Your search keyword '"Falzetti, Franca"' showing total 9 results

1. Immunoselection and clinical use of T regulatory cells in HLA-haploidentical stem cell transplantation.

Author

Di Ianni, Mauro, Falzetti, Franca, Carotti, Alessandra, Terenzi, Adelmo, Del Papa, Beatrice, Perruccio, Katia, Ruggeri, Loredana, Sportoletti, Paolo, Rosati, Emanuela, Marconi, Pierfrancesco, Falini, Brunangelo, Reisner, Yair, Velardi, Andrea, Aversa, Franco, and Martelli, Massimo F.

Subjects

T cells, HLA histocompatibility antigens, HEMATOPOIETIC stem cells, STEM cell transplantation, IMMUNOREGULATION, CELLULAR immunity, GRAFT versus host disease, PATIENTS

Abstract

Introduction: Haploidentical transplantation, with extensive T cell depletion to prevent GvHD, is associated with a high incidence of infection-related deaths. The key challenge is to improve immune recovery with allogeneic donor T cells without triggering GvHD. As T regulatory cells (Tregs) controlled GvHD in pre-clinical studies, the present study evaluated the impact of an infusion of donor CD4/CD25 + Tregs, followed by an inoculum of donor mature T cells (Tcons) and positively immunoselected CD34 + cells in the setting of haploidentical stem cell transplantation. Patients and methods: Twenty-eight patients were enrolled in this study (22 AML; 5 ALL; 1 NHL). All received immunoselected Tregs (CliniMACS, Miltenyi Biotec) followed by positively immunoselected CD34 + cells together with Tcons 4 days later. No GvHD prophylaxis was administered. Results: 26/28 patients engrafted. No acute GvHD developed in 24/26 patients; 2 developed ≥ grade II acute GvHD. No patient has developed chronic GvHD. CD4 and CD8 counts rapidly increased after transplant. Episodes of CMV reactivation were significantly fewer than in controls. Conclusions: In the setting of haploidentical transplantation infusion of Tregs makes administration of a high dose of T cells feasible. This strategy provides a long-term protection from GvHD and robust immune reconstitution. [Copyright &y& Elsevier]

Published

2011

2. Activated autologous T cells exert an anti-B-cell chronic lymphatic leukemia effect in vitro and in vivo.

Author

Di Ianni, Mauro, Moretti, Lorenzo, Terenzi, Adelmo, Bazzucchi, Federico, Del Papa, Beatrice, Bazzucchi, Moira, Ciurnelli, Raffaella, Lucchesi, Alessandro, Sportoletti, Paolo, Rosati, Emanuela, Marconi, Pier Francesco, Falzetti, Franca, and Tabilio, Antonio

Subjects

CHRONIC lymphocytic leukemia, T cells, B cells, IMMUNE system, CANCER cells, CELL lines, CELL differentiation

Abstract

Background aims The impact of chronic lymphatic leukemia (CLL) tumor burden on the autologous immune system has already been demonstrated. This study attempted to elucidate the molecular mechanisms underlying T-cell immunologic deficiencies in CLL. Methods Freshly isolated CD3+ T cells from patients with a diagnosis of CLL and healthy donors were analyzed by gene expression profiling. Activated T cells from 20 patients with CLL were tested in vitro for cytotoxicity against mutated and unmutated autologous B cells and DAUDI, K562 and P815 cell lines. To investigate T-cell mediated cytotoxicity in vivo, we co-transplanted OKT3-activated T lymphocytes and autologous B-cell CLL (B-CLL) cells into NOD/SCID mice. Results Gene expression profiles of peripheral blood T cells from B-CLL patients showed 25 down-regulated, and 31 up-regulated, genes that were mainly involved in cell differentiation, proliferation, survival, apoptosis, cytoskeleton formation, vesicle trafficking and T-cell activation. After culture, the T-cell count remained unchanged, CD8 cells expanded more than CD4 and a cytotoxicity index >30% was present in 5/20 patients. Cytotoxicity against B autologous leukemic cells did not correlate with B-cell mutational status. Only activated T cells exerting cytotoxicity against autologous leukemic B cells prevented CLL in a human-mouse chimera. Conclusions This study indicates that patients with CLL are affected by a partial immunologic defect that might be somewhat susceptible to repair. This study identifies the molecular pathways underlying T-cell deficiencies in CLL and shows that cytotoxic T-cell functions against autologous B-CLL can be rebuilt at least in part in vitro and in vivo. [ABSTRACT FROM AUTHOR]

