Your search keyword '"Del Bufalo, F"' showing total 157 results

1. Chimeric Antigen Receptor (CAR) T-Cell Products for Pediatric Cancers: Why Alternative Development Paths Are Needed

Author

Rossig, C, Pearson, A, Vassal, G, Scobie, N, Bird, N, Blanc, P, Vormoor, H, Calkoen, F, Locatelli, F, del Bufalo, F, Rives, S, Jacoby, E, Balduzzi, A, Bourquin, J, Baruchel, A, Rossig C., Pearson A. D., Vassal G., Scobie N., Bird N., Blanc P., Vormoor H. J., Calkoen F. G., Locatelli F., del Bufalo F., Rives S., Jacoby E., Balduzzi A., Bourquin J. P., Baruchel A., Rossig, C, Pearson, A, Vassal, G, Scobie, N, Bird, N, Blanc, P, Vormoor, H, Calkoen, F, Locatelli, F, del Bufalo, F, Rives, S, Jacoby, E, Balduzzi, A, Bourquin, J, Baruchel, A, Rossig C., Pearson A. D., Vassal G., Scobie N., Bird N., Blanc P., Vormoor H. J., Calkoen F. G., Locatelli F., del Bufalo F., Rives S., Jacoby E., Balduzzi A., Bourquin J. P., and Baruchel A.

Published

2024

2. GD2-CART01 for Relapsed or Refractory High-Risk Neuroblastoma

Author

Del Bufalo, F., De Angelis, B., Caruana, I., Del Baldo, G., De Ioris, M. A., Serra, A., Mastronuzzi, A., Cefalo, M. G., Pagliara, D., Amicucci, M., Li Pira, G., Leone, G., Bertaina, V., Sinibaldi, M., Di Cecca, S., Guercio, M., Abbaszadeh, Z., Iaffaldano, L., Gunetti, M., Iacovelli, S., Bugianesi, R., Macchia, S., Algeri, M., Merli, P., Galaverna, F., Abbas, R., Garganese, M. C., Villani, M. F., Colafati, G. S., Bonetti, F., Rabusin, M., Perruccio, K., Folsi, V., Quintarelli, C., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Del Bufalo, F., De Angelis, B., Caruana, I., Del Baldo, G., De Ioris, M. A., Serra, A., Mastronuzzi, A., Cefalo, M. G., Pagliara, D., Amicucci, M., Li Pira, G., Leone, G., Bertaina, V., Sinibaldi, M., Di Cecca, S., Guercio, M., Abbaszadeh, Z., Iaffaldano, L., Gunetti, M., Iacovelli, S., Bugianesi, R., Macchia, S., Algeri, M., Merli, P., Galaverna, F., Abbas, R., Garganese, M. C., Villani, M. F., Colafati, G. S., Bonetti, F., Rabusin, M., Perruccio, K., Folsi, V., Quintarelli, C., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Background: Immunotherapy with chimeric antigen receptor (CAR)-expressing T cells that target the disialoganglioside GD2 expressed on tumor cells may be a therapeutic option for patients with high-risk neuroblastoma. Methods: In an academic, phase 1-2 clinical trial, we enrolled patients (1 to 25 years of age) with relapsed or refractory, high-risk neuroblastoma in order to test autologous, third-generation GD2-CAR T cells expressing the inducible caspase 9 suicide gene (GD2-CART01). Results: A total of 27 children with heavily pretreated neuroblastoma (12 with refractory disease, 14 with relapsed disease, and 1 with a complete response at the end of first-line therapy) were enrolled and received GD2-CART01. No failure to generate GD2-CART01 was observed. Three dose levels were tested (3-, 6-, and 10×106 CAR-positive T cells per kilogram of body weight) in the phase 1 portion of the trial, and no dose-limiting toxic effects were recorded; the recommended dose for the phase 2 portion of the trial was 10×106 CAR-positive T cells per kilogram. Cytokine release syndrome occurred in 20 of 27 patients (74%) and was mild in 19 of 20 (95%). In 1 patient, the suicide gene was activated, with rapid elimination of GD2-CART01. GD2-targeted CAR T cells expanded in vivo and were detectable in peripheral blood in 26 of 27 patients up to 30 months after infusion (median persistence, 3 months; range, 1 to 30). Seventeen children had a response to the treatment (overall response, 63%); 9 patients had a complete response, and 8 had a partial response. Among the patients who received the recommended dose, the 3-year overall survival and event-free survival were 60% and 36%, respectively. Conclusions: The use of GD2-CART01 was feasible and safe in treating high-risk neuroblastoma. Treatment-related toxic effects developed, and the activation of the suicide gene controlled side effects. GD2-CART01 may have a sustained antitumor effect. (Funded by the Italian Medicines Agency and others

Published

2023

3. Human leukocyte antigen evolutionary divergence influences outcomes of paediatric patients and young adults affected by malignant disorders given allogeneic haematopoietic stem cell transplantation from unrelated donors

Author

Merli, P., Crivello, P., Strocchio, L., Pinto, R. M., Algeri, M., Del Bufalo, F., Pagliara, D., Becilli, M., Carta, R., Gaspari, S., Galaverna, F., Quagliarella, F., Boz, G., Catanoso, M. L., Boccieri, E., Troiano, M., Fleischhauer, K., Andreani, M., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Merli, P., Crivello, P., Strocchio, L., Pinto, R. M., Algeri, M., Del Bufalo, F., Pagliara, D., Becilli, M., Carta, R., Gaspari, S., Galaverna, F., Quagliarella, F., Boz, G., Catanoso, M. L., Boccieri, E., Troiano, M., Fleischhauer, K., Andreani, M., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

High genetic heterogeneity in the human leukocyte antigen (HLA) increases the likelihood of efficient immune response to pathogens and tumours. As measure of HLA diversity, HLA evolutionary divergence (HED) has been shown to predict the response of tumours to immunotherapy and haematopoietic stem cell transplantation (HSCT) in adults. We retrospectively investigated the association of HED with outcomes of 153 paediatric/young adults patients, treated for malignant disorders with HSCT from 9–10/10 HLA-matched unrelated donors. HED was calculated as pairwise genetic distance between alleles in patient HLA-A, -B, -C, -DRB1, -DQB1 and -DPB1, using the locus median to stratify patients with ‘high’ or ‘low’ HED. Patients with high HED-B and -DRB1 showed significantly improved disease-free survival (DFS), especially when combined (70.8% vs 53.7% p = 0.008). High HED-B + -DRB1 was also associated with improved overall survival (OS) (82.1 vs 66.4% p = 0.014), and concomitant reduction of non-relapse-mortality (5.1% vs 21.1% p = 0.006). The impact on OS and DFS of combined HED-B + -DRB1 was confirmed in multivariate analysis [hazard ratio (HR) 0.39, p = 0.009; and HR 0.45, p = 0.007 respectively]. Only high HED scores for HLA-DPB1 were associated, in univariate analysis, with reduced incidence of relapse (15.9% vs 31.1%, p = 0.03). These results support HED as prognostic marker in allogeneic HSCT and, if confirmed in larger cohorts, would allow its use to inform clinical risk and potentially influence clinical practice.

Published

2023

4. Allogeneic, donor-derived, second-generation, CD19-directed CAR-T cells for the treatment of pediatric relapsed/refractory BCP-ALL

Author

del Bufalo, F., Becilli, M., Rosignoli, C., De Angelis, B., Algeri, M., Hanssens, L., Gunetti, M., Iacovelli, S., Li Pira, G., Girolami, E., Leone, G., Lazzaro, S., Bertaina, V., Sinibaldi, M., Di Cecca, S., Iaffaldano, L., Kunkele, A., Boccieri, E., Del Baldo, G., Pagliara, D., Merli, P., Carta, R., Quintarelli, C., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), del Bufalo, F., Becilli, M., Rosignoli, C., De Angelis, B., Algeri, M., Hanssens, L., Gunetti, M., Iacovelli, S., Li Pira, G., Girolami, E., Leone, G., Lazzaro, S., Bertaina, V., Sinibaldi, M., Di Cecca, S., Iaffaldano, L., Kunkele, A., Boccieri, E., Del Baldo, G., Pagliara, D., Merli, P., Carta, R., Quintarelli, C., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Autologous CD19-directed chimeric antigen receptor (CAR)-T cells have shown unprecedented efficacy in children with relapsed/refractory B-cell precursor acute lymphoblastic leukemia (BCP-ALL). However, patients either relapsing after allogeneic hematopoietic stem cell transplantation (allo-HSCT) or displaying profound lymphopenia and/or rapidly progressing disease often cannot access autologous products. These hurdles may be overcome by allogeneic, donor-derived CAR-T cells. We tested donor-derived T cells transduced with a second-generation (4.1BB) CD19-directed CAR for treatment of patients with BCP-ALL in a hospital-exemption setting. Two constructs were tested: a retroviral construct incorporating the suicide gene inducible caspase-9 (CD19-CAR–Retro_ALLO) first and then a lentiviral construct and an automated, Prodigy-based manufacturing process (CD19-CAR–Lenti_ALLO). Thirteen children/young adults received ALLO–CAR-T cells between March 2021 and October 2022. Doses ranged between 1.0 × 106 and 3.0 × 106 CAR-T cells per kg. The toxicity profile was comparable with that of autologous CAR-T cells, characterized mainly by cytopenia, cytokine release syndrome (maximum grade 1), and grade 2 immune-effector cell–associated neurotoxicity syndrome. One case of acute graft-versus-host disease (GVHD) occurred and was rapidly controlled with steroids and ruxolitinib. None of the other patients, including 3 given ALLO–CAR-T cells from an HLA-haploidentical donor, experienced GVHD. Two patients received ALLO–CAR-T cells before HSCT and showed a significant expansion of CAR-T cells without any sign of GVHD. All patients obtained complete remission (CR) with absence of minimal residual disease in the bone marrow. With a median follow-up of 12 months (range, 5-21), 8 of 13 patients maintained CR. Allogeneic anti-CD19 CAR-T cells can effectively treat highly refractory BCP-ALL relapsing after allo-HSCT without showing increased toxicity as compared with autologous CAR-T cells.

Published

2023

5. GD2-CART01 for Relapsed or Refractory High-Risk Neuroblastoma. Reply

Author

Quintarelli, C., Del Bufalo, F., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Quintarelli, C., Del Bufalo, F., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

To the Editor: Del Bufalo et al. (April 6 issue)(1) describe the treatment of patients with relapsed or refractory pediatric neuroblastoma with chimeric antigen receptor (CAR)-expressing T cells that target the disialoganglioside GD2 and express the inducible capsase 9 suicide gene (GD2-CART01). Among the children who had a relapse after this treatment, the authors did not observe reexpansion of T cells, and the GD2 antigen was still expressed on tumor cells. We were surprised by the surface-marker analysis of the GD2-CAR T cells that led the authors to conclude that these cells were not exhausted. The data show that the . . .

Published

2023

6. Strategy to prevent epitope masking in CAR.CD19+ B-cell leukemia blasts

Author

Quintarelli, C, Guercio, M, Manni, S, Boffa, I, Sinibaldi, M, DI Cecca, S, Caruso, S, Abbaszadeh, Z, Camera, A, Cembrola, B, Ciccone, R, Orfao, A, Martin-Martin, L, Gutierrez-Herrero, S, Herrero-Garcia, M, Cazzaniga, G, Nunes, V, Songia, S, Marcatili, P, Marin, F, Ruella, M, Bertaina, V, Vinti, L, Del Bufalo, F, Algeri, M, Merli, P, De Angelis, B, Locatelli, F, Quintarelli C., Guercio M., Manni S., Boffa I., Sinibaldi M., DI Cecca S., Caruso S., Abbaszadeh Z., Camera A., Cembrola B., Ciccone R., Orfao A., Martin-Martin L., Gutierrez-Herrero S., Herrero-Garcia M., Cazzaniga G., Nunes V., Songia S., Marcatili P., Marin F. I., Ruella M., Bertaina V., Vinti L., Del Bufalo F., Algeri M., Merli P., De Angelis B., Locatelli F., Quintarelli, C, Guercio, M, Manni, S, Boffa, I, Sinibaldi, M, DI Cecca, S, Caruso, S, Abbaszadeh, Z, Camera, A, Cembrola, B, Ciccone, R, Orfao, A, Martin-Martin, L, Gutierrez-Herrero, S, Herrero-Garcia, M, Cazzaniga, G, Nunes, V, Songia, S, Marcatili, P, Marin, F, Ruella, M, Bertaina, V, Vinti, L, Del Bufalo, F, Algeri, M, Merli, P, De Angelis, B, Locatelli, F, Quintarelli C., Guercio M., Manni S., Boffa I., Sinibaldi M., DI Cecca S., Caruso S., Abbaszadeh Z., Camera A., Cembrola B., Ciccone R., Orfao A., Martin-Martin L., Gutierrez-Herrero S., Herrero-Garcia M., Cazzaniga G., Nunes V., Songia S., Marcatili P., Marin F. I., Ruella M., Bertaina V., Vinti L., Del Bufalo F., Algeri M., Merli P., De Angelis B., and Locatelli F.

Abstract

Chimeric antigen receptor T-cells (CAR T-cells) for the treatment of relapsing/refractory B-cell precursor acute lymphoblastic leukemia have led to exciting clinical results. However, CAR T-cell approaches revealed a potential risk of CD19-/CAR+ leukemic relapse due to inadvertent transduction of leukemia cells. BackgroundMethods We evaluated the impact of a high percentage of leukemia blast contamination in patient-derived starting material (SM) on CAR T-cell drug product (DP) manufacturing. In vitro as well as in vivo models were employed to identify characteristics of the construct associated with better profile of safety in case of inadvertent B-cell leukemia transduction during CAR T-cell manufacturing. Results The presence of large amounts of CD19+ cells in SM did not affect the transduction level of DPs, as well as the CAR T-cell rate of expansion at the end of standard production of 14 days. DPs were deeply characterized by flow cytometry and molecular biology for Ig-rearrangements, showing that the level of B-cell contamination in DPs did not correlate with the percentage of CD19+ cells in SM, in the studied patient cohort. Moreover, we investigated whether CAR design may affect the control of CAR+ leukemia cells. We provided evidences that CAR.CD19 short linker (SL) prevents complete epitope masking in CD19+CAR+ leukemia cells and we demonstrated in vitro and in vivo that CD19 +CAR(SL)+leukemic cells are killed by CAR.CD19 T-cells. Conclusions Taken together, these data suggest that a VL-VH SL may result in a safe CAR-T product, even when manufacturing starts from biological materials characterized by heavy contamination of leukemia blasts.

Published

2021

7. Brentuximab vedotin in combination with bendamustine in pediatric patients or young adults with relapsed or refractory Hodgkin lymphoma

Author

Vinti, L., Pagliara, D., Buffardi, S., Di Ruscio, V., Stocchi, F., Mariggio, E., Parasole, R., Di Matteo, A., Petruzziello, F., Paganelli, V., De Vito, R., Del Bufalo, F., Strocchio, L., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Vinti, L., Pagliara, D., Buffardi, S., Di Ruscio, V., Stocchi, F., Mariggio, E., Parasole, R., Di Matteo, A., Petruzziello, F., Paganelli, V., De Vito, R., Del Bufalo, F., Strocchio, L., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Although children and young adults with Hodgkin's lymphoma usually have a favorable prognosis, patients with primary refractory disease and some subsets of relapsed patients still have a dismal outcome. Brentuximab vedotin (BV) in combination with bendamustine may represent a suitable salvage therapy; data on 32 patients aged less than 25 years were retrospectively analyzed. Patients received up to six cycles of treatment of BV 1.8 mg/kg on day 1 and bendamustine 90–120 mg/m2 on days 2 and 3. At the end of treatment, the overall response rate was 81%. The 3-year overall and progression-free survivals are 78.1% and 67%, respectively.

Published

2022

8. Fecal microbiota transplantation for the treatment of steroid-refractory, intestinal, graft-versus-host disease in a pediatric patient

Author

Merli, P., Massa, M., Russo, A., Rea, F., Del Chierico, F., Galaverna, F., Del Bufalo, F., Pane, S., Algeri, M., Romeo, E. F., Masucci, Luca, De Angelis, P., Putignani, L., Locatelli, Franco, Masucci L. (ORCID:0000-0002-8358-6726), Locatelli F. (ORCID:0000-0002-7976-3654), Merli, P., Massa, M., Russo, A., Rea, F., Del Chierico, F., Galaverna, F., Del Bufalo, F., Pane, S., Algeri, M., Romeo, E. F., Masucci, Luca, De Angelis, P., Putignani, L., Locatelli, Franco, Masucci L. (ORCID:0000-0002-8358-6726), and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

NO ABSTRACT AVAILABLE

Published

2022

9. TCRab/CD19 depleted HSCT from an HLA-haploidentical relative to treat children with different non malignant disorders

Author

Merli, P., Pagliara, D., Galaverna, F., Pira, G. L., Andreani, M., Leone, G., Amodio, D., Pinto, R. M., Bertaina, A., Bertaina, V., Mastronuzzi, A., Strocchio, L., Boccieri, E., Pende, D., Falco, M., Nardo, M. D., Del Bufalo, F., Algeri, M., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Merli, P., Pagliara, D., Galaverna, F., Pira, G. L., Andreani, M., Leone, G., Amodio, D., Pinto, R. M., Bertaina, A., Bertaina, V., Mastronuzzi, A., Strocchio, L., Boccieri, E., Pende, D., Falco, M., Nardo, M. D., Del Bufalo, F., Algeri, M., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Several nonmalignant disorders (NMDs), either inherited or acquired, can be cured by allogeneic hematopoietic stem cell transplantation (HSCT). Between January 2012 and April 2020, 70 consecutive children affected by primary immunodeficiencies, inherited/acquired bone marrow failure syndromes, red blood cell disorders, or metabolic diseases, lacking a fully matched donor or requiring urgent transplantation underwent TCRab/CD19-depleted haploidentical HSCT from an HLA-partially matched relative as part of a prospective study. The median age at transplant was 3.5 years (range 0.3-16.1); the median time from diagnosis to transplant was 10.5 months (2.7 for SCID patients). Primary engraftment was obtained in 51 patients, while 19 and 2 patients experienced either primary or secondary graft failure (GF), the overall incidence of this complication being 30.4%. Most GFs were observed in children with disease at risk for this complication (eg, aplastic anemia, thalassemia). All but 5 patients experiencing GF were successfully retransplanted. Six patients died of infectious complications (4 had active/ recent infections at the time of HSCT), the cumulative incidence of transplant-related mortality (TRM) being 8.5%. Cumulative incidence of grade 1-2 acute GVHD was 14.4% (no patient developed grade 3-4 acute GVHD). Only one patient at risk developed mild chronic GVHD. With a median follow-up of 3.5 years, the 5-year probability of overall and disease-free survival was 91.4% and 86.8%, respectively. In conclusion, TCRab/CD19-depleted haploidentical HSCT from an HLA-partially matched relative is confirmed to be an effective treatment of children with NMDs. Prompt donor availability, low incidence of GVHD, and TRM make this strategy an attractive option in NMDs patients. The study is registered at ClinicalTrial.gov as NCT01810120.

Published

2022

10. Dual IGF1R/IR inhibitors in combination with GD2-CAR T-cells display a potent anti-tumor activity in diffuse midline glioma H3K27M-mutant

Author

De Billy, E., Pellegrino, M., Orlando, D., Pericoli, G., Ferretti, R., Businaro, P., Ajmone-Cat, M. A., Rossi, S., Petrilli, L. L., Maestro, N., Diomedi-Camassei, F., Pezzullo, M., De Stefanis, C., Bencivenga, P., Palma, A., Rota, R., Del Bufalo, F., Massimi, Luca, Weber, G., Jones, C., Carai, A., Caruso, S., De Angelis, B., Caruana, I., Quintarelli, C., Mastronuzzi, A., Locatelli, Franco, Vinci, M., Massimi L., Locatelli F. (ORCID:0000-0002-7976-3654), De Billy, E., Pellegrino, M., Orlando, D., Pericoli, G., Ferretti, R., Businaro, P., Ajmone-Cat, M. A., Rossi, S., Petrilli, L. L., Maestro, N., Diomedi-Camassei, F., Pezzullo, M., De Stefanis, C., Bencivenga, P., Palma, A., Rota, R., Del Bufalo, F., Massimi, Luca, Weber, G., Jones, C., Carai, A., Caruso, S., De Angelis, B., Caruana, I., Quintarelli, C., Mastronuzzi, A., Locatelli, Franco, Vinci, M., Massimi L., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Background: Diffuse midline gliomas (DMG) H3K27M-mutant, including diffuse intrinsic pontine glioma (DIPG), are pediatric brain tumors associated with grim prognosis. Although GD2-CAR T-cells demonstrated significant anti-tumor activity against DMG H3K27M-mutant in vivo, a multimodal approach may be needed to more effectively treat patients. We investigated GD2 expression in DMG/DIPG and other pediatric high-grade gliomas (pHGG) and sought to identify chemical compounds that would enhance GD2-CAR T-cell anti-tumor efficacy. Methods: Immunohistochemistry in tumor tissue samples and immunofluorescence in primary patient-derived cell lines were performed to study GD2 expression. We developed a high-throughput cell-based assay to screen 42 kinase inhibitors in combination with GD2-CAR T-cells. Cell viability, western blots, flow-cytometry, real time PCR experiments, DIPG 3D culture models, and orthotopic xenograft model were applied to investigate the effect of selected compounds on DIPG cell death and CAR T-cell function. Results: GD2 was heterogeneously, but widely, expressed in the tissue tested, while its expression was homogeneous and restricted to DMG/DIPG H3K27M-mutant cell lines. We identified dual IGF1R/IR antagonists, BMS-754807 and linsitinib, able to inhibit tumor cell viability at concentrations that do not affect CAR T-cells. Linsitinib, but not BMS-754807, decreases activation/exhaustion of GD2-CAR T-cells and increases their central memory profile. The enhanced anti-tumor activity of linsitinib/GD2-CAR T-cell combination was confirmed in DIPG models in vitro, ex vivo, and in vivo. Conclusion: Our study supports the development of IGF1R/IR inhibitors to be used in combination with GD2-CAR T-cells for treating patients affected by DMG/DIPG and, potentially, by pHGG.

