Your search keyword '"Vinti, L."' showing total 100 results

1. Improved survival and MRD remission with blinatumomab vs. chemotherapy in children with first high-risk relapse B-ALL

Author

Locatelli, F, Zugmaier, G, Rizzari, C, Morris, J, Gruhn, B, Klingebiel, T, Parasole, