Your search keyword '"Budelli, Silvia"' showing total 8 results

1. First clinical application of cord blood mesenchymal stromal cells in children with multi-drug resistant nephrotic syndrome.

Author

Morello, William, Budelli, Silvia, Bernstein, Daniel Ari, Montemurro, Tiziana, Montelatici, Elisa, Lavazza, Cristiana, Ghio, Luciana, Edefonti, Alberto, Peruzzi, Licia, Molino, Daniela, Benetti, Elisa, Gianoglio, Bruno, Mehmeti, Florian, Catenacci, Laura, Rotella, Jessica, Tamburello, Chiara, Moretta, Antonia, Lazzari, Lorenza, Giordano, Rosaria, and Prati, Daniele

Subjects

*CORD blood, *STROMAL cells, *NEPHROTIC syndrome, *CLINICAL medicine, *REGULATORY T cells, *CHILD patients

Abstract

Background and objectives: Children with multi-drug resistant idiopathic nephrotic syndrome (MDR-INS) usually progress to end-stage kidney disease with a consistent risk of disease recurrence after transplantation. New therapeutic options are needed for these patients. Mesenchymal stromal cells (MSCs) are multipotential non-hematopoietic cells with several immunomodulatory properties and growing clinical applications. Cord blood-derived MSC have peculiar anti-inflammatory and immunosuppressive properties. We aimed at assessing safety and efficacy of cord-blood-derived MSCs (CB-MSCs) in children with MDR-INS. Design, setting, participants: Prospective, open-label, single arm phase I–II pilot study. Pediatric patients with MDR-INS, resistant to at least two lines of therapy, were enrolled. Allogenic CB-MSCs were administered intravenously on days 0, 14, and 21 at a dose of 1.5 × 106 cells/kg. Patients were followed for at least 12 months. The primary outcomes were safety and toxicity. The secondary outcome was remission at 12 months evaluated by urinary protein/urinary creatinine ratio (uPr/uCr). Circulating regulatory T cells (Tregs) were monitored. Results: Eleven pediatric patients with MDR-INS (10 females, median age 13 years) resistant to a median of 3 previous lines of therapy were enrolled. All patients completed the CB-MSC infusion schedule. No patient experienced any infusion-related adverse event or toxicity. Nine patients were assessable for efficacy. At the 12 months follow-up after the treatment, the median uPr/uCr did not change significantly from baseline (8.13 vs. 9.07; p = 0.98), while 3 patients were in partial or complete remission. A lower baseline uPr/uCr was a predictor of remission (2.55 vs. 8.74; p = 0.0238). Tregs count was not associated with CB-MSCs therapy. Conclusions: CB-MSCs are safe and may have a role in the immunosuppressive therapy of pediatric patients with MDR-INS. This preliminary experience paves the way toward further phase II studies addressing MSC efficacy in immune-mediated kidney diseases. [ABSTRACT FROM AUTHOR]

Published

2022

2. Process development and validation of expanded regulatory T cells for prospective applications: an example of manufacturing a personalized advanced therapy medicinal product.

Author

Lavazza, Cristiana, Budelli, Silvia, Montelatici, Elisa, Viganò, Mariele, Ulbar, Francesca, Catani, Lucia, Cannone, Marta Giulia, Savelli, Sara, Groppelli, Elisa, Lazzari, Lorenza, Lemoli, Roberto M., Cescon, Matteo, La Manna, Gaetano, Giordano, Rosaria, and Montemurro, Tiziana

Subjects

*REGULATORY T cells, *T cells, *TYPE 1 diabetes, *CURRENT good manufacturing practices, *GRAFT versus host disease, *MANUFACTURING cells, *IMMUNOLOGICAL tolerance, *RESEARCH, *CELLULAR therapy, *RESEARCH methodology, *EVALUATION research, *COMPARATIVE studies, *RESEARCH funding, *LONGITUDINAL method

Abstract

Background: A growing number of clinical trials have shown that regulatory T (Treg) cell transfer may have a favorable effect on the maintenance of self-tolerance and immune homeostasis in different conditions such as graft-versus-host disease (GvHD), solid organ transplantation, type 1 diabetes, and others. In this context, the availability of a robust manufacturing protocol that is able to produce a sufficient number of functional Treg cells represents a fundamental prerequisite for the success of a cell therapy clinical protocol. However, extended workflow guidelines for nonprofit manufacturers are currently lacking. Despite the fact that different successful manufacturing procedures and cell products with excellent safety profiles have been reported from early clinical trials, the selection and expansion protocols for Treg cells vary a lot. The objective of this study was to validate a Good Manufacturing Practice (GMP)-compliant protocol for the production of Treg cells that approaches the whole process with a risk-management methodology, from process design to completion of final product development. High emphasis was given to the description of the quality control (QC) methodologies used for the in-process and release tests (sterility, endotoxin test, mycoplasma, and immunophenotype).Results: The GMP-compliant protocol defined in this work allows at least 4.11 × 109 Treg cells to be obtained with an average purity of 95.75 ± 4.38% and can be used in different clinical settings to exploit Treg cell immunomodulatory function.Conclusions: These results could be of great use for facilities implementing GMP-compliant cell therapy protocols of these cells for different conditions aimed at restoring the Treg cell number and function, which may slow the progression of certain diseases. [ABSTRACT FROM AUTHOR]

Published

2022

3. Off-the-Shelf Cord-Blood Mesenchymal Stromal Cells: Production, Quality Control, and Clinical Use.

Author

Montemurro, Tiziana, Lavazza, Cristiana, Montelatici, Elisa, Budelli, Silvia, La Rosa, Salvatore, Barilani, Mario, Mei, Cecilia, Manzini, Paolo, Ratti, Ilaria, Cimoni, Silvia, Brasca, Manuela, Prati, Daniele, Saporiti, Giorgia, Astori, Giuseppe, Elice, Francesca, Giordano, Rosaria, and Lazzari, Lorenza

Subjects

*STROMAL cells, *QUALITY control, *DYSPLASIA, *CURRENT good manufacturing practices, *CORD blood, *MANUFACTURING processes

Abstract

Background Recently, mesenchymal stromal cells (MSCs) have gained recognition for their clinical utility in transplantation to induce tolerance and to improve/replace pharmacological immunosuppression. Cord blood (CB)-derived MSCs are particularly attractive for their immunological naivety and peculiar anti-inflammatory and anti-apoptotic properties. Objectives: The objective of this study was to obtain an inventory of CB MSCs able to support large-scale advanced therapy medicinal product (ATMP)-based clinical trials. Study design: We isolated MSCs by plastic adherence in a GMP-compliant culture system. We established a well-characterized master cell bank and expanded a working cell bank to generate batches of finished MSC(CB) products certified for clinical use. The MSC(CB) produced by our facility was used in approved clinical trials or for therapeutic use, following single-patient authorization as an immune-suppressant agent. Results: We show the feasibility of a well-defined MSC manufacturing process and describe the main indications for which the MSCs were employed. We delve into a regulatory framework governing advanced therapy medicinal products (ATMPs), emphasizing the need of stringent quality control and safety assessments. From March 2012 to June 2023, 263 of our Good Manufacturing Practice (GMP)-certified MSC(CB) preparations were administered as ATMPs in 40 subjects affected by Graft-vs.-Host Disease, nephrotic syndrome, or bronco-pulmonary dysplasia of the newborn. There was no infusion-related adverse event. No patient experienced any grade toxicity. Encouraging preliminary outcome results were reported. Clinical response was registered in the majority of patients treated under therapeutic use authorization. Conclusions: Our 10 years of experience with MSC(CB) described here provides valuable insights into the use of this innovative cell product in immune-mediated diseases. [ABSTRACT FROM AUTHOR]

Published

2024

4. A comprehensive report of long-term stability data for a range ATMPs: A need to develop guidelines for safe and harmonized stability studies.

Author

Capelli, Chiara, Frigerio, Simona, Lisini, Daniela, Nava, Sara, Gaipa, Giuseppe, Belotti, Daniela, Cabiati, Benedetta, Budelli, Silvia, Lazzari, Lorenza, Bagnarino, Jessica, Tanzi, Matteo, Comoli, Patrizia, Perico, Norberto, Introna, Martino, and Golay, Josée

Subjects

*ENDOTOXINS, *DRUGS, *EXCIPIENTS, *DRUG standards, *LIQUID nitrogen, *CELL survival, *CURRENT good manufacturing practices

Abstract

Advanced therapy medicinal products (ATMPs) are novel drugs based on genes, cells or tissues developed to treat many different diseases. Stability studies of each new ATMP need to be performed to define its shelf life and guarantee efficacy and safety upon infusion, and these are presently based on guidelines originally drafted for standard pharmaceutical drugs, which have properties and are stored in conditions quite different from cell products. The aim of this report is to provide evidence-based information for stability studies on ATMPs that will facilitate the interlaboratory harmonization of practices in this area. We have collected and analyzed the results of stability studies on 19 different cell-based experimental ATMPs, produced by five authorized cell factories forming the Lombardy "Plagencell network" for use in 36 approved phase I/II clinical trials; most were cryopreserved and stored in liquid nitrogen vapors for 1 to 13 years. The cell attributes collected in stability studies included cell viability, immunophenotype and potency assays, in particular immunosuppression, cytotoxicity, cytokine release and proliferation/differentiation capacity. Microbiological attributes including sterility, endotoxin levels and mycoplasma contamination were also analyzed. All drug products (DPs), cryopreserved in various excipients containing 10% DMSO and in different primary containers, were very stable long term at <–150°C and did not show any tendency for diminished viability or efficacy for up to 13.5 years. Our data indicate that new guidelines for stability studies, specific for ATMPs and based on risk analyses, should be drafted to harmonize practices, significantly reduce the costs of stability studies without diminishing safety. Some specific suggestions are presented in the discussion. [ABSTRACT FROM AUTHOR]