Published

2022

11. Epigenetic Profiling and Response to CD19 Chimeric Antigen Receptor T-Cell Therapy in B-Cell Malignancies

Author

Garcia-Prieto, C. A., Villanueva, L., Bueno-Costa, A., Davalos, V., Gonzalez-Navarro, E. A., Juan, M., Urbano-Ispizua, A., Delgado, J., Ortiz-Maldonado, V., Del Bufalo, F., Locatelli, Franco, Quintarelli, C., Sinibaldi, M., Soler, M., Castro De Moura, M., Ferrer, G., Urdinguio, R. G., Fernandez, A. F., Fraga, M. F., Bar, D., Meir, A., Itzhaki, O., Besser, M. J., Avigdor, A., Jacoby, E., Esteller, M., Locatelli F. (ORCID:0000-0002-7976-3654), Garcia-Prieto, C. A., Villanueva, L., Bueno-Costa, A., Davalos, V., Gonzalez-Navarro, E. A., Juan, M., Urbano-Ispizua, A., Delgado, J., Ortiz-Maldonado, V., Del Bufalo, F., Locatelli, Franco, Quintarelli, C., Sinibaldi, M., Soler, M., Castro De Moura, M., Ferrer, G., Urdinguio, R. G., Fernandez, A. F., Fraga, M. F., Bar, D., Meir, A., Itzhaki, O., Besser, M. J., Avigdor, A., Jacoby, E., Esteller, M., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Background: Chimeric antigen receptor (CAR) T cells directed against CD19 (CART19) are effective in B-cell malignancies, but little is known about the molecular factors predicting clinical outcome of CART19 therapy. The increasingly recognized relevance of epigenetic changes in cancer immunology prompted us to determine the impact of the DNA methylation profiles of CART19 cells on the clinical course. Methods: We recruited 114 patients with B-cell malignancies, comprising 77 patients with acute lymphoblastic leukemia and 37 patients with non-Hodgkin lymphoma who were treated with CART19 cells. Using a comprehensive DNA methylation microarray, we determined the epigenomic changes that occur in the patient T cells upon transduction of the CAR vector. The effects of the identified DNA methylation sites on clinical response, cytokine release syndrome, immune effector cell-associated neurotoxicity syndrome, event-free survival, and overall survival were assessed. All statistical tests were 2-sided. Results: We identified 984 genomic sites with differential DNA methylation between CAR-untransduced and CAR-transduced T cells before infusion into the patient. Eighteen of these distinct epigenetic loci were associated with complete response (CR), adjusting by multiple testing. Using the sites linked to CR, an epigenetic signature, referred to hereafter as the EPICART signature, was established in the initial discovery cohort (n = 79), which was associated with CR (Fisher exact test, P <. 001) and enhanced event-free survival (hazard ratio [HR] = 0.36; 95% confidence interval [CI] = 0.19 to 0.70; P =. 002; log-rank P =. 003) and overall survival (HR = 0.45; 95% CI = 0.20 to 0.99; P =. 047; log-rank P =. 04;). Most important, the EPICART profile maintained its clinical course predictive value in the validation cohort (n = 35), where it was associated with CR (Fisher exact test, P <. 001) and enhanced overall survival (HR = 0.31; 95% CI = 0.11 to 0.84; P =. 02; log-rank P

Published

2022

12. Oncolytic adenovirus and gene therapy with EphA2-BiTE for the treatment of pediatric high-grade gliomas

Author

Arnone, C. M., Polito, V. A., Mastronuzzi, A., Carai, A., Diomedi, F. C., Antonucci, L., Petrilli, L. L., Vinci, M., Ferrari, F., Salviato, E., Scarsella, M., De Stefanis, C., Weber, G., Quintarelli, C., De Angelis, B., Brenner, M. K., Gottschalk, S., Hoyos, V., Locatelli, Franco, Caruana, I., Del Bufalo, F., Locatelli F. (ORCID:0000-0002-7976-3654), Arnone, C. M., Polito, V. A., Mastronuzzi, A., Carai, A., Diomedi, F. C., Antonucci, L., Petrilli, L. L., Vinci, M., Ferrari, F., Salviato, E., Scarsella, M., De Stefanis, C., Weber, G., Quintarelli, C., De Angelis, B., Brenner, M. K., Gottschalk, S., Hoyos, V., Locatelli, Franco, Caruana, I., Del Bufalo, F., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Background Pediatric high-grade gliomas (pHGGs) are among the most common and incurable malignant neoplasms of childhood. Despite aggressive, multimodal treatment, the outcome of children with high-grade gliomas has not significantly improved over the past decades, prompting the development of innovative approaches. Methods To develop an effective treatment, we aimed at improving the suboptimal antitumor efficacy of oncolytic adenoviruses (OAs) by testing the combination with a gene-Therapy approach using a bispecific T-cell engager (BiTE) directed towards the erythropoietin-producing human hepatocellular carcinoma A2 receptor (EphA2), conveyed by a replication-incompetent adenoviral vector (EphA2 adenovirus (EAd)). The combinatorial approach was tested in vitro, in vivo and thoroughly characterized at a molecular level. Results After confirming the relevance of EphA2 as target in pHGGs, documenting a significant correlation with worse clinical outcome of the patients, we showed that the proposed strategy provides significant EphA2-BiTE amplification and enhanced tumor cell apoptosis, on coculture with T cells. Moreover, T-cell activation through an agonistic anti-CD28 antibody further increased the activation/proliferation profiles and functional response against infected tumor cells, inducing eradication of highly resistant, primary pHGG cells. The gene-expression analysis of tumor cells and T cells, after coculture, revealed the importance of both EphA2-BiTE and costimulation in the proposed system. These in vitro observations translated into significant tumor control in vivo, in both subcutaneous and a more challenging orthotopic model. Conclusions The combination of OA and EphA2-BiTE gene therapy strongly enhances the antitumor activity of OA, inducing the eradication of highly resistant tumor cells, thus supporting the clinical translation of the approach.

Published

2021

13. NPM1 mutational status underlines different biological features in pediatric AML

Author

Tregnago, C., Benetton, M., Padrin, D., Polato, K., Borella, G., Da Ros, A., Marchetti, A., Porcu, E., Del Bufalo, F., Mecucci, C., Locatelli, Franco, Pigazzi, M., Locatelli F. (ORCID:0000-0002-7976-3654), Tregnago, C., Benetton, M., Padrin, D., Polato, K., Borella, G., Da Ros, A., Marchetti, A., Porcu, E., Del Bufalo, F., Mecucci, C., Locatelli, Franco, Pigazzi, M., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Nucleophosmin (NPM1) is a nucleocytoplasmic shuttling protein, predominantly located in the nucleolus, that regulates a multiplicity of different biological processes. NPM1 localization in the cell is finely tuned by specific signal motifs, with two tryptophan residues (Trp) being essential for the nucleolar localization. In acute myeloid leukemia (AML), several NPM1 mutations have been reported, all resulting in cytoplasmic delocalization, but the putative biological and clinical significance of different variants are still debated. We explored HOXA and HOXB gene expression profile in AML patients and found a differential expression between NPM1 mutations inducing the loss of two (A-like) Trp residues and those determining the loss of one Trp residue (non-A-like). We thus expressed NPM1 A-like-or non-A-like-mutated vectors in AML cell lines finding that NPM1 partially remained in the nucleolus in the non-A-like NPM1-mutated cells. As a result, only in A-like-mutated cells we detected HOXA5, HOXA10, and HOXB5 hyper-expression and p14ARF/p21/p53 pathway deregulation, leading to reduced sensitivity to the treatment with either chemotherapy or Venetoclax, as compared to non-A-like cells. Overall, we identified that the NPM1 mutational status mediates crucial biological characteristics of AML cells, providing the basis for further sub-classification and, potentially, management of this subgroup of patients.

Published

2021

14. Antifungal effect of all-trans retinoic acid against aspergillus fumigatus in vitro and in a pulmonary aspergillosis in vivo model

Author

Campione, E., Gaziano, R., Doldo, E., Marino, D., Falconi, M., Iacovelli, F., Tagliaferri, D., Pacello, L., Bianchi, L., Lanna, C., Aurisicchio, L., Centofanti, F., Di Francesco, P., Del Principe, I., Del Bufalo, F., Locatelli, Franco, Pistoia, E. S., Marra, E., Orlandi, A., Locatelli F. (ORCID:0000-0002-7976-3654), Campione, E., Gaziano, R., Doldo, E., Marino, D., Falconi, M., Iacovelli, F., Tagliaferri, D., Pacello, L., Bianchi, L., Lanna, C., Aurisicchio, L., Centofanti, F., Di Francesco, P., Del Principe, I., Del Bufalo, F., Locatelli, Franco, Pistoia, E. S., Marra, E., Orlandi, A., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Aspergillus fumigatus is the most common opportunistic fungal pathogen and causes invasive pulmonary aspergillosis (IPA), with high mortality among immunosuppressed patients. The fungistatic activity of all-trans retinoic acid (ATRA) has been recently described in vitro. We evaluated the efficacy of ATRA in vivo and its potential synergistic interaction with other antifungal drugs. A rat model of IPA and in vitro experiments were performed to assess the efficacy of ATRA against Aspergillus in association with classical antifungal drugs and in silico studies used to clarify its mechanism of action. ATRA (0.5 and 1 mM) displayed a strong fungistatic activity in Aspergillus cultures, while at lower concentrations, synergistically potentiated fungistatic efficacy of subinhibitory concentration of amphotericin B (AmB) and posaconazole (POS). ATRA also enhanced macrophagic phagocytosis of conidia. In a rat model of IPA, ATRA reduced mortality similarly to posaconazole. Fungistatic efficacy of ATRA alone and synergistically with other antifungal drugs was documented in vitro, likely by inhibiting fungal heat shock protein 90 (Hsp90) expression and Hsp90-related genes. ATRA treatment reduced mortality in a model of IPA in vivo. Those findings suggest ATRA as a suitable fungistatic agent that can also reduce dosage and adverse reactions of classical antifungal drugs and add to the development of new therapeutic strategies against IPA and systemic fungal infections.

Published

2021

15. Strategy to prevent epitope masking in CAR.CD19+ B-cell leukemia blasts

Author

Quintarelli, C., Guercio, M., Manni, S., Boffa, I., Sinibaldi, M., DI Cecca, S., Caruso, S., Abbaszadeh, Z., Camera, A., Cembrola, B., Ciccone, R., Orfao, A., Martin-Martin, L., Gutierrez-Herrero, S., Herrero-Garcia, M., Cazzaniga, G., Nunes, V., Songia, S., Marcatili, P., Marin, F. I., Ruella, M., Bertaina, V., Vinti, L., Del Bufalo, F., Algeri, M., Merli, P., De Angelis, B., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Quintarelli, C., Guercio, M., Manni, S., Boffa, I., Sinibaldi, M., DI Cecca, S., Caruso, S., Abbaszadeh, Z., Camera, A., Cembrola, B., Ciccone, R., Orfao, A., Martin-Martin, L., Gutierrez-Herrero, S., Herrero-Garcia, M., Cazzaniga, G., Nunes, V., Songia, S., Marcatili, P., Marin, F. I., Ruella, M., Bertaina, V., Vinti, L., Del Bufalo, F., Algeri, M., Merli, P., De Angelis, B., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Chimeric antigen receptor T-cells (CAR T-cells) for the treatment of relapsing/refractory B-cell precursor acute lymphoblastic leukemia have led to exciting clinical results. However, CAR T-cell approaches revealed a potential risk of CD19-/CAR+ leukemic relapse due to inadvertent transduction of leukemia cells. BackgroundMethods We evaluated the impact of a high percentage of leukemia blast contamination in patient-derived starting material (SM) on CAR T-cell drug product (DP) manufacturing. In vitro as well as in vivo models were employed to identify characteristics of the construct associated with better profile of safety in case of inadvertent B-cell leukemia transduction during CAR T-cell manufacturing. Results The presence of large amounts of CD19+ cells in SM did not affect the transduction level of DPs, as well as the CAR T-cell rate of expansion at the end of standard production of 14 days. DPs were deeply characterized by flow cytometry and molecular biology for Ig-rearrangements, showing that the level of B-cell contamination in DPs did not correlate with the percentage of CD19+ cells in SM, in the studied patient cohort. Moreover, we investigated whether CAR design may affect the control of CAR+ leukemia cells. We provided evidences that CAR.CD19 short linker (SL) prevents complete epitope masking in CD19+CAR+ leukemia cells and we demonstrated in vitro and in vivo that CD19 +CAR(SL)+leukemic cells are killed by CAR.CD19 T-cells. Conclusions Taken together, these data suggest that a VL-VH SL may result in a safe CAR-T product, even when manufacturing starts from biological materials characterized by heavy contamination of leukemia blasts.

Published

2021

16. Developing cell therapies as drug products

Author

Ciccocioppo, R., Comoli, P., Astori, G., del Bufalo, F., Prapa, M., Dominici, M., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Ciccocioppo, R., Comoli, P., Astori, G., del Bufalo, F., Prapa, M., Dominici, M., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

In the last 20 years, the global regulatory frameworks for drug assessment have been managing the challenges posed by using cellular products as new therapeutic tools. Currently, they are defined as “Advanced Therapy Medicinal Products”, comprising a large group of cellular types that either alone or in combination with gene and tissue engineering technology. They have the potential to change the natural course of still lethal or highly debilitating diseases, including cancers, opportunistic infections and chronic inflammatory conditions. Globally, more than 50 cell-based products have obtained market authorization. This overview describes the advantages and unsolved challenges on developing cells as innovative therapeutic vehicles. The main cell therapy players and the legal framework are discussed, starting from chimeric antigen receptor T-cells for leukaemia and solid tumours, dealing then with lymphocytes as potent anti-microbiological tools and then focusing on mesenchymal stem/stromal cells whose role covers regenerative medicine, immunology and anti-tumour therapy.

Published

2021

17. Hemoperfusion with CytoSorb to Manage Multiorgan Dysfunction in the Spectrum of Hemophagocytic Lymphohistiocytosis Syndrome in Critically Ill Children

Author

Bottari, G., Murciano, M., Merli, P., Bracaglia, C., Guzzo, I., Stoppa, F., Pardeo, M., Nunziata, J., Del Bufalo, F., Genuini, L., De Benedetti, F., Locatelli, Franco, Cecchetti, C., Locatelli F. (ORCID:0000-0002-7976-3654), Bottari, G., Murciano, M., Merli, P., Bracaglia, C., Guzzo, I., Stoppa, F., Pardeo, M., Nunziata, J., Del Bufalo, F., Genuini, L., De Benedetti, F., Locatelli, Franco, Cecchetti, C., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Hemophagocytic lymphohistiocytosis (HLH) is a life-threatening condition characterized by a state of hyperinflammation. Blood purification techniques can blunt the inflammatory process with a rapidly relevant nonselective effect on the cytokine storm, thus potentially translating into survival benefit for these patients. In this cohort, we evaluated the impact of hemoadsorption with CytoSorb combined with continuous kidney replacement therapy used as adjunctive therapy in 6 critically ill children with multiple organ dysfunction due to HLH. In our series, we found a reduction in inflammatory biomarkers in patients with HLH secondary to infection. Ferritin, one of the most important bedside biomarkers of HLH, showed a reduction in most of the treated patients. The same results were found measuring interleukin-6 and interleukin-10. The same patients showed hemodynamic stabilization measured by the Vasopressor-Inotropic-Score, and reduction in the organ disease score measured with the Pediatric Logistic Organ Dysfunction score. In our cohort, mortality was less than expected based on the Pediatric Index of Mortality 3 score at pediatric intensive care unit admission. Our study shows that hemoperfusion could be a valuable therapeutic option in HLH: stronger scientific evidence is needed to confirm our preliminary experience.

Published

2021

18. Inclusion of the Inducible Caspase 9 Suicide Gene in CAR Construct Increases Safety of CAR.CD19 T Cell Therapy in B-Cell Malignancies

Author

Guercio, M., Manni, S., Boffa, I., Caruso, S., Di Cecca, S., Sinibaldi, M., Abbaszadeh, Z., Camera, A., Ciccone, R., Polito, V. A., Ferrandino, F., Reddel, S., Catanoso, M. L., Bocceri, E., Del Bufalo, F., Algeri, M., De Angelis, B., Quintarelli, C., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Guercio, M., Manni, S., Boffa, I., Caruso, S., Di Cecca, S., Sinibaldi, M., Abbaszadeh, Z., Camera, A., Ciccone, R., Polito, V. A., Ferrandino, F., Reddel, S., Catanoso, M. L., Bocceri, E., Del Bufalo, F., Algeri, M., De Angelis, B., Quintarelli, C., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

T cells engineered with chimeric antigen receptor (CAR-T cells) are an effective treatment in patients with relapsed/refractory B-cell precursor acute lymphoblastic leukemia or B-cell non-Hodgkin lymphoma. Despite the reported exciting clinical results, the CAR-T cell approach needs efforts to improve the safety profile, limiting the occurrence of adverse events in patients given this treatment. Besides the most common side effects, such as cytokine release syndrome and CAR-T cell–related encephalopathy syndrome, another potential issue involves the inadvertent transduction of leukemia B cells with the CAR construct during the manufacturing process, thus leading to the possibility of a peculiar mechanism of antigen masking and treatment resistance. In this study, we investigated whether the inclusion of the inducible caspase 9 (iC9) suicide gene in the CAR construct design could be an effective safety switch to control malignant CAR+ B cells, ultimately counteracting this serious adverse event. iC9 is a suicide gene able to be activated through binding with an otherwise inert small biomolecule, known as AP1903. The exposure of iC9.CAR.CD19-DAUDI lymphoma and iC9.CAR.CD19-NALM-6 leukemia cells in vitro to 20 nM of AP1903 resulted into the prompt elimination of CAR+ B-leukemia/lymphoma cell lines. The results obtained in the animal model corroborate in vitro data, since iC9.CAR.CD19+ tumor cells were controlled in vivo by the activation of the suicide gene through administration of AP1903. Altogether, our data indicate that the inclusion of the iC9 suicide gene may result in a safe CAR-T cell product, even when manufacturing starts from biological materials characterized by heavy leukemia blast contamination.

Published

2021

19. Use of ruxolitinib to control graft-versus-host–like disease in Omenn syndrome and successfully bridging to HSCT

Author

Grasso, A. G., Del Bufalo, F., Boccieri, E., Russo, A. F., Carta, R., Algeri, M., Lombardo, M., Pagliara, D., Corsetti, T., Locatelli, Franco, Merli, P., Locatelli F. (ORCID:0000-0002-7976-3654), Grasso, A. G., Del Bufalo, F., Boccieri, E., Russo, A. F., Carta, R., Algeri, M., Lombardo, M., Pagliara, D., Corsetti, T., Locatelli, Franco, Merli, P., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

NO ABSTRACT

Published

2021

20. Polymorphonuclear myeloid-derived suppressor cells impair the anti-tumor efficacy of GD2.CAR T-cells in patients with neuroblastoma

Author

Tumino, N., Weber, G., Besi, F., Del Bufalo, F., Bertaina, V., Paci, P., Quatrini, L., Antonucci, L., Sinibaldi, M., Quintarelli, C., Maggi, E., De Angelis, B., Locatelli, Franco, Moretta, L., Vacca, P., Caruana, I., Locatelli F. (ORCID:0000-0002-7976-3654), Tumino, N., Weber, G., Besi, F., Del Bufalo, F., Bertaina, V., Paci, P., Quatrini, L., Antonucci, L., Sinibaldi, M., Quintarelli, C., Maggi, E., De Angelis, B., Locatelli, Franco, Moretta, L., Vacca, P., Caruana, I., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

The outcome of patients affected by high-risk or metastatic neuroblastoma (NB) remains grim, with ≥ 50% of the children experiencing relapse or progression of the disease despite multimodal, intensive treatment. In order to identify new strategies to improve the overall survival and the quality of life of these children, we recently developed and optimized a third-generation GD2-specific chimeric antigen receptor (CAR) construct, which is currently under evaluation in our Institution in a phase I/II clinical trial (NCT03373097) enrolling patients with relapsed/refractory NB. We observed that our CAR T-cells are able to induce marked tumor reduction and even achieve complete remission with a higher efficiency than that of other CAR T-cells reported in previous studies. However, often responses are not sustained and relapses occur. Here, we demonstrate for the first time a mechanism of resistance to GD2.CAR T-cell treatment, showing how polymorphonuclear myeloid-derived suppressor cells (PMN-MDSC) increase in the peripheral blood (PB) of NB patients after GD2.CAR T-cell treatment in case of relapse and loss of response. In vitro, isolated PMN-MDSC demonstrate to inhibit the anti-tumor cytotoxicity of different generations of GD2.CAR T-cells. Gene-expression profiling of GD2.CAR T-cells “conditioned” with PMN-MDSC shows downregulation of genes involved in cell activation, signal transduction, inflammation and cytokine/chemokine secretion. Analysis of NB gene-expression dataset confirms a correlation between expression of these genes and patient outcome. Moreover, in patients treated with GD2.CAR T-cells, the frequency of circulating PMN-MDSC inversely correlates with the levels of GD2.CAR T-cells, resulting more elevated in patients who did not respond or lost response to the treatment. The presence and the frequency of PMN-MDSC in PB of high-risk and metastatic NB represents a useful prognostic marker to predict the response to GD2.CAR T-cells and other adoptive immun

Published

2021

21. NK cells as adoptive cellular therapy for hematological malignancies: Advantages and hurdles

Author

Caruso, S., De Angelis, B., Carlomagno, S., Del Bufalo, F., Sivori, S., Locatelli, Franco, Quintarelli, C., Locatelli F. (ORCID:0000-0002-7976-3654), Caruso, S., De Angelis, B., Carlomagno, S., Del Bufalo, F., Sivori, S., Locatelli, Franco, Quintarelli, C., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Natural killer cells are an essential component of the innate immune system and play a crucial role in immunity against malignancies, without, at difference with T cells, requiring antigen priming or inducing graft-versus-host-disease. Hence, Natural Killer cells can provide a valuable source of allogeneic “off-the-shelf” adoptive therapy and mediate major antileukemia effects, without inducing potentially lethal alloreactivity. Several cell sources have been used for producing and expanding large numbers of clinical-grade natural killer cells. In this review, we will discuss the advantages and challenges of Natural Killer cell-based therapeutic approaches for hematological malignancies, also exploring different strategies to potentiate their clinical application.

Published

2020

22. Efficacy of third-party chimeric antigen receptor modified peripheral blood natural killer cells for adoptive cell therapy of B-cell precursor acute lymphoblastic leukemia

Author

Quintarelli, C., Sivori, S., Caruso, S., Carlomagno, S., Falco, M., Boffa, I., Orlando, D., Guercio, M., Abbaszadeh, Z., Sinibaldi, M., Di Cecca, S., Camera, A., Cembrola, B., Pitisci, A., Andreani, M., Vinti, L., Gattari, S., Del Bufalo, F., Algeri, M., Li Pira, G., Moseley, A., De Angelis, B., Moretta, L., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Quintarelli, C., Sivori, S., Caruso, S., Carlomagno, S., Falco, M., Boffa, I., Orlando, D., Guercio, M., Abbaszadeh, Z., Sinibaldi, M., Di Cecca, S., Camera, A., Cembrola, B., Pitisci, A., Andreani, M., Vinti, L., Gattari, S., Del Bufalo, F., Algeri, M., Li Pira, G., Moseley, A., De Angelis, B., Moretta, L., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

We developed an innovative and efficient, feeder-free culture method to genetically modify and expand peripheral blood-derived NK cells with high proliferative capacity, while preserving the responsiveness of their native activating receptors. Activated peripheral blood NK cells were efficiently transduced by a retroviral vector, carrying a second-generation CAR targeting CD19. CAR expression was demonstrated across the different NK-cell subsets. CAR.CD19-NK cells display higher antileukemic activity toward CD19+ cell lines and primary blasts obtained from patients with B-cell precursor ALL compared with unmodified NK cells. In vivo animal model data showed that the antileukemia activity of CAR.CD19-NK cell is superimposable to that of CAR-T cells, with a lower xenograft toxicity profile. These data support the feasibility of generating feeder-free expanded, genetically modified peripheral blood NK cells for effective “off-the-shelf” immuno-gene-therapy, while their innate alloreactivity can be safely harnessed to potentiate allogeneic cell therapy.

Published

2020

23. Cancer Predisposition Syndromes Associated With Pediatric High-Grade Gliomas

Author

Ceglie, G., Del Baldo, G., Agolini, E., Rinelli, M., Cacchione, A., Del Bufalo, F., Vinci, M., Carta, R., Boccuto, L., Miele, E., Mastronuzzi, A., Locatelli, Franco, Carai, A., Locatelli F. (ORCID:0000-0002-7976-3654), Ceglie, G., Del Baldo, G., Agolini, E., Rinelli, M., Cacchione, A., Del Bufalo, F., Vinci, M., Carta, R., Boccuto, L., Miele, E., Mastronuzzi, A., Locatelli, Franco, Carai, A., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Pediatric High-Grade Gliomas (pHGG) are among the deadliest childhood brain tumors and can be associated with an underlying cancer predisposing syndrome. The thorough understanding of these syndromes can aid the clinician in their prompt recognition, leading to an informed genetic counseling for families and to a wider understanding of a specific genetic landscape of the tumor for target therapies. In this review, we summarize the main pHGG-associated cancer predisposing conditions, providing a guide for suspecting these syndromes and referring for genetic counseling.