Published

2009

3. Homing and survival of thymidine kinase-transduced human T cells in NOD/SCID mice.

Author

Di Ianni, Mauro, Terenzi, Adelmo, Falzetti, Franca, Bartoli, Andrea, Di Florio, Sabrina, Benedetti, Roberta, Venditti, Gigliola, Alfonsi, Diego, De Ioanni, Mariangela, Falini, Brunangelo, and Tabilio, Antonio

Subjects

THYMIDINE, T cells

Abstract

The herpes simplex virus thymidine kinase (HSV-tk) gene conferring ganciclovir (GCV)-specific sensitivity to transduced cells might control Graft-versus-Leukemia (GvL)/Graft-versus-Host Disease (GvHD). Human T lymphocytes were engineered with an LSN-tk retroviral vector encoding tk and neomycin resistance (NeoR) genes. A total of 80×106 tk+ lymphocytes were injected intraperitoneally in NOD-SCID mice. Engraftment was evaluated by human CD45+/CD3+ cytofluorimetric analysis and NeoR-based polymerase chain reaction (PCR) on peripheral blood, bone marrow, liver, thymus, and spleen on day +5. After 14 days, GCV (10 mg/kg daily) cytofluorimetric analysis and PCR were repeated (day +19). Immunohistological studies with anti-CD3 monoclonal antibody followed by alkaline phosphatase and monoclonal anti–alkaline phosphatase staining were performed on spleen and liver at the same time points. Human CD45+/CD3+ cells were engrafted in all tissues on day +5 according to cytofluorimetry, immunohistology, and PCR. Lymphocytes “homed” to the white pulp T-cell area and to the red pulp; liver localization is prevalently at the periportal area. After GCV (day +19), cytofluorimetry and immunohistology showed very few CD3+ cells. PCR identified the transgene in 22% tissue samples (positive only in thymus and spleen). GvHD did not occur in any animal. These data demonstrate elevated doses of human-transduced CD3+ cells engraft in NOD/SCID mice; after GCV, very few CD3+ cells can be detected and those that escape treatment can be found in the thymus and in the spleen on day +19. Lack of full response to GCV may account for cases of GvHD in patients receiving tk-transduced T lymphocytes. Cancer Gene Therapy (2002) 9, 756–761 doi:10.1038/sj.cgt.7700495 [ABSTRACT FROM AUTHOR]

Published

2002

4. Clinical-Grade–Expanded Regulatory T Cells Prevent Graft-versus-Host Disease While Allowing a Powerful T Cell–Dependent Graft-versus-Leukemia Effect in Murine Models.

Author

Del Papa, Beatrice, Ruggeri, Loredana, Urbani, Elena, Cecchini, Debora, Zei, Tiziana, Iacucci Ostini, Roberta, Crescenzi, Barbara, Carotti, Alessandra, Pierini, Antonio, Sportoletti, Paolo, Falzetti, Franca, Mecucci, Cristina, Velardi, Andrea, Martelli, Massimo F., Baldoni, Stefano, Di Bartolomeo, Paolo, and Di Ianni, Mauro

Subjects

*T cells, *GRAFT versus host disease prevention, *REGULATOR genes, *LEUKEMIA treatment, *CD antigens, *CLINICAL trials, *THERAPEUTICS

