reparixin do not support a role of CXCR1/2 inhibition in preventing islet inflammation-mediated damage.

Published
2020

5. Targeting CXCR1/2 does not improve insulin secretion after pancreatic islet transplantation: A phase 3, double-blind, randomized, placebo-controlled trial in type 1 diabetes

Author

Maffi, P, Lundgren, T, Tufveson, G, Rafael, E, Shaw, J, Liew, A, Saudek, F, Witkowski, P, Golab, K, Bertuzzi, F, Gustafsson, B, Daffonchio, L, Ruffini, P, Piemonti, L, Nano, R, Mercalli, A, Lampasona, V, Magistretti, P, Sordi, V, Antonio, S, Antonioli, B, Galuzzi, M, Tosca, M, De Carlis, L, Colussi, G, Korsgren, O, Pollard, H, Maffi P., Lundgren T., Tufveson G., Rafael E., Shaw J. A. M., Liew A., Saudek F., Witkowski P., Golab K., Bertuzzi F., Gustafsson B., Daffonchio L., Ruffini P. A., Piemonti L., Nano R., Mercalli A., Lampasona V., Magistretti P., Sordi V., Antonio S., Antonioli B., Galuzzi M., Tosca M. C., De Carlis L., Colussi G., Korsgren O., Pollard H., Maffi, P, Lundgren, T, Tufveson, G, Rafael, E, Shaw, J, Liew, A, Saudek, F, Witkowski, P, Golab, K, Bertuzzi, F, Gustafsson, B, Daffonchio, L, Ruffini, P, Piemonti, L, Nano, R, Mercalli, A, Lampasona, V, Magistretti, P, Sordi, V, Antonio, S, Antonioli, B, Galuzzi, M, Tosca, M, De Carlis, L, Colussi, G, Korsgren, O, Pollard, H, Maffi P., Lundgren T., Tufveson G., Rafael E., Shaw J. A. M., Liew A., Saudek F., Witkowski P., Golab K., Bertuzzi F., Gustafsson B., Daffonchio L., Ruffini P. A., Piemonti L., Nano R., Mercalli A., Lampasona V., Magistretti P., Sordi V., Antonio S., Antonioli B., Galuzzi M., Tosca M. C., De Carlis L., Colussi G., Korsgren O., and Pollard H.

Abstract

OBJECTIVE Reparixin is an inhibitor of CXCR1/2 chemokine receptor shown to be an effective anti-inflammatory adjuvant in a pilot clinical trial in allotransplant recipients. RESEARCH DESIGN AND METHODS A phase 3, multicenter, randomized, double-blind, parallel-assignment study (NCT01817959) was conducted in recipients of islet allotransplants randomized (2:1) to reparixin or placebo in addition to immunosuppression. Primary outcome was the area under the curve (AUC) for C-peptide during the mixed-meal tolerance test at day 75 6 5 after the first and day 365 6 14 after the last transplant. Secondary end points included insulin independence and standard measures of glycemic control. RESULTS The intention-to-treat analysis did not show a significant difference in C-peptide AUC at both day 75 (27 on reparixin vs. 18 on placebo, P 5 0.99) and day 365 (24 on reparixin vs. 15 on placebo, P 5 0.71). There was no statistically significant difference between treatment groups at any time point for any secondary variable. Analysis of patient subsets showed a trend for a higher percentage of subjects retaining insulin independence for 1 year after a single islet infusion in patients receiving reparixin as compared with patients receiving placebo (26.7% vs. 0%, P 5 0.09) when antithymocyte globulin was used as induction immunosuppression. CONCLUSIONS In this first double-blind randomized trial, islet transplantation data obtained with reparixin do not support a role of CXCR1/2 inhibition in preventing islet inflammation-mediated damage.

Published
2020

9. In vitro assessment of radiobiology of meningioma: A pilot study

Author

Pinzi, V, Bisogno, I, Ciusani, E, Canazza, A, Calatozzolo, C, Vetrano, I, Pasi, F, De Martin, E, Fumagalli, M, Nano, R, Fariselli, L, Pinzi V., Bisogno I., Ciusani E., Canazza A., Calatozzolo C., Vetrano I. G., Pasi F., De Martin E., Fumagalli M. L., Nano R., Fariselli L., Pinzi, V, Bisogno, I, Ciusani, E, Canazza, A, Calatozzolo, C, Vetrano, I, Pasi, F, De Martin, E, Fumagalli, M, Nano, R, Fariselli, L, Pinzi V., Bisogno I., Ciusani E., Canazza A., Calatozzolo C., Vetrano I. G., Pasi F., De Martin E., Fumagalli M. L., Nano R., and Fariselli L.

Abstract

Background: Meningioma are the second most common brain tumors in adults and can cause significant morbidity and mortality. The scarcity of in vitro and in vivo models represents the major obstacle to understand the molecular basis of meningioma tumorigenesis. The main aim of this study was to assess a method for radiobiology of meningioma cells colture by means of well-known meningioma lines. New method: We carried out a protocol of cells culture for irradiation of meningioma cells. We used the immortalized cell lines IOMM-Lee and CH-157 to study their radiation-reponse by means of clonogenic assays and to evaluate their proliferation and apoptosis. We irradiated the cells with different total doses using two different linear accelerators. Results: We observed a more radiation resistance of the IOMM-Lee than the CH-157. Indeed, the cellular death of CH-157 was obtained at a very low dose irradiation. Moreover, we showed a dose-response effect due to the early and late apoptosis, in fact the rate of apoptotic cells is greater than that of the necrotic cells at any dose of irradiation and at any time of analysis. Comparison with existing methods: There is not a standardized method for radiobiology of meningioma experiments. Conclusions: Our method of cells culture appears suitable for radiosensitivity studies on meningioma. We can confirm that the response to radiotherapy depends not only on irradiation features, but also on tumor radiosensitivity.

Published
2019

28. Analysis and characterization of the X-ray beam produced by a PF device for radiotherapy applications

Author

SUMINI, MARCO, MOSTACCI, DOMIZIANO, VIRELLI, ANGELA, ZIRONI, ISABELLA, CASTELLANI, GASTONE, PREVITI, ALBERTO, Galassi, D., Ceccolini, E., Rocchi, F., Tartari, A., Pasi, F., Facoetti, A., Mazzini, G., Nano, R., Cucchi, G., Orecchia, R., Sumini, M., Previti, A., Galassi, D., Ceccolini, E., Rocchi, F., Mostacci, D., Tartari, A., Pasi, F., Facoetti, A., Mazzini, G., Nano, R., Virelli, A., Zironi, I., Castellani, G., Cucchi, G., and Orecchia, R.

Subjects
Plasma Focu, Electron beam, X-ray, Radiotherapy, Dose rate
Abstract

A plasma focus device, devoted to the study of a possible application to the radiotherapy treatment of malignant cells, has been recently put into operation. The low-energy (up to 200 keV) X-rays are produced by conversion of the electron beam generated by the device during the pinch phase. The X-ray spectrum has already been fully characterized, and an initial campaign of irradiation of specific cell cultures has been completed. At present, the links between the operational parameters of the actual device, the beam intensity, and the cell irradiation effects are being analyzed, trying to evaluate the advantage of the very high dose rate that can be delivered, of the order of several Gy in a few tens of nanoseconds. Preliminary results on radiobiological effectiveness are presented and discussed.

Published
2015

29. MR Imaging Monitoring of Iron-Labeled Pancreatic Islets in a Small Series of Patients: Islet Fate in Successful, Unsuccessful, and Autotransplantation

Author

Malosio, Ml, ESPOSITO, ANTONIO, Brigatti, C, Palmisano, A, PIEMONTI, LORENZO, Nano, R, Maffi, P, DE COBELLI, FRANCESCO, DEL MASCHIO, ALESSANDRO, SECCHI, ANTONIO, PALMISANO , ANNA, Malosio, Ml, Esposito, Antonio, Brigatti, C, Palmisano, A, Piemonti, Lorenzo, Nano, R, Maffi, P, DE COBELLI, Francesco, DEL MASCHIO, Alessandro, Secchi, Antonio, and Pathology/molecular and cellular medicine

Subjects
Adult, Male, medicine.medical_specialty, medicine.medical_treatment, Biomedical Engineering, Urology, Islets of Langerhans Transplantation, lcsh:Medicine, Pilot Projects, contrast media, Transplantation, Autologous, Diabetes mellitus, medicine, Journal Article, Humans, magnetic resonance imaging, Magnetite Nanoparticles, Aged, Transplantation, Type 1 diabetes, geography, geography.geographical_feature_category, medicine.diagnostic_test, business.industry, Pancreatic islets, Research Support, Non-U.S. Gov't, lcsh:R, Magnetic resonance imaging, Dextrans, Cell Biology, Middle Aged, clinical study, medicine.disease, Islet, Autotransplantation, Surgery, medicine.anatomical_structure, Diabetes Mellitus, Type 1, Pancreatic islet transplantation, Female, business
Abstract