Published

2020

24. Multimodal Therapeutic Approach of Cytokine Release Syndrome Developing in a Child Given Chimeric Antigen Receptor-Modified T Cell Infusion

Author

Bottari, G., Merli, P., Guzzo, I., Stoppa, F., Ruggeri, A., Di Nardo, M., Del Bufalo, F., Galaverna, F., Corrado, C., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Bottari, G., Merli, P., Guzzo, I., Stoppa, F., Ruggeri, A., Di Nardo, M., Del Bufalo, F., Galaverna, F., Corrado, C., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Objectives: To describe a pediatric case of cytokine release syndrome secondary to chimeric antigen receptor-modified T cells associated with acute respiratory distress syndrome. Design: Case report. Setting: PICU. Patients: A 14-year-old boy with refractory B cell precursor acute lymphoblastic leukemia given chimeric antigen receptor cells developed severe cytokine release syndrome 7 days after the drug product infusion with progressive respiratory failure. He was admitted to PICU with a clinical picture of acute respiratory distress syndrome, requiring mechanical ventilation, and secondary hemophagocytic lymphohistiocytosis. Interventions: Hemoadsorption with cartridge column (Cytosorb) in combination with continuous renal replacement therapy was associated to the anti-cytokine therapy (tocilizumab, a monoclonal antibody targeting interleukin-6 receptor). Measurements and Main Results: Decrease of the inflammatory biomarkers (ferritin, interleukin-6, interleukin-10) in the first 96 hours associated with a progressive improvement of acute respiratory distress syndrome (Pao2/Fio2ratio) 7 day after the start of the multimodal treatment. Conclusions: This case suggests that hemoadsorption with cartridge column in combination with continuous renal replacement therapy and tocilizumab is safe and potentially effective in pediatric patients with severe cytokine release syndrome.

Published

2020

25. Reversible induction of mitophagy by an optogenetic bimodular system

Author

D'Acunzo, P., Strappazzon, F., Caruana, I., Meneghetti, G., Di Rita, A., Simula, L., Weber, G., Del Bufalo, F., Dalla Valle, L., Campello, S., Locatelli, Franco, Cecconi, Francesco, Locatelli F. (ORCID:0000-0002-7976-3654), Cecconi F. (ORCID:0000-0002-5614-4359), D'Acunzo, P., Strappazzon, F., Caruana, I., Meneghetti, G., Di Rita, A., Simula, L., Weber, G., Del Bufalo, F., Dalla Valle, L., Campello, S., Locatelli, Franco, Cecconi, Francesco, Locatelli F. (ORCID:0000-0002-7976-3654), and Cecconi F. (ORCID:0000-0002-5614-4359)

Abstract

Autophagy-mediated degradation of mitochondria (mitophagy) is a key process in cellular quality control. Although mitophagy impairment is involved in several patho-physiological conditions, valuable methods to induce mitophagy with low toxicity in vivo are still lacking. Herein, we describe a new optogenetic tool to stimulate mitophagy, based on light-dependent recruitment of pro-autophagy protein AMBRA1 to mitochondrial surface. Upon illumination, AMBRA1-RFP-sspB is efficiently relocated from the cytosol to mitochondria, where it reversibly mediates mito-aggresome formation and reduction of mitochondrial mass. Finally, as a proof of concept of the biomedical relevance of this method, we induced mitophagy in an in vitro model of neurotoxicity, fully preventing cell death, as well as in human T lymphocytes and in zebrafish in vivo. Given the unique features of this tool, we think it may turn out to be very useful for a wide range of both therapeutic and research applications.

Published

2019

26. B-cell depleting immunotherapies: therapeutic opportunities and toxicities

Author

Del Bufalo, F., Merli, P., Alessi, I., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Del Bufalo, F., Merli, P., Alessi, I., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Introduction: The last few years have witnessed what can certainly be defined as a ‘period of renaissance’ for immunotherapy in the field of hematological malignancies. In particular, antibody-mediated and cell-mediated immunotherapy have significantly changed the treatment approach of patients with B-cell lymphoproliferative disorders. These therapies, initially employed in patients with refractory/relapsed disease, are now integrated in the treatment of newly diagnosed patients. Together with the therapeutic success, we have also learnt that these innovative therapies can induce relevant, sometimes life-threatening or even fatal, side effects. Areas covered: In this review article, we analyzed the applicative therapeutic scenario and the peculiar toxicities associated with approaches of immunotherapy, paying particular attention to the new emerging side effects, substantially unknown before the introduction of these therapies. Expert commentary: Both monoclonal antibodies and cell therapy with lymphocytes genetically modified to be redirected against leukemia targets through the transduction with chimeric antigen receptors (CARs) have obtained unprecedented success in rescuing patients with resistant B-cell malignancies. Complications, such as neurotoxicity, cytokine release syndrome or persistent B-cell lymphopenia, must always be taken into consideration and diagnosed in a timely manner in patients with B-cell neoplasms to guarantee optimal management, thus avoiding they blunting the efficacy of immunotherapy.

Published

2019

27. Vemurafenib treatment of pleomorphic xanthoastrocytoma in a child with down syndrome

Author

Petruzzellis, G., Valentini, D., Del Bufalo, F., Ceglie, G., Carai, A., Colafati, G. S., Agolini, E., Diomedi-Camassei, F., Corsetti, T., Alessi, I., Mastronuzzi, A., Locatelli, Franco, Cacchione, A., Locatelli F. (ORCID:0000-0002-7976-3654), Petruzzellis, G., Valentini, D., Del Bufalo, F., Ceglie, G., Carai, A., Colafati, G. S., Agolini, E., Diomedi-Camassei, F., Corsetti, T., Alessi, I., Mastronuzzi, A., Locatelli, Franco, Cacchione, A., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Brain tumors are the most common solid neoplasms of childhood, but they are very rarely reported in children with Down Syndrome (DS), who develop more commonly different types of malignancies. In particular, we hereby report the case of an 8-years-old child with DS that presented to our attention for neurological and endocrinological issues. Brain imaging revealed the presence of a mass that was partially resected revealing a histological diagnosis of Pleomorphic Xanthoastrocytoma (PXA), a rare WHO grade II tumor extending from the diencephalic region into the surrounding brain tissue. These tumors can harbor the BRAF mutation p.V600E, targetable by the specific inhibitor Vemurafenib. After confirming the presence of the mutation in the tumor, the patient was treated with Vemurafenib. The treatment proved to be effective, leading to a partial response and a stabilization of the disease. Usually, in patients with DS a reduction of the dose of chemotherapeutic drugs is necessary. Vemurafenib was instead well-tolerated as the only observed adverse effect was grade I skin toxicity. This is, to our knowledge, the first case of a PXA reported in a child with DS and the first DS patient treated with Vemurafenib.

Published

2019

28. Hematopoietic Stem Cell Transplantation in Pediatric Acute Lymphoblastic Leukemia

Author

Merli, P., Algeri, M., Del Bufalo, F., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Merli, P., Algeri, M., Del Bufalo, F., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Purpose of Review: The remarkable improvement in the prognosis of children with acute lymphoblastic leukemia (ALL) has been mainly achieved through the administration of risk-adapted therapy, including allogeneic hematopoietic stem cell transplantation (HSCT). This paper reviews the current indications to HSCT in ALL children, as well as the type of donor and conditioning regimens commonly used. Finally, it will focus on future challenges in immunotherapy. Recent Findings: As our comprehension of disease-specific risk factors improves, indications to HSCT continue to evolve. Future studies will answer the year-old question on the best conditioning regimen to be used in this setting, while a recent randomized controlled study fixed the optimal anti-thymocyte globulin dose in unrelated donor HSCT. Summary: HSCT, the oldest immunotherapy used in clinical practice, still represents the gold standard consolidation treatment for a number of pediatric patients with high-risk/relapsed ALL. New immunotherapies hold the promise of further improving outcomes in this setting.

Published

2019

29. Results of a Multicentre, Randomized, Controlled Open-Label Study on the Use of Anti-T-Lymphocyte Globulin (ATLG) and Rituximab for Immunomodulation of Graft-Versus-Host Disease (GvHD) and Graft Failure (GF) in Patients with Non-Malignant Disorders.

Author

Algeri, M, Galimberti, S, Bernardo, M, Rovelli, A, Zecca, M, La Nasa, G, Marktel, S, Merli, P, Bertaina, A, Pagliara, D, Boccieri, E, Del Bufalo, F, Gaspari, S, Ruggeri, A, Capitoli, G, Valsecchi, M, Locatelli, F, Bernardo, ME, Valsecchi, MG, Algeri, M, Galimberti, S, Bernardo, M, Rovelli, A, Zecca, M, La Nasa, G, Marktel, S, Merli, P, Bertaina, A, Pagliara, D, Boccieri, E, Del Bufalo, F, Gaspari, S, Ruggeri, A, Capitoli, G, Valsecchi, M, Locatelli, F, Bernardo, ME, and Valsecchi, MG

Published

2019

30. Efficacy of third-party chimeric antigen receptor modified peripheral blood natural killer cells for adoptive cell therapy of B-cell precursor acute lymphoblastic leukemia

Author

Quintarelli, C., primary, Sivori, S., additional, Caruso, S., additional, Carlomagno, S., additional, Falco, M., additional, Boffa, I., additional, Orlando, D., additional, Guercio, M., additional, Abbaszadeh, Z., additional, Sinibaldi, M., additional, Di Cecca, S., additional, Camera, A., additional, Cembrola, B., additional, Pitisci, A., additional, Andreani, M., additional, Vinti, L., additional, Gattari, S., additional, Del Bufalo, F., additional, Algeri, M., additional, Li Pira, G., additional, Moseley, A., additional, De Angelis, B., additional, Moretta, L., additional, and Locatelli, F., additional

Published

2019

31. S1635 ACADEMIC, PHASE1 TRIAL ON T CELLS EXPRESSING BOTH CD19 CHIMERIC ANTIGEN RECEPTOR AND INDUCIBLE CASPASE 9 SAFETY SWITCH FOR TREATMENT OF CHILDHOOD ACUTE LYMPHOBLASTIC LEUKAEMIA AND NON-HODGKIN LYMPHOMA

Author

Del Bufalo, F., primary, Merli, P., additional, Vinti, L., additional, Algeri, M., additional, Cefalo, M.G., additional, Bertaina, V., additional, Li Pira, G., additional, Caruana, I., additional, De Angelis, B., additional, Boffa, I., additional, De Cecca, S., additional, Orlando, D., additional, Guercio, M., additional, Sinibaldi, M., additional, Abbaszadeh, Z., additional, Polito, V.A., additional, Cristantielli, R., additional, Quintarelli, C., additional, and Locatelli, F., additional

Published

2019

32. Choice of costimulatory domains and of cytokines determines CAR T-cell activity in neuroblastoma

Author

Quintarelli, C., Orlando, D., Boffa, I., Guercio, M., Polito, V. A., Petretto, A., Lavarello, C., Sinibaldi, M., Weber, G., Del Bufalo, F., Giorda, E., Scarsella, M., Petrini, S., Pagliara, D., Locatelli, Franco, De Angelis, B., Caruana, I., Locatelli F. (ORCID:0000-0002-7976-3654), Quintarelli, C., Orlando, D., Boffa, I., Guercio, M., Polito, V. A., Petretto, A., Lavarello, C., Sinibaldi, M., Weber, G., Del Bufalo, F., Giorda, E., Scarsella, M., Petrini, S., Pagliara, D., Locatelli, Franco, De Angelis, B., Caruana, I., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Chimeric antigen receptor (CAR) T-cell therapy has been shown to be dramatically effective in the treatment of B-cell malignancies. However, there are still substantial obstacles to overcome, before similar responses can be achieved in patients with solid tumors. We evaluated both in vitro and in a preclinical murine model the efficacy of different 2nd and 3rd generation CAR constructs targeting GD2, a disial-ganglioside expressed on the surface of neuroblastoma (NB) tumor cells. In order to address potential safety concerns regarding clinical application, an inducible safety switch, namely inducible Caspase-9 (iC9), was also included in the vector constructs. Our data indicate that a 3rd generation CAR incorporating CD28.4-1BB costimulatory domains is associated with improved anti-tumor efficacy as compared with a CAR incorporating the combination of CD28.OX40 domains. We demonstrate that the choice of 4-1BB signaling results into significant amelioration of several CAR T-cell characteristics, including: 1) T-cell exhaustion, 2) basal T-cell activation, 3) in vivo tumor control and 4) T-cell persistence. The fine-tuning of T-cell culture conditions obtained using IL7 and IL15 was found to be synergic with the CAR.GD2 design in increasing the anti-tumor activity of CAR T cells. We also demonstrate that activation of the suicide gene iC9, included in our construct without significantly impairing neither CAR expression nor anti-tumor activity, leads to a prompt induction of apoptosis of GD2.CAR T cells. Altogether, these findings are instrumental in optimizing the function of CAR T-cell products to be employed in the treatment of children with NB.

Published

2018

33. Current and future role of bispecific T-cell engagers in pediatric acute lymphoblastic leukemia

Author

Algeri, M., Del Bufalo, F., Galaverna, F., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Algeri, M., Del Bufalo, F., Galaverna, F., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Introduction: The clinical application of immunotherapy has resulted into a significant improvement in the outcome of children with relapsed/refractory B-cell precursor acute lymphoblastic leukemia (r/r BCP-ALL). In this setting, the use of bispecific T-cell-engager antibodies (BiTEs), such as blinatumomab, which harness the cytotoxic activity of T cells against CD19-positive lymphoblasts, has emerged as a most promising and impactful strategy. Areas covered: This review discusses the main structural and functional features of BiTEs, as well as the current status of their clinical application in childhood ALL. Moreover, future prospects to increase the efficacy of BiTEs are addressed. Expert commentary: The promising results obtained in patients with advanced BCP-ALL pave the way for further improvement in the context of less resistant/advanced disease. Future research is rapidly progressing on several aspects, including the use of blinatumomab in first-line protocols, identification of factors predicting response, use of combinatorial approaches and bioengineering of new molecules with dual specificity or increased potency, stability and half-life. The results of these studies, expected to be available in the next future, will provide further advancement in the development of effective, impactful, targeted immunotherapy for treatment of childhood BCP-ALL, with the concrete potential to revolutionize the clinical practice.

Published

2018

34. Trapianto di midollo osseo allogeneico da donatore HLA-aploidentico con deplezione negativa di linfociti T-alfa/beta o da donatore non consaguineo: confronto tra 2 approcci nella popolazione pediatrica

Author

Galaverna, F., Zecca, M., Algeri, M., Saglio, F., Perotti, C., Rovelli, A., Lanino, E., Prete, A., Iori, A. P., Tumino, M., Favre, C., Cesaro, S., Ripaldi, M., Casazza, G., Rabusin, M., Del Bufalo, F., Fagioli, F., Bertaina, A., and Locatelli, F.

Subjects

aploidentico, trapianto di cellule staminali emopoietiche, aploidentico, donatore volontario, donatore volontario, trapianto di cellule staminali emopoietiche

Published

2017

35. Efficacy and Safety of Dimeticone in the Treatment of Lice Infestation through Prophylaxis of Classmates

Author

Ferrara, P., Del Bufalo, F., Romano, V., Eloisa Tiberi, Bottaro, G., Romani, L., Malamisura, M., Ian-Niello, F., Ceni, L., Mottini, G., and Gatto, A.

Subjects

School, Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA, Dimeticone, lcsh:Public aspects of medicine, parasitic diseases, Head Lice, Original Article, lcsh:RA1-1270

Abstract

Background We conducted a study to evaluate efficacy and safety of dimeticone 4%, a lotion with no conventional insecticide activity, to cure lice infection and to prevent spread of infestation/reinfestation by prophylaxis of classmates. Methods: The study is carried out between April 2008 and June 2008 in Petranova International Institute in Rome. A total of 131 children, aged 3 to 13 years (median age: 7 years) were included in the study. All participants received treatment with dimeticone 4% that was applied both to children with the infestation, to cure it, and to all classmates, to prevent the spreading of the infestation. They have been controlled after 7 and 30 days from the application of dimeticone. Results: At baseline we found a positivity of lice infestation in 23/131 children (17.6%), whereas 108/131 (82.4%) children were free from lice. After 7 days of treatment with dimeticone 4%, 7/23 (30.4%) positive children still had lice infestation, with a cure rate of 69.6% (16/23). At 30 days 26/131 children (19.9%) were infested: 15 children were lice free at baseline whereas 11 had lice at both evaluations; the cure rate amounted to 52.2% (12/23). The reinfestation rate (percentage of positive children that showed negativity at baseline) was 5.3% (7/131) at 7 days and 11.5% (15/131) at 30 days. Conclusion: The lower reinfestation rate showed in our trial suggests that this approach could be effective in reducing spreading of head lice in small communities. More studies are needed to confirm our findings.

Published

2013

36. Nephrotic Syndrome Following H1N1 Influenza in a 3-Year-Old Boy

Author

Ferrara, P., Antonio Gatto, Vitelli, O., Liberatore, P., Del Bufalo, F., and Bottaro, G.

Subjects

Nephrotic Syndrome, Oseltamivir, H1N1, virus diseases, Prednisone, Case Report, Influenza A

Abstract

Background The pandemic influenza A/H1N1, spread through the world in 2009, producing a serious epidemic in Italy. Complications are generally limited to patients at the extremes of age (65 years) and those with comorbid medical illness. The most frequent complications of influenza involve the respiratory system. Case Presentation A 3-year-old boy with a recent history of upper respiratory tract infection developed a nephrotic syndrome. Together with prednisone, furosemide and albumin bolus, a therapy with oseltamivir was started since the nasopharyngeal swab resulted positive for influenza A/H1N1. Clinical conditions and laboratory findings progressively improved during hospitalization, becoming normal during a 2 month follow up. Conclusion The possibility of a renal involvement after influenza A/H1N1 infection should be considered.

Published

2012

37. Systemic granulomatosis after surgical injection of silicone oil for retinal detachment in a child affected by Fisher-Evans syndrome

Author

Del Bufalo, F., angela mastronuzzi, Vito, R., Lombardi, A., Bernardi, B., Cefalo, M. G., and Locatelli, F.

Subjects

Churg-Strauss Syndrome, Thrombocytopenia, Childhood, Systemic granulomatosis, Injections, Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA, Vitrectomy, Retinal detachment, Humans, Silicone Oils, Female, Anemia, Hemolytic, Autoimmune, Child, Aged, Fisher-Evans syndrome, Silicon oil

Abstract

Silicone oil is used for complicated retinal detachment, but it can be associated with relevant side effects. We report a 6-year-old South American female admitted to our hospital with steroid-resistant Fisher-Evans syndrome. She also had developed a retinal detachment, managed with intravitreal oil injection. During treatment for Fisher-Evans syndrome, she progressively developed recurrent and refractory bronchospasm, peaks of hypereosinophilia and orbital soft-tissue swelling. Despite the persistent negativity of all microbiologic tests, she was treated empirically with antibiotics. Failure of the treatment led to the execution of a biopsy of the periocular tissue that revealed an intense polymorphous infiltrate constituted by numerous monoclonal population (FR2 monoclonality) of plasma-cells. A diagnosis of lymphoma with plasmacytoid differentiation was suspected and cytotoxic treatment was started without response. For the appearance of swelling in left parotid and laterocervical region, an excisional biopsy was performed and a diagnosis of granulomatous reaction to ocular implant of silicone oil was made. In consideration of the clinical evolution, enucleation was considered, but parents did not consent to the procedure until the child developed cerebral lesions suspected to be silicone localizations. After enucleation, eosinophilic count normalized and the child no longer presented any new episode of fever or swelling.In this patient a granulomatous reaction is present at distance from the site of oil injection. This case suggests caution in using this substance even in ocular diseases, especially in immunocompromised patients.

Published

2015

38. TUMOUR BIOLOGY

Author

Geller, T., primary, Prakash, V., additional, Batanian, J., additional, Guzman, M., additional, Duncavage, E., additional, Gershon, T., additional, Crowther, A., additional, Wu, J., additional, Liu, H., additional, Fang, F., additional, Davis, I., additional, Tripolitsioti, D., additional, Ma, M., additional, Kumar, K., additional, Grahlert, J., additional, Egli, K., additional, Fiaschetti, G., additional, Shalaby, T., additional, Grotzer, M., additional, Baumgartner, M., additional, Braoudaki, M., additional, Lambrou, G. I., additional, Giannikou, K., additional, Millionis, V., additional, Papadodima, S. A., additional, Settas, N., additional, Sfakianos, G., additional, Stefanaki, K., additional, Kattamis, A., additional, Spiliopoulou, C. A., additional, Tzortzatou-Stathopoulou, F., additional, Kanavakis, E., additional, Gholamin, S., additional, Mitra, S., additional, Feroze, A., additional, Zhang, M., additional, Esparza, R., additional, Kahn, S., additional, Richard, C., additional, Achrol, A., additional, Volkmer, A., additional, Liu, J., additional, Volkmer, J., additional, Majeti, R., additional, Weissman, I., additional, Cheshier, S., additional, Bhatia, K., additional, Brown, N., additional, Teague, J., additional, Lo, P., additional, Challis, J., additional, Beshay, V., additional, Sullivan, M., additional, Mechinaud, F., additional, Hansford, J., additional, Arifin, M. Z., additional, Dahlan, R. H., additional, Sobana, M., additional, Saputra, P., additional, Tisell, M. T., additional, Danielsson, A., additional, Caren, H., additional, Bhardwaj, R., additional, Chakravadhanula, M., additional, Hampton, C., additional, Ozals, V., additional, Georges, J., additional, Decker, W., additional, Kodibagkar, V., additional, Nguyen, A., additional, Legrain, M., additional, Gaub, M. P., additional, Pencreach, E., additional, Chenard, M. P., additional, Guenot, D., additional, Entz-Werle, N., additional, Kanemura, Y., additional, Ichimura, K., additional, Shofuda, T., additional, Nishikawa, R., additional, Yamasaki, M., additional, Shibui, S., additional, Arai, H., additional, Xia, J., additional, Brian, A., additional, Prins, R., additional, Pennell, C., additional, Moertel, C., additional, Olin, M., additional, Bie, L., additional, Zhang, X., additional, Olsson, M., additional, Kling, T., additional, Nelander, S., additional, Biassoni, V., additional, Bongarzone, I., additional, Verderio, P., additional, Massimino, M., additional, Magni, R., additional, Pizzamiglio, S., additional, Ciniselli, C., additional, Taverna, E., additional, De Bortoli, M., additional, Luchini, A., additional, Liotta, L., additional, Barzano, E., additional, Spreafico, F., additional, Visse, E., additional, Sanden, E., additional, Darabi, A., additional, Siesjo, P., additional, Jackson, S., additional, Cohen, K., additional, Lin, D., additional, Burger, P., additional, Rodriguez, F., additional, Yao, X., additional, Liucheng, R., additional, Qin, L., additional, Na, T., additional, Meilin, W., additional, Zhengdong, Z., additional, Yongjun, F., additional, Pfeifer, S., additional, Nister, M., additional, de Stahl, T. D., additional, Basmaci, E., additional, Orphanidou-Vlachou, E., additional, Brundler, M.-A., additional, Sun, Y., additional, Davies, N., additional, Wilson, M., additional, Pan, X., additional, Arvanitis, T., additional, Grundy, R., additional, Peet, A., additional, Eden, C., additional, Ju, B., additional, Phoenix, T., additional, Nimmervoll, B., additional, Tong, Y., additional, Ellison, D., additional, Lessman, C., additional, Taylor, M., additional, Gilbertson, R., additional, Folgiero, V., additional, del Bufalo, F., additional, Carai, A., additional, Cefalo, M. G., additional, Citti, A., additional, Rutella, S., additional, Locatelli, F., additional, Mastronuzzi, A., additional, Maher, O., additional, Khatua, S., additional, Zaky, W., additional, Lourdusamy, A., additional, Meijer, L., additional, Layfield, R., additional, Jones, D. T. W., additional, Capper, D., additional, Sill, M., additional, Hovestadt, V., additional, Schweizer, L., additional, Lichter, P., additional, Zagzag, D., additional, Karajannis, M. A., additional, Aldape, K. D., additional, Korshunov, A., additional, von Deimling, A., additional, Pfister, S., additional, Chakrabarty, A., additional, Feltbower, R., additional, Sheridon, E., additional, Hassan, H., additional, Shires, M., additional, Picton, S., additional, Hatziagapiou, K., additional, Tsorteki, F., additional, Bethanis, K., additional, Gemou-Engesaeth, V., additional, Chi, S. N., additional, Bandopadhayay, P., additional, Janeway, K., additional, Pinches, N., additional, Malkin, H., additional, Kieran, M. W., additional, Manley, P. E., additional, Green, A., additional, Goumnerova, L., additional, Ramkissoon, S., additional, Harris, M. H., additional, Ligon, K. L., additional, Kahlert, U., additional, Suarez, M., additional, Maciaczyk, J., additional, Bar, E., additional, Eberhart, C., additional, Kenchappa, R., additional, Krishnan, N., additional, Forsyth, P., additional, McKenzie, B., additional, Pisklakova, A., additional, McFadden, G., additional, Pan, W., additional, Rodriguez, L., additional, Glod, J., additional, Levy, J. M., additional, Thompson, J., additional, Griesinger, A., additional, Amani, V., additional, Donson, A., additional, Birks, D., additional, Morgan, M., additional, Handler, M., additional, Foreman, N., additional, Thorburn, A., additional, Lulla, R. R., additional, Laskowski, J., additional, Fangusaro, J., additional, DiPatri, A. J., additional, Alden, T., additional, Tomita, T., additional, Vanin, E. F., additional, Goldman, S., additional, Soares, M. B., additional, Remke, M., additional, Ramaswamy, V., additional, Wang, X., additional, Jorgensen, F., additional, Morrissy, A. S., additional, Marra, M., additional, Packer, R., additional, Bouffet, E., additional, Jabado, N., additional, Cole, B., additional, Rudzinski, E., additional, Anderson, M., additional, Bloom, K., additional, Lee, A., additional, Leary, S., additional, Leprivier, G., additional, Rotblat, B., additional, Agnihotri, S., additional, Kool, M., additional, Derry, B., additional, Taylor, M. D., additional, Sorensen, P. H., additional, Dobson, T., additional, Busschers, E., additional, Taylor, H., additional, Hatcher, R., additional, Lulla, R., additional, Rajaram, V., additional, Das, C., additional, and Gopalakrishnan, V., additional