Abstract

We developed a good manufacturing practices–compatible expansion protocol to improve number and purity of regulatory T cells (Tregs) available for clinical trials. Six clinical-grade separation procedures were performed, followed by expansion with high-dose interleukin (IL)-2, anti-CD3/anti-CD28 TCR stimulation, and rapamycin for 19 days achieving a median of 8.5-fold (range, 6.25 to 13.7) expansion. FOXP3 expression was stably maintained over the culture period, while the percentage of CD127 was significantly reduced. The in vitro suppression assay showed a strong Mixed Lymphocytes Reaction inhibition. In vitro amplification did not induce any karyotypic modification. To evaluate the graft-versus-host disease (GVHD)/graft-versus-leukemia (GVL) bifunctional axis, expanded Tregs and conventional T cells (Tcons) were tested in NOD/SCID/IL2Rgnull mice injected with primary acute myeloid leukemia (AML) cells, AML cell line, acute lymphoid leukemia Philadelphia cell line, or Burkitt-like lymphoma cell line. All mice that received leukemia cells together with expanded Tregs and Tcons were rescued from leukemia and survived without GVHD, showing that Treg expansion procedure did not compromise GVHD control and the strong Tcon-mediated GVL activity. This report might represent the basis for treating high-risk leukemia and/or relapsed/refractory leukemia patients with high-dose Treg/Tcons. [ABSTRACT FROM AUTHOR]

Published

2017

5. The Total Body Irradiation Schedule Affects Acute Leukemia Relapse After Matched T Cell-Depleted Hematopoietic Stem Cell Transplantation.

Author

Aristei, Cynthia, Carotti, Alessandra, Palazzari, Elisa, Amico, Lucia, Ruggeri, Loredana, Perrucci, Elisabetta, Falcinelli, Lorenzo, Lancellotta, Valentina, Palumbo, Isabella, Falzetti, Franca, Aversa, Franco, Merluzzi, Mara, Velardi, Andrea, and Martelli, Massimo Fabrizio

Subjects

*HEMATOPOIETIC stem cell transplantation, *TOTAL body irradiation, *ACUTE myeloid leukemia treatment, *AGE differences, *MULTIVARIATE analysis, *GRAFT versus host disease prevention, *LYMPHOBLASTIC leukemia treatment, *SIBLINGS, *CAUSES of death, *HISTOCOMPATIBILITY, *IMMUNOSUPPRESSION, *LYMPHOBLASTIC leukemia, *PROGNOSIS, *RADIATION doses, *RADIOTHERAPY, *T cells, *TIME, *DISEASE relapse, *ACUTE myeloid leukemia, *TREATMENT effectiveness, *DISEASE remission, DISEASE relapse prevention

Abstract

Purpose: We sought to determine whether the total body irradiation (TBI) schedule affected outcome in patients with acute leukemia in complete remission who received T cell-depleted allogeneic hematopoietic stem cell transplantation from HLA identical siblings.Methods and Materials: The study recruited 55 patients (median age, 48 years; age range, 20-66 years; 30 men and 25 women; 34 with acute myeloid leukemia and 21 with acute lymphoid leukemia). Hyperfractionated TBI (HTBI) (1.2 Gy thrice daily for 4 days [for a total dose of 14.4 Gy] from day -12 to day -9) was administered to 29 patients. Single-dose TBI (STBI) (8 Gy, at a median dose rate of 10.7 cGy/min on day -9) was given to 26 patients.Results: All patients achieved primary, sustained engraftment with full donor-type chimerism. At 10 years, the overall cumulative incidence of transplant-related mortality was 11% (SE, ±0.1%). It was 7% (SE, ±0.2%) after HTBI and 15% (SE, ±0.5%) after STBI (P=.3). The overall cumulative incidence of relapse was 33% (SE, ±0.5). It was 13% (SE, ±0.5%) after HTBI and 46% (SE, ±1%) after STBI (P=.02). The overall probability of disease-free survival (DFS) was 59% (SE, ±7%). It was 67% (SE, ±0.84%) after HTBI and 37% (SE, ±1.4%) after STBI (P=.01). Multivariate analyses showed the TBI schedule was the only risk factor that significantly affected relapse and DFS (P=.01 and P=.03, respectively).Conclusions: In patients with acute leukemia, HTBI is more efficacious than STBI in eradicating minimal residual disease after HLA-matched T cell-depleted hematopoietic stem cell transplantation, thus affecting DFS. [ABSTRACT FROM AUTHOR]

Published

2016

6. HLA-haploidentical transplantation with regulatory and conventional T-cell adoptive immunotherapy prevents acute leukemia relapse.