Islet transplantation is one of the most promising and effective therapies for restoring normoglycemia in type 1 diabetes (T1D) patients, but islet engraftment is one of the main obstacles hampering long-term success. Monitoring graft loss, caused either by immunological or nonimmunological events, occurring in the first phase after transplantation and at later stages of a patient's life is a very important issue. Among the imaging approaches previously applied, magnetic resonance imaging (MRI) monitoring of islet fate following labeling with superparamagnetic iron oxide agents yielded promising results. The aim of this study was to translate into patients the method of islet labeling and MRI monitoring developed in our preclinical setting and to compare imaging results with graft clinical outcome. Three T1D patients and one nondiabetic patient undergoing autotransplantation following subtotal pancreatectomy received Endorem®-labeled islets. Patients were monitored by MRI and metabolically (HbA1c, exogenous insulin requirement, and C-peptide, TEF) at 1, 3, and 7 days following transplantation and once a month up to 10 months. Labeled transplanted islets appeared as hypointense areas scattered within the liver parenchyma, whose absolute number at 24 h after transplantation reflected the labeling efficiency. In patients #1 and #3 with good midterm graft function, MRI follow-up showed an important early loss of hypointense spots followed by a slow and progressive disappearance at later timepoints. Graft loss of function in patient #2 4 weeks after transplantation was associated with the complete disappearance of all hypointense signals. The autotransplanted patient, stably insulin free, showed no significant signal reduction during the first 3 days, followed by loss of spots similar to a patient with good midterm graft function. These results suggest that MRI monitoring of islet transplantation at early time points could represent a meaningful readout for helping in predicting transplant failure or success, but its relevance for mid/long-term islet function assessment appears evanescent.

Published
2015

30. Relaparotomy for a pancreatic fistula after a pancreaticoduodenectomy: A comparison of different surgical strategies

Author

Balzano, G, Pecorelli, N, Piemonti, L, Ariotti, R, Carvello, M, Nano, R, Braga, M, Staudacher, C, Balzano G, Pecorelli N, PIEMONTI , LORENZO, Ariotti R, Carvello M, Nano R, BRAGA, MARCO, Staudacher C., Balzano, G, Pecorelli, N, Piemonti, L, Ariotti, R, Carvello, M, Nano, R, Braga, M, Staudacher, C, Balzano G, Pecorelli N, PIEMONTI , LORENZO, Ariotti R, Carvello M, Nano R, BRAGA, MARCO, and Staudacher C.

Abstract

Introduction A relaparotomy for a pancreatic fistula (PF) after a pancreaticoduodenectomy (PD) is a formidable operation, and the appropriate treatment of anastomotic leakage is under debate. The objective of this study was to compare the outcomes of different strategies in managing the pancreatic remnant during a relaparotomy for PF after a PD. Methods In this retrospective study on prospectively collected data, 669 PD were performed between 2004 and 2011. The study group comprised 31 patients requiring a relaparotomy, because of delayed haemorrhage (n = 19) or sepsis (n = 12). The pancreatic stump was treated either using pancreas-preserving techniques (simple drainage or duct occlusion) or completion of a pancreatectomy (CP). In 2008, autologous islet transplantation (AIT) was introduced for endocrine tissue rescue of CP. Results The mortality rate, blood loss and transfusion requirement were similar for all techniques. Patients undergoing a CP required a further relaparotomy less frequently than patients with pancreas preservation (7% versus 59%, P < 0.01), and the intensive care unit (ICU) stay was reduced after CP (P = 0.058). PF persisted at discharge in 66% of patients after pancreas-preserving techniques. AIT was associated with CP in 7 patients, of whom one died post-operatively. Long-term graft function was maintained in four out of six surviving patients, with one insulin-independent patient at 36 months after transplantation. Conclusions When a PF requires a relaparotomy, CP has become our favoured technique. AIT can reduce the metabolic impact of the procedure.