Published

2014

39. NEUROPSYCHOLOGY

Author

Boman, K. K., primary, Hornquist, L., additional, Rickardsson, J., additional, Lannering, B., additional, Gustafsson, G., additional, Pitchford, N., additional, Davis, E., additional, Walker, D., additional, Hoang, D. H., additional, Pagnier, A., additional, Cousin, E., additional, Guichardet, K., additional, Schiff, I., additional, Dubois-Teklali, F., additional, Krainik, A., additional, Lazar, M. B., additional, Resnik, K., additional, Olsson, I. T., additional, Perrin, S., additional, Burtscher, I. B., additional, Lundgren, J., additional, Kahn, A., additional, Johanson, A., additional, Korzeniewska, J., additional, Dembowska-Baginska, B., additional, Perek-Polnik, M., additional, Walsh, K., additional, Gioia, A., additional, Wells, E., additional, Packer, R., additional, de Speville, E. D., additional, Dufour, C., additional, Bolle, S., additional, Giraudat, K., additional, Longaud, A., additional, Kieffer, V., additional, Grill, J., additional, Puget, S., additional, Valteau-Couanet, D., additional, Hetz-Pannier, L., additional, Noulhiane, M., additional, Chieffo, D., additional, Tamburrini, G., additional, Caldarelli, M., additional, Di Rocco, C., additional, Margelisch, K., additional, Studer, M., additional, Steinlin, M., additional, Leibundgut, K., additional, Heinks, T., additional, Longaud-Vales, A., additional, Chevignard, M., additional, Pujet, S., additional, Sainte-Rose, C., additional, Dellatolas, G., additional, Kahalley, L., additional, Grosshans, D., additional, Paulino, A., additional, Ris, M. D., additional, Chintagumpala, M., additional, Okcu, F., additional, Moore, B., additional, Stancel, H., additional, Minard, C., additional, Guffey, D., additional, Mahajan, A., additional, Herrington, B., additional, Raiker, J., additional, Manning, E., additional, Criddle, J., additional, Karlson, C., additional, Guerry, W., additional, Finlay, J., additional, Sands, S., additional, Dockstader, C., additional, Skocic, J., additional, Bouffet, E., additional, Laughlin, S., additional, Tabori, U., additional, Mabbott, D., additional, Moxon-Emre, I., additional, Scantlebury, N., additional, Taylor, M. D., additional, Malkin, D., additional, Law, N., additional, Kumabe, T., additional, Leonard, J., additional, Rubin, J., additional, Jung, S., additional, Kim, S.-K., additional, Gupta, N., additional, Weiss, W., additional, Faria, C., additional, Vibhakar, R., additional, Spiegler, B., additional, Janzen, L., additional, Liu, F., additional, Decker, L., additional, Lemiere, J., additional, Vercruysse, T., additional, Haers, M., additional, Vandenabeele, K., additional, Geuens, S., additional, Jacobs, S., additional, Van Gool, S., additional, Riggs, L., additional, Piscione, J., additional, Timmons, B., additional, Cunningham, T., additional, Bartels, U., additional, Chakravarty, M., additional, Laperriere, N., additional, Pipitone, J., additional, Strother, D., additional, Hukin, J., additional, Fryer, C., additional, McConnell, D., additional, Secco, D. E., additional, Cappelletti, S., additional, Gentile, S., additional, Cacchione, A., additional, Del Bufalo, F., additional, Staccioli, S., additional, Spagnoli, A., additional, Messina, R., additional, Carai, A., additional, Marras, C. E., additional, Mastronuzzi, A., additional, Brinkman, T., additional, Armstrong, G., additional, Kimberg, C., additional, Gajjar, A., additional, Srivastava, D. K., additional, Robison, L., additional, Hudson, M., additional, Krull, K., additional, Hardy, K., additional, Hostetter, S., additional, Hwang, E., additional, Leiss, U., additional, Bemmer, A., additional, Pletschko, T., additional, Grafeneder, J., additional, Schwarzinger, A., additional, Deimann, P., additional, Slavc, I., additional, Batchelder, P., additional, Wilkening, G., additional, Hankinson, T., additional, Foreman, N., additional, and Handler, M., additional

Published

2014

40. Efficacy and Safety of Dimeticone in the Treatment of Lice Infestation through Prophylaxis of Classmates

Author

Ferrara, Pietro, Del Bufalo, F, Romano, Valerio, Tiberi, Eloisa, Bottaro, G, Romani, L, Malamisura, M, Ianniello, Francesca, Ceni, L, Mottini, G, Gatto, Antonio, Ferrara, Pietro (ORCID:0000-0001-9449-3464), Ferrara, Pietro, Del Bufalo, F, Romano, Valerio, Tiberi, Eloisa, Bottaro, G, Romani, L, Malamisura, M, Ianniello, Francesca, Ceni, L, Mottini, G, Gatto, Antonio, and Ferrara, Pietro (ORCID:0000-0001-9449-3464)

Abstract

We conducted a study to evaluate efficacy and safety of dimeticone 4%, a lotion with no conventional insecticide activity, to cure lice infection and to prevent spread of infestation/reinfestation by prophylaxis of classmates.

Published

2013

41. Does anticonvulsant treatment influence pain perception in epileptic children?

Author

Ferrara, Pietro, Bottaro, G, Angeletti, S, Ianniello, F, Romano, V, Del Bufalo, F, Chiaretti, Antonio, Battaglia, Domenica Immacolata, Dicuonzo, G., Ferrara, Pietro (ORCID:0000-0001-9449-3464), Chiaretti, A (ORCID:0000-0002-9971-1640), Battaglia, Domenica Immacolata (ORCID:0000-0003-0491-4021), Ferrara, Pietro, Bottaro, G, Angeletti, S, Ianniello, F, Romano, V, Del Bufalo, F, Chiaretti, Antonio, Battaglia, Domenica Immacolata, Dicuonzo, G., Ferrara, Pietro (ORCID:0000-0001-9449-3464), Chiaretti, A (ORCID:0000-0002-9971-1640), and Battaglia, Domenica Immacolata (ORCID:0000-0003-0491-4021)

Abstract

The aims of our study were to evaluate pain perception in epileptic children and to establish the influence of anticonvulsant drugs on pain perception.

Published

2013

42. Humanitarian mission improves health conditions of schoolchildren in Ethiopia. the case of Adwa

Author

Ferrara, Pietro, Romano, Valerio, Del Bufalo, F, Bottaro, G, Caporale, O, Del Volgo, V, Vena, F, Pecoraro, R, Malamisura, M, De Angelis, Mc, Fasano, Alfonso, Ferrara, Pietro (ORCID:0000-0001-9449-3464), Ferrara, Pietro, Romano, Valerio, Del Bufalo, F, Bottaro, G, Caporale, O, Del Volgo, V, Vena, F, Pecoraro, R, Malamisura, M, De Angelis, Mc, Fasano, Alfonso, and Ferrara, Pietro (ORCID:0000-0001-9449-3464)

Abstract

OBJECTIVE: The objective of this study is to compare health conditions of schoolchildren receiving aids from the mission Kidane Mehret Integrated Project (KMIP) in the city of Adwa, Ethiopia, with the ones of the general population. METHODS: From September, 2008, to November, 2008, 400 children were randomly selected in the school inside KMIP and in the one of Adi Abetu. In phase 1, a questionnaire was distributed to children's families. In phase 2, children underwent physical examination. RESULTS: Girls from KMIP started weaning on average at 7.3+/-3.9 vs 8.3+/-4.7 months of the control group (p>0.05); boys from KMIP started weaning on average at 6.7+/-4.1 vs 8.7+/-5.1 months of the control group (p<0.01). Centiles for height for age, weight for age and BMI for age were significantly higher in girls attending KMIP compared to the control group. CONCLUSIONS: Merged data suggests the significant impact of KMIP on the schoolchildren of Adwa. Moreover, women and youngest children, usually the most discriminates, were the band of the society that benefited most from the aids coming from the mission.

Published

2013

43. Humanitarian mission improves health conditions of schoolchildren in Ethiopia. The case of Adwa

Author

Ferrara, P., primary, Romano, V., additional, Del Bufalo, F., additional, Bottaro, G., additional, Caporale, O., additional, Del Volgo, V., additional, Vena, F., additional, Pecoraro, R., additional, Malamisura, M., additional, De Angelis, M.C., additional, and Fasano, A., additional

Published

2013

44. Nephrotic Syndrome Following H1N1 Influenza in a 3-Year-Old Boy

Author

Ferrara, Pietro, Gatto, Antonio, Vitelli, O, Liberatore, P, Del Bufalo, F, Bottaro, G., Ferrara, Pietro (ORCID:0000-0001-9449-3464), Ferrara, Pietro, Gatto, Antonio, Vitelli, O, Liberatore, P, Del Bufalo, F, Bottaro, G., and Ferrara, Pietro (ORCID:0000-0001-9449-3464)

Abstract

BACKGROUND: The pandemic influenza A/H1N1, spread through the world in 2009, producing a serious epidemic in Italy. Complications are generally limited to patients at the extremes of age (<6 months or >65 years) and those with comorbid medical illness. The most frequent complications of influenza involve the respiratory system. CASE PRESENTATION: A 3-year-old boy with a recent history of upper respiratory tract infection developed a nephrotic syndrome. Together with prednisone, furosemide and albumin bolus, a therapy with oseltamivir was started since the nasopharyngeal swab resulted positive for influenza A/H1N1. Clinical conditions and laboratory findings progressively improved during hospitalization, becoming normal during a 2 month follow up. CONCLUSION: The possibility of a renal involvement after influenza A/H1N1 infection should be considered.