Author

Martelli, Massimo F., Di lanni, Mauro, Ruggeri, Loredana, Falzetti, Franca, Carotti, Alessandra, Terenzi, Adelmo, Pierini, Antonio, Massei, Maria Speranza, Amico, Lucia, Urbani, Elena, Del Papa, Beatrice, Zei, Tiziana, Ostini, Roberta Iacucci, Cecchini, Debora, Tognellini, Rita, Reisner, Yair, Aversa, Franco, Falini, Brunangelo, and Velardi, Andrea

Subjects

*HLA histocompatibility antigens, *IMMUNOTHERAPY, *T cells, *GRAFT versus host disease, *CELL transplantation, *STEM cells, DISEASE relapse prevention

Abstract

Posttransplant relapse is still the major cause of treatment failure in high-risk acute leukemia. Attempts to manipulate alloreactive T cells to spare normal cells while killing leukemic cells have been unsuccessful. In HLA-haploidentical transplantation, we reported that donor-derived T regulatory cells (Tregs), coinfused with conventional T cells (Tcons), protected recipients against graft-versus-host disease (GVHD). The present phase 2 study investigated whether Treg-Tcon adoptive immunotherapy prevents posttransplant leukemia relapse. Forty-three adults with high-risk acute leukemia (acute myeloid leukemia 33; acute lymphoblastic leukemia 10) were conditioned with a total body irradiation-based regimen. Grafts included CD34+ cells (mean 9.7 × 106/kg), Tregs (mean 2.5 × 106/kg), and Tcons (mean 1.1 × 106/kg). No posttransplant immunosuppression was given. Ninety-five percent of patients achieved full-donor type engraftment and 15% developed sgrade 2 acute GVHD. The probability of disease-free survival was 0.56 at a median follow-up of 46 months. The very low cumulative incidence of relapse (0.05) was significantly better than in historical controls. These results demonstrate the immunosuppressive potential of Tregs can be used to suppress GVHD without loss of the benefits of graft-versus-leukemia (GVL) activity. Humanized murine models provided insights into the mechanisms underlying separation of GVL from GVHD, suggesting the GVL effect is due to largely unopposed Tcon alloantigen recognition in bone marrow. [ABSTRACT FROM AUTHOR]

Published

2014

7. "Designed" grafts for HLA-haploidentical stem cell transplantation.

Author

Martelli, Massimo F., Di Ianni, Mauro, Ruggeri, Loredana, Pierini, Antonio, Falzetti, Franca, Carotti, Alessandra, Terenzi, Adelmo, Reisner, Yair, Aversa, Franco, Falini, Brunangelo, and Velardi, Andrea

Subjects

*HLA histocompatibility antigens, *STEM cell transplantation, *T cells, *IMMUNOTHERAPY, *LEUKEMIA

Abstract

Today human leukocyte antigen-haploidentical transplantation is a feasible option for patients with high-risk acute leukemia who do not have matched donors. Whether it is T-cell replete or T-cell depleted, it is still, however, associated with issues of transplant-related mortality and posttrans-plant leukemia relapse. After reports that adoptive immunotherapy with T-regulatory cells controls the alloreactivity of conventional T lymphocytes in animal models, tomorrow's world of haploidentical transplantation will focus on new "designed" grafts. They will contain an appropriate ratio of conventional T lymphocytes and T-regulatory cells, natural killer cells, γ δ T cells, and other accessory cells. Preliminary results of ongoing clinical trials show the approach is feasible. It is associated with better immune reconstitution and a quite powerful graft-versus-leukemia effect with a low incidence of graft-versus-host disease and no need for posttransplant pharmacological prophylaxis. Future strategies will focus on enhancing the clinical benefit of T-regulatory cells by increasing their number and strengthening their function. [ABSTRACT FROM AUTHOR]