Published
2014

31. Calcineurin inhibitor-free immunosuppressive regimen in type 1 diabetes patients receiving islet transplantation: single-group phase 1/2 trial

Author

Maffi P, Berney T, Nano R, Niclauss N, Bosco D, Melzi R, Mercalli A, Magistretti P, DE COBELLI , FRANCESCO, BATTAGLIA, MARCO MARIA, Scavini M, Demuylder-mischler S, SECCHI , ANTONIO, PIEMONTI, LORENZO, Maffi, P, Berney, T, Nano, R, Niclauss, N, Bosco, D, Melzi, R, Mercalli, A, Magistretti, P, DE COBELLI, Francesco, Battaglia, MARCO MARIA, Scavini, M, Demuylder-mischler, S, Secchi, Antonio, and Piemonti, Lorenzo

Published
2014

32. Extending indications for islet autotransplantation in pancreatic surgery

Author

Balzano, G, Maffi, P, Nano, R, Zerbi, A, Venturini, M, Melzi, R, Mercalli, A, Magistretti, P, Scavini, M, Castoldi, R, Carvello, M, Braga, M, Del Maschio, A, Secchi, A, Staudacher, C, Piemonti, L, Balzano G, Maffi P, Nano R, Zerbi A, Venturini M, Melzi R, Mercalli A, Magistretti P, Scavini M, Castoldi R, Carvello M, Braga M, Del Maschio A, Secchi A, Staudacher C, Piemonti L, Balzano, G, Maffi, P, Nano, R, Zerbi, A, Venturini, M, Melzi, R, Mercalli, A, Magistretti, P, Scavini, M, Castoldi, R, Carvello, M, Braga, M, Del Maschio, A, Secchi, A, Staudacher, C, Piemonti, L, Balzano G, Maffi P, Nano R, Zerbi A, Venturini M, Melzi R, Mercalli A, Magistretti P, Scavini M, Castoldi R, Carvello M, Braga M, Del Maschio A, Secchi A, Staudacher C, and Piemonti L

Abstract

OBJECTIVE:: To assess metabolic and oncologic outcomes of islet autotransplantation (IAT) in patients undergoing pancreatic surgery for either benign or malignant disease. BACKGROUND:: IAT is performed to improve glycemic control after extended pancreatectomy, almost exclusively in patients with chronic pancreatitis. Limited experience is available for other indications or in patients with pancreatic malignancy. METHODS:: In addition to chronic pancreatitis, indications for IAT were grade C pancreatic fistula (treated with completion or left pancreatectomy, as indicated); total pancreatectomy as an alternative to high-risk anastomosis during pancreaticoduodenectomy; and distal pancreatectomy for benign/borderline neoplasm of pancreatic body-neck. Malignancy was not an exclusion criterion. Metabolic and oncologic follow-up is presented. RESULTS:: From November 2008 to June 2012, 41 patients were candidates to IAT (accounting for 7.5% of all pancreatic resections). Seven of 41 did not receive transplantation for inadequate islet mass (4 pts), patient instability (2 pts), or contamination of islet culture (1 pt). IAT-related complications occurred in 8 pts (23.5%): 4 bleeding, 3 portal thromboses (1 complete, 2 partial), and 1 sepsis. Median follow-up was 546 days. Fifteen of 34 patients (44%) reached insulin independence, 16 patients (47%) had partial graft function, 2 patients (6%) had primary graft nonfunction, and 1 patient (3%) had early graft loss. Seventeen IAT recipients had malignancy (pancreatic or periampullary adenocarcinoma in 14). Two of them had already liver metastases at surgery, 13 were disease-free at last follow-up, and none of 2 patients with tumor recurrence developed metastases in the transplantation site. CONCLUSIONS:: Although larger data are needed to definitely exclude the risk of disease dissemination, the present study suggests that IAT indications can be extended to selected patients with neoplasm.

Published
2013

33. Cytoskeleton actin changes in IL-2 activated cells

Author

Capelli, E., Nano, R., Panelli, S., Sciola, L., Alessandra SPANO, and Barni, S.

Subjects
lcsh:Biology (General), QH301-705.5, macromolecular substances, Biology (General), lcsh:QH301-705.5
Abstract

In the present study we analysed the changes in cytoskeletal actin in lymphoid cells following IL-2 activation and during cell interactions by means of light and electron microscopy, immunofluorescence and molecular analysis. By morphological analysis we observed a higher fluorescence in the activated cells than in the quiescent ones with no modifications in the cytoskeleton pattern comparing activated to resting cells. The results of molecular analysis indicate that, after IL-2 activation, there is a reorganisation of the actin component of the cell cytoskeleton accompanied by the differential expression of the corresponding genes. A future study will be extended to the analysis of others components of the cytoskeleton network.