Published

2022

5. Finding a new therapeutic approach for no-option Parkinsonisms: mesenchymal stromal cells for progressive supranuclear palsy.

Author

Canesi, Margherita, Giordano, Rosaria, Lazzari, Lorenza, Isalberti, Maurizio, Isaias, Ioannis Ugo, Benti, Riccardo, Rampini, Paolo, Marotta, Giorgio, Colombo, Aurora, Cereda, Emanuele, Dipaola, Mariangela, Montemurro, Tiziana, ViganÒ, Mariele, Budelli, Silvia, Montelatici, Elisa, Lavazza, Cristiana, Cortelezzi, Agostino, Pezzoli, Gianni, and Viganò, Mariele

Subjects

*PARKINSONIAN disorders, *PROGRESSIVE supranuclear palsy, *NEURODEGENERATION, *CEREBRAL arteries, *DISEASE progression, *STEM cell transplantation, *BONE marrow, *CLINICAL trials, *COMPARATIVE studies, *CONNECTIVE tissue cells, *KINEMATICS, *LONGITUDINAL method, *RESEARCH methodology, *MEDICAL cooperation, *RESEARCH, *POSITRON emission tomography, *EVALUATION research, *SINGLE-photon emission computed tomography, *THERAPEUTICS

Abstract

Background: The trophic, anti-apoptotic and regenerative effects of bone marrow mesenchymal stromal cells (MSC) may reduce neuronal cell loss in neurodegenerative disorders.Methods: We used MSC as a novel candidate therapeutic tool in a pilot phase-I study for patients affected by progressive supranuclear palsy (PSP), a rare, severe and no-option form of Parkinsonism. Five patients received the cells by infusion into the cerebral arteries. Effects were assessed using the best available motor function rating scales (UPDRS, Hoehn and Yahr, PSP rating scale), as well as neuropsychological assessments, gait analysis and brain imaging before and after cell administration.Results: One year after cell infusion, all treated patients were alive, except one, who died 9 months after the infusion for reasons not related to cell administration or to disease progression (accidental fall). In all treated patients motor function rating scales remained stable for at least six-months during the one-year follow-up.Conclusions: We have demonstrated for the first time that MSC administration is feasible in subjects with PSP. In these patients, in whom deterioration of motor function is invariably rapid, we recorded clinical stabilization for at least 6 months. These encouraging results pave the way to the next randomized, placebo-controlled phase-II study that will definitively provide information on the efficacy of this innovative approach. Trial registration ClinicalTrials.gov NCT01824121. [ABSTRACT FROM AUTHOR]

Published

2016

6. Adipogenic potential in human mesenchymal stem cells strictly depends on adult or foetal tissue harvest.

Author

Ragni, Enrico, Viganò, Mariele, Parazzi, Valentina, Montemurro, Tiziana, Montelatici, Elisa, Lavazza, Cristiana, Budelli, Silvia, Vecchini, Alba, Rebulla, Paolo, Giordano, Rosaria, and Lazzari, Lorenza

Subjects

*ADIPOGENESIS, *MESENCHYMAL stem cells, *CELL populations, *REGENERATIVE medicine, *BONE marrow, *AMNIOTIC liquid

Abstract

Highlights: [•] Human MSCs are promising cell populations for regenerative medicine. [•] Stem cell from different sources display different adipogenic potential. [•] Activation of the PPARγ pathway is crucial for adipogenesis. [•] ADMSC are a valid alternative to immortalized lines for adipogenesis related studies. [Copyright &y& Elsevier]

Published

2013

7. Terutroban, a thromboxane/prostaglandin endoperoxide receptor antagonist, prevents hypertensive vascular hypertrophy and fibrosis.