Published

2012

45. Atypical presentation of renal angiomyolipomas in a child with tuberous sclerosis complex

Author

Ferrara, Pietro, Gatto, Antonio, Vitelli, O, Liberatore, P, Del Bufalo, F, Bottaro, G., Ferrara, Pietro (ORCID:0000-0001-9449-3464), Ferrara, Pietro, Gatto, Antonio, Vitelli, O, Liberatore, P, Del Bufalo, F, Bottaro, G., and Ferrara, Pietro (ORCID:0000-0001-9449-3464)

Abstract

Tuberous sclerosis complex (TSC) is an autosomal dominant genetic disorder with a birth incidence of 1:6.000. It can virtually affect any organ system and all racial and ethnic groups. Clinical manifestations of TSC have variable penetrance. Many affected patients come to medical attention because of seizures or dermatological manifestations. Since no single feature of TSC is pathognomonic, an evaluation of all clinical features is necessary. Sparagana et al recommend, the execution of cranial imaging, such as brain magnetic resonance imaging (MRI) or computerized tomography (CT), and of renal ultrasound (US), on a 1-3 years basis. Brain tumors and renal lesions, in fact, account for most of the long-term morbidity and mortality caused by TSC. Renal involvement occurs with high frequency and with a wide range of severity in patients with TSC. Renal angiomyolipomas (AMLs) and cysts represent the most frequent findings in patients affected by TSC.We report the case of an 8-year old boy, born after a near term uncomplicated pregnancy, affected by TSC.

Published

2011

46. Wolf-Hirschhorn syndrome with improvement of renal function

Author

Ferrara, Pietro, Del Bufalo, F, Nicoletti, Alessandro, Romano, Valerio, Gatto, Antonio, Leoni, Chiara, Zampino, Giuseppe, Ferrara, Pietro (ORCID:0000-0001-9449-3464), Gatto , Antonio, Zampino, Giuseppe (ORCID:0000-0003-3865-3253), Ferrara, Pietro, Del Bufalo, F, Nicoletti, Alessandro, Romano, Valerio, Gatto, Antonio, Leoni, Chiara, Zampino, Giuseppe, Ferrara, Pietro (ORCID:0000-0001-9449-3464), Gatto , Antonio, and Zampino, Giuseppe (ORCID:0000-0003-3865-3253)

Abstract

Wolf-Hirschhorn syndrome (WHS) is a chromosomal disorder characterized by partial deletion of the short arm of chromosome 4. We describe a girl with a de novo unbalanced traslocation t(4;7)(p16.2;p22), associated with a mild version of a classical WHS phenotype. She did not present major urinary tract abnormalities but had parenchymal hyperechogenicity at renal ultrasound at the birth with normal renal scintigraphy. She had also a reduction of GFR with elevated levels of blood urea nitrogen and serum potassium until the age of 6 months. We followed the patient with periodic clinical examination and laboratory and radiological investigations and observed at the age of 5 years a normal renal ultrasound without parenchymal hyperechogenicity.

Published

2010

47. QUALITY OF LIFE/AFTERCARE

Author

Rednam, S., primary, Scheurer, M., additional, Adesina, A., additional, Lau, C., additional, Okcu, M., additional, Deatrick, J., additional, Ogle, S., additional, Fisher, M., additional, Barakat, L., additional, Hardie, T., additional, Li, Y., additional, Ginsberg, J., additional, Ben-Arush, M., additional, Krivoy, E., additional, Rosenkranz, R., additional, Peretz-Nahum, M., additional, Brown, R. J., additional, Love, J., additional, Warburton, D., additional, McBride, W. H., additional, Bluml, S., additional, Mueller, S., additional, Sear, K., additional, Hills, N., additional, Chettout, N., additional, Afghani, S., additional, Lew, L., additional, Tolentino, E., additional, Haas-Kogan, D., additional, Fullerton, H., additional, Reddick, W., additional, Palmer, S., additional, Glass, J., additional, Ogg, R., additional, Gajjar, A., additional, Omar, A., additional, Perkins, S., additional, Shinohara, E., additional, Spoljaric, D., additional, Isenberg, J., additional, Whittington, M., additional, Hauff, M., additional, King, A., additional, Litzelman, K., additional, Barker, E., additional, Catrine, K., additional, Puccetti, D., additional, Possin, P., additional, Witt, W., additional, Mallucci, C., additional, Kumar, R., additional, Pizer, B., additional, Williams, D., additional, Pettorini, B., additional, Piscione, J., additional, Bouffet, E., additional, Shams, I., additional, Kulkarni, A., additional, Remes, T., additional, Harila-Saari, A., additional, Suo-Palosaari, M., additional, Arikoski, P., additional, Riikonen, P., additional, Sutela, A., additional, Koskenkorva, P., additional, Ojaniemi, M., additional, Rantala, H., additional, Campen, C. J., additional, Ashby, D., additional, Fisher, P. G., additional, Monje, M., additional, Kulkarni, A. V., additional, Nakamura, H., additional, Makino, K., additional, Yano, S., additional, Kuratsu, J.-i., additional, Jadrijevic-Cvrlje, F., additional, Batinica, M., additional, Toledano, H., additional, Hoffman, T., additional, Ezer-Cohen, Y., additional, Michowiz, S., additional, Yaniv, I., additional, Cohen, I. J., additional, Adler, I., additional, Mindel, S., additional, Gopalakrishnamoorthy, M., additional, Saunders, D., additional, Gaze, M., additional, Spoudeas, H., additional, Kieffer, V., additional, Dellatolas, G., additional, Chevignard, M., additional, Puget, S., additional, Dhermain, F., additional, Grill, J., additional, Dufour, C., additional, Muir, R., additional, Hunter, A., additional, Latchman, A., additional, de Camargo, O., additional, Scheinemann, K., additional, Dhir, N., additional, Zaky, W., additional, Zomorodian, T., additional, Wong, K., additional, Dhall, G., additional, Macy, M., additional, Lauro, C., additional, Zeitler, P., additional, Foreman, N., additional, Liu, A., additional, Chocholous, M., additional, Dodier, P., additional, Peyrl, A., additional, Dieckmann, K., additional, Hausler, G., additional, Slavc, I., additional, Avula, S., additional, Garlick, D., additional, Armstrong, G., additional, Kawashima, T., additional, Leisenring, W., additional, Stovall, M., additional, Sklar, C., additional, Robison, L., additional, Samaan, C., additional, Duckworth, J., additional, Greenberg-Kushnir, N., additional, Freedman, S., additional, Eshel, R., additional, Zverling, N., additional, Elhasid, R., additional, Dvir, R., additional, Yalon, M., additional, Constantini, S., additional, Wilne, S., additional, Liu, J.-F., additional, Trusler, J., additional, Lundsell, S., additional, Kennedy, C., additional, Clough, L., additional, Dickson, N., additional, Lakhanpaul, M., additional, Baker, M., additional, Dudley, J., additional, Grundy, R., additional, Walker, D., additional, von Hoff, K., additional, Herzog, N., additional, Ottensmeier, H., additional, Grabow, D., additional, Gerber, N. U., additional, Friedrich, C., additional, von Bueren, A. O., additional, Resch, A., additional, Kortmann, R. D., additional, Kaatsch, P., additional, Doerr, H. G., additional, Rutkowski, S., additional, del Bufalo, F., additional, Mastronuzzi, A., additional, Serra, A., additional, de Sio, L., additional, Locatelli, F., additional, Biassoni, V., additional, Leonardi, M., additional, Ajovalasit, D., additional, Riva, D., additional, Vago, C., additional, Usilla, A., additional, Fidani, P., additional, Schiavello, E., additional, Gariboldi, F., additional, Massimino, M., additional, Lober, R., additional, Perrault, S., additional, Partap, S., additional, Edwards, M., additional, Fisher, P., additional, Yeom, K., additional, Salgado, D., additional, Nunes, S., additional, Vinhais, S., additional, Wells, E. M., additional, Seidel, K., additional, Ullrich, N. J., additional, Diller, L., additional, Krull, K. R., additional, Neglia, J., additional, Robison, L. L., additional, Whelan, K., additional, Russell, C. E., additional, Brownstone, D., additional, Kaise, C., additional, Bull, K., additional, Culliford, D., additional, Calaminus, G., additional, Bertin, D., additional, Vallero, S., additional, Romano, E., additional, Basso, M. E., additional, Biasin, E., additional, Fagioli, F., additional, Ziara, K., additional, L'Hotta, A., additional, Williams, A., additional, Thede, R., additional, Moore, K., additional, James, A., additional, Bjorn, E., additional, Franzen, P., additional, Haag, A., additional, Lax, A.-K., additional, Moreno, I., additional, Obeid, J., additional, Timmons, B. W., additional, Iwata, W., additional, Wagner, S., additional, Lai, J.-S., additional, Waddell, K., additional, VanLeeuwen, S., additional, Newmark, M., additional, Noonan, J., additional, O'Connell, K., additional, Urban, M., additional, Yount, S., additional, Goldman, S., additional, Igoe, D., additional, Cunningham, T., additional, Orfus, M., additional, Mabbott, D., additional, Liptak, C., additional, Manley, P., additional, Recklitis, C., additional, Zhang, P., additional, Shaikh, F., additional, Narang, I., additional, Matsumoto, K., additional, Yamasaki, K., additional, Okada, K., additional, Fujisaki, H., additional, Osugi, Y., additional, Hara, J., additional, Phipps, K., additional, Gumley, D., additional, Jacques, T., additional, Hargrave, D., additional, Michalski, A., additional, Chordas, C., additional, Chi, S., additional, Robison, N., additional, Bandopadhayay, P., additional, Marcus, K., additional, Zimmerman, M. A., additional, Goumnerova, L., additional, Kieran, M., additional, Brand, S., additional, Brinkman, T., additional, Delaney, B., additional, Diver, T., additional, Rey, C., additional, Madden, J. R., additional, Hemenway, M. S., additional, Dorneman, L., additional, Stiller, D., additional, Liu, A. K., additional, Foreman, N. K., additional, Vibhakar, R., additional, Mitchell, M., additional, Hemenway, M., additional, Madden, J., additional, Ryan, M., additional, O'Kane, R., additional, Picton, S., additional, Kenny, T., additional, Stiller, C., additional, Chumas, P., additional, Bendel, A., additional, Patterson, R., additional, Barrera, M., additional, Schulte, F., additional, Bartels, U., additional, Janzen, L., additional, Johnston, D., additional, Cataudella, D., additional, Chung, J., additional, Sung, L., additional, Hancock, K., additional, Hukin, J., additional, Zelcer, S., additional, Brandon, S., additional, Montour-Proulx, I., additional, Strother, D., additional, Cooksey, R., additional, Bowers, D., additional, Gargan, L., additional, Gode, A., additional, Klesse, L., additional, Oden, J., additional, Vega, G., additional, Sala, F., additional, Nuzzi, D., additional, Mulino, M., additional, Masotto, B., additional, Mazza, C., additional, Bricolo, A., additional, Gerosa, M., additional, Tong, M., additional, Laughlin, S., additional, Mackie, S., additional, Taylor, L., additional, Sharpe, G., additional, Al-Salihi, O., additional, and Nicolin, G., additional

Published

2012

48. Bevacizumab in pediatric cancer patients (pts): Safety concerns.

Author

Jenkner, A., primary, De Pasquale, M., additional, Castellano, A., additional, Pessolano, R., additional, Ilari, I., additional, De Ioris, M., additional, Demelas, F., additional, Del Bufalo, F., additional, Serra, A., additional, and Donfrancesco, A., additional

Published

2010

49. Wolf-Hirschhorn syndrome with improvement of renal function

Author

Ferrara, P., primary, Del Bufalo, F., additional, Nicoletti, A., additional, Romano, V., additional, Gatto, A., additional, Leoni, C., additional, and Zampino, G., additional

Published

2010

50. Diet and other metabolic approaches for patients with glioblastoma multiforme

Author

Carai, A., Benedictis, A., Del Bufalo, F., Raffaella Messina, Randi, F., and Mastronuzzi, A.