Published
2009

34. Liver perfusion changes occurring during pancreatic islet engraftment: a dynamic contrast-enhanced magnetic resonance study

Author

ESPOSITO, ANTONIO, DE COBELLI, FRANCESCO, PIEMONTI, LORENZO, SECCHI, ANTONIO, DEL MASCHIO, ALESSANDRO, Palmisano, A, Maffi, P, Malosio, Ml, Nano, R, Canu, T, Ironi, G, PALMISANO , ANNA, Esposito, Antonio, Palmisano, A, Maffi, P, Malosio, Ml, Nano, R, Canu, T, DE COBELLI, Francesco, Piemonti, Lorenzo, Ironi, G, Secchi, Antonio, and DEL MASCHIO, Alessandro

Subjects
Adult, Male, medicine.medical_specialty, Liver perfusion, Urology, Islets of Langerhans Transplantation, Internal medicine, medicine, Magnetic resonance study, Immunology and Allergy, Humans, Pharmacology (medical), Aged, Transplantation, geography, geography.geographical_feature_category, medicine.diagnostic_test, business.industry, Pancreatic islets, Magnetic resonance imaging, Middle Aged, Islet, Magnetic Resonance Imaging, Dynamic contrast, Endocrinology, medicine.anatomical_structure, Diabetes Mellitus, Type 1, Liver, Microvessels, Pancreatic islet transplantation, Female, business
Abstract

The aim of this study was to investigate liver microvascular adaptation following the intraportal infusion of pancreatic islets (pancreatic islet transplantation [islet-tx]) in diabetic patients using dynamic contrast-enhanced magnetic resonance imaging (DCE-MRI). DCE-MRI was performed before and 7 days after islet-tx in six diabetic patients. Initial area under curve (AUC60) and volume transfer coefficient (Ktrans) were assessed as markers of liver perfusion. Clinical and metabolic monthly follow-up was performed in all patients, considering fasting C-peptide and β-score as main indices of graft function. High variability in the response of liver microvasculature to islet infusion was observed: two patients showed a significant reduction in liver perfusion after transplantation (pt.2: AUC60 = −23.4%, Ktrans = −31.7%; pt.4: AUC60 = −23.7%, Ktrans = −27.9%); three patients did not show any significant variation of liver perfusion and one patient showed a significant increase (pt.3: AUC60 = +31%, Ktrans = +42.8%). Interestingly, a correlation between DCE-MRI parameters and indices of graft function was observed and, in particular, both patients with DCE-MRI evidence of posttransplantation liver perfusion reduction experienced premature graft failure. Our preliminary study demonstrated that DCE-MRI may identify different adaptive responses of liver microvasculature in patients submitted to islet-tx. These different responses could have an impact on islet engraftment, although reported findings need confirmation from larger studies.

Published
2013

36. Early Effects Comparison of X-Rays Delivered at High and Low Dose-rate Pulses on Human Tumor Cells

Author

ZIRONI, ISABELLA, VIRELLI, ANGELA, CECCOLINI, ELISA, ROCCHI, FEDERICO, MOSTACCI, DOMIZIANO, CUCCHI, GIORGIO, CASTELLANI, GASTONE, SUMINI, MARCO, Pasi, F., Nano, R., Facoetti, A., Fiore, M. R., Orecchia, R., Zironi, I., Virelli, A., Pasi, F., Ceccolini, E., Nano, R., Rocchi, F., Facoetti, A., Mostacci, D., Fiore, M.R., Cucchi, G., Castellani, G., Sumini, M., and Orecchia, R.

Subjects
biological effects, radiation therapy
Published
2013

37. Laparoscopic Spleen Preserving Distal Pancreatectomy with Autologous Islet Transplantation. A New Minimally Invasive Technique To Treat Benign Neoplasm of the Pancreatic Body. Case Series of 3 Patients

Author

Carvello MM, Balzano G, Maffi P, Mercalli A, Melzi R, Angiolini R, Ariotti R, Nano R, Braga M, Orsenigo E, Staudacher C, PIEMONTI , LORENZO, Carvello, Mm, Balzano, G, Maffi, P, Mercalli, A, Melzi, R, Angiolini, R, Ariotti, R, Nano, R, Braga, M, Orsenigo, E, Staudacher, C, and Piemonti, Lorenzo

Published
2012

43. ANTICANCER RESEARCH

Author

Altieri, S., Ballarini, F., Bortolussi, S., Postuma, I., Protti, N., Nano, R., Rovelli, C., Cansolino, L., Clerici, A. M., Ferrari, C., Laura, Ciani, Sandra, Ristori, Panza, L., Lanzardo, S., Deagostino, A., GENINATTI CRICH, Simonetta, and Aime, Silvio