Author

Gelosa, Paolo, Sevin, Gulnur, Pignieri, Alice, Budelli, Silvia, Catiglioni, Laura, Blanc-Guillemaud, Vanessa, Lerond, Laurence, Tremoli, Elena, and Sironi, Luigi

Subjects

*THROMBOXANES, *PROSTAGLANDINS, *HYPERTENSION, *FIBROSIS, *CELL proliferation, *HEAT shock proteins, *LABORATORY rats

Abstract

Thromboxane A2 and other eicosanoids such as isoprostanes contribute to vascular proliferation and atherosclerosis by binding to the thromboxane/prostaglandin endoperoxide receptors. The effects of terutroban, a thromboxane/prostaglandin endoperoxide receptor antagonist, on aorta remodeling were evaluated in spontaneously hypertensive stroke-prone rats (SHRSPs), a model of severe hypertension, endothelial dysfunction, vascular inflammation, and cerebrovascular diseases. Male SHRSPs were allocated to three groups receiving a standard diet (n = 5) or a high-sodium permissive diet plus vehicle (n = 6) or plus terutroban (30 mg·kg-1·day-1; n = 6). After 6 wk of dietary treatment, all of the animals were injected with bromodeoxyuridine and simultaneously euthanized for aorta collection. The aortic media thickness-to-lumen ratio significantly (P < 0.0001) increased in the salt-loaded rats compared with the rats fed a standard diet, whereas terutroban treatment completely prevented media thickening (P < 0.001). When compared with vehicle, terutroban was also effective in preventing cell proliferation in the media, as indicated by the reduced number of bromodeoxyuridine-positive (P < 0.0001) and proliferating cell nuclear antigen-positive cells (P < 0.0001). Severe fibrosis characterized by a significant accumulation of collagen and fibronectin in the vascular wall was observed in the vehicle-treated rats (P < 0.01) but was completely prevented by terutroban (P < 0.001). The latter also inhibited heat shock protein-47 (P < 0.01) and TGF-1β expression (P < 0.001), which were significantly increased by the high-salt diet. In conclusion, terutroban prevents the development of aorta hyperplasia and has beneficial effects on fibrotic processes by affecting TGF-β and heat shock protein-47 expression in SHRSPs. These findings provide mechanistic data supporting the beneficial effects of terutroban in preventing or retarding atherogenesis. [ABSTRACT FROM AUTHOR]

Published

2011

8. Regulatory T cells from patients with end-stage organ disease can be isolated, expanded and cryopreserved according good manufacturing practice improving their function.

Author

Ulbar, Francesca, Montemurro, Tiziana, Jofra, Tatiana, Capri, Miriam, Comai, Giorgia, Bertuzzo, Valentina, Lavazza, Cristiana, Mandelli, Alessandra, Viganò, Mariele, Budelli, Silvia, Bacalini, Maria Giulia, Pirazzini, Chiara, Garagnani, Paolo, Giudice, Valeria, Sollazzo, Daria, Curti, Antonio, Arpinati, Mario, La Manna, Gaetano, Cescon, Matteo, and Pinna, Antonio Daniele

Subjects

*CRYOPRESERVATION of organs, tissues, etc., *T cells, *CURRENT good manufacturing practices, *FROZEN semen, *CYTOTOXIC T cells

Abstract

Background: Here, we isolated, expanded and functionally characterized regulatory T cells (Tregs) from patients with end stage kidney and liver disease, waiting for kidney/liver transplantation (KT/LT), with the aim to establish a suitable method to obtain large numbers of immunomodulatory cells for adoptive immunotherapy post-transplantation.Methods: We first established a preclinical protocol for expansion/isolation of Tregs from peripheral blood of LT/KT patients. We then scaled up and optimized such protocol according to good manufacturing practice (GMP) to obtain high numbers of purified Tregs which were phenotypically and functionally characterized in vitro and in vivo in a xenogeneic acute graft-versus-host disease (aGVHD) mouse model. Specifically, immunodepressed mice (NOD-SCID-gamma KO mice) received human effector T cells with or without GMP-produced Tregs to prevent the onset of xenogeneic GVHD.Results: Our small scale Treg isolation/expansion protocol generated functional Tregs. Interestingly, cryopreservation/thawing did not impair phenotype/function and DNA methylation pattern of FOXP3 gene of the expanded Tregs. Fully functional Tregs were also isolated/expanded from KT and LT patients according to GMP. In the mouse model, GMP Tregs from LT or KT patient proved to be safe and show a trend toward reduced lethality of acute GVHD.Conclusions: These data demonstrate that expanded/thawed GMP-Tregs from patients with end-stage organ disease are fully functional in vitro. Moreover, their infusion is safe and results in a trend toward reduced lethality of acute GVHD in vivo, further supporting Tregs-based adoptive immunotherapy in solid organ transplantation. [ABSTRACT FROM AUTHOR]

Published

2019