Published

2014

8. T regulatory cell separation for clinical application

Author

Di Ianni, Mauro, Del Papa, Beatrice, Zei, Tiziana, Iacucci Ostini, Roberta, Cecchini, Debora, Cantelmi, Maria Grazia, Baldoni, Stefano, Sportoletti, Paolo, Cavalli, Laura, Carotti, Alessandra, Pierini, Antonio, Falini, Brunangelo, Martelli, Massimo F., and Falzetti, Franca

Subjects

*T cells, *CELL separation, *LEUKAPHERESIS, *CD8 antigen, *BIOLOGICAL assay, *HEMATOPOIETIC stem cell transplantation, *GRAFT versus host disease

Abstract

Abstract: We selected T regulatory cells (Tregs) from standard leukapheresis using double-negative selection (anti-CD8 and anti-CD19) followed by positive selection (anti-CD25) and 72 procedures were performed. A median of 263×106 cells (range 143–470×106) were recovered with a mean of CD4+/CD25+ cells of 94.5±2.4% (36.5±18.6% CD4+/CD25+hi). FoxP3+ cells were equal to 79.8%±22.2. CD127+ cells were 12.5%±8.2. The inhibition assay showed an inhibition rate of 67±22. Cells isolated by means of this approach can be used in allogeneic hematopoietic stem cell transplantation to reduce the incidence and severity of GvHD without bystander inhibition of general immunity. [Copyright &y& Elsevier]

Published

2012

9. Interleukin-7–Engineered Mesenchymal Cells: In Vitro Effects on Naive T-Cell Population

Author

Sportoletti, Paolo, Del Papa, Beatrice, De Ioanni, Mariangela, Moretti, Lorenzo, Bonifacio, Elisabetta, Lanterna, Vania, Bell, Alain, Fettucciari, Katia, Carnevali, Eugenia, Zei, Tiziana, Falzetti, Franca, Martelli, Massimo F., Tabilio, Antonio, and Di Ianni, Mauro

Subjects

*CELL proliferation, *T cells, *LYMPHOCYTES, *PHYSIOLOGICAL control systems

Abstract

Abstract: T-cell homeostasis is regulated by several molecules; among these, interleukin (IL)-7 plays an essential role in the survival and homeostatic proliferation of peripheral naive T cells. In a previous study, we investigated whether human mesenchymal stromal cells (MSCs) could be engineered with the IL-7 gene to produce functional level of this cytokine. In the present study, we analyzed the impact of different quantities of IL-7 produced by MSCs on the survival and proliferation of a negative immunoselected naive (CD3+/CD45RA+) T-cell population. Co-cultivation of peripheral naive T cells with MSCs producing low (16 pg/mL) or high (1000 pg/mL) IL-7 levels or in the presence of exogenous IL-7 (0.01 ng/mL and 100 ng/mL) maintained the CD3+/CD45RA+ naive T-cell phenotype. Chemokine receptor CCR7+ expression was also maintained among this T-cell population. Naive T-cell molecular characteristics were maintained as assessed by the Vβ spectratyping complexity score, which showed the maintenance of a broad T-cell repertoire. No Th1 or Th2 differentiation was observed, as assessed by interferon-γ or IL-4 accumulation. In contrast, only MSCs producing high amounts of IL-7 caused increased activation (CD25 31.2% ± 12% vs 10% ± 3.5%; P < .05), proliferation (CD71 17.8±7% vs 9.3%±3, P < .05), apoptosis (assessed by annexin V: 18.6% ± 5% vs 14.9% ± 2.6%; P > .05), and the phase S cell cycle (15% vs 6.9%, P > .05). Exogenous IL-7 exhibited no significant effect. In conclusion, we demonstrated that IL-7 produced by MSCs has a dose-independent effect on naive T-cell survival while exerting a dose-dependent effect on activation/proliferation. Due to the continuous production of IL-7 by engineered cells, our system is more efficacious than exogenous IL-7. [Copyright &y& Elsevier]

Published

2006