Subjects
NEUTRON CAPTURE THERAPY
Published
2014

44. BIOLOGIA - Cellula e Tessuti 2°edizione

Author

Bacci, S, Canapa, A, Cimini, Am, Cioni, C, Colasanti, M, Colombo, R, Della Giovampaola, C., Deri, P, Ferri, D, Gornati, R, Liquori, Ge, Luparello, C, Nano, R, Odierna, G, Olmo, E, Ottaviani, E, Panzica, Gc, Rosati, F, Rossi, Ar, Sciola, Gl, and Sinatra, Fulvia

Published
2014

46. Biologia - Cellula e Tessuti (Seconda Edizione), a cura di R. Colombo e E. Olmo

Author

Bacci, S., Canapa, A., Cimini, A. M., Cioni, C., Colasanti, M., Colombo, R., DELLA GIOVAMPAOLA, C., Deri, Paolo, Ferri, D., Gornati, R., Liquori, G. E., Luparello, C., Nano, R., Odierna, G., Olmo, E., Ottaviani, E., Panzica, G. C., Rosati, F., Rossi, A. R., Sciola, G. L., and Sinatra, F.

Published
2014

47. NEUTRON CAPTURE THERAPY RESEARCH AT INFN AND UNIVERSITY OF PAVIA

Author

Altieri, S., Ballarini, F., Bortolussi, S., Postuma, I., Protti, N., Nano, R., Rovelli, C., Cansolino, L., Clerici, A. M., Ferrari, C., Ciani, L., Ristori, S., Panza, L., Lanzardo, Stefania, Deagostino, Annamaria, GENINATTI CRICH, Simonetta, and Aime, Silvio

Published
2014

49. Kidney Function after Islet Transplant Alone in Type 1 Diabetes: Impact of immunosuppressive therapy on progression of diabetic nephropathy

Author

Maffi, P, Bertuzzi, F, De Taddeo, F, Magistretti, P, Nano, R, Fiorina, P, Caumo, A, Pozzi, P, Socci, C, Venturini, M, Del Maschio, A, Secchi, A, Maffi, P, Bertuzzi, F, De Taddeo, F, Magistretti, P, Nano, R, Fiorina, P, Caumo, A, Pozzi, P, Socci, C, Venturini, M, DEL MASCHIO, Alessandro, and Secchi, Antonio

Abstract

OBJECTIVE— Islet transplantation alone is an alternative for the replacement of pancreatic endocrine function in patients with type 1 diabetes. The aim of our study was to assess the impact of the Edmonton immunosuppressive protocol (tacrolimus-sirolimus association) on kidney function. RESEARCH DESIGN AND METHODS— Nineteen patients with type 1 diabetes and metabolic instability received islet transplantation alone and immunosuppressive therapy according to the Edmonton protocol. Serum creatinine (sCr), creatinine clearance (CrCl), and 24-h urinary protein excretion (UPE) were assessed at baseline and during a follow-up of 339 patientmonths. RESULTS— After islet transplantation we observed 1) sCr within the normal range in all but two patients in whom sCr increased immediately after islet transplantation, and despite withdrawal of immunosuppression, patients progressed to end-stage renal disease (ESRD); 2) CrCl remained within the normal range for those patients who had normal baseline values and decreased, progressing to ESRD in two patients with a decreased baseline CrCl; and 3) 24-h UPE worsened (300 mg/24 h) in four patients. In the two patients who progressed to ESRD, the worsening of 24-h UPE occurred immediately after islet transplantation. In one patient 24-h UPE worsening occurred at 18 months, and, after withdrawal of immunosuppression, it returned to the normal range. In another patient 24-h UPE increased at 24 months and remained stable while immunosuppression was continued. CONCLUSIONS— In type 1 diabetic patients receiving islet transplantation alone, the association of tacrolimus and sirolimus should be used only in patients with normal kidney function. Alternative options for immunosuppressive treatment should be considered for patients with even a mild decrease of kidney function.

Published
2007

50. Islet transplantation in type 1 diabetes: overall experience in a single Center

Author

Maffi P, Bertuzzi F, Nano R, De Taddeo F, Magistretti P, Antonioli B, Venturini M, DEL MASCHIO, ALESSANDRO, Secchi A., PIEMONTI , LORENZO, Maffi, P, Bertuzzi, F, Nano, R, De Taddeo, F, Magistretti, P, Antonioli, B, Venturini, M, Piemonti, Lorenzo, DEL MASCHIO, Alessandro, and Secchi, A.

Published
2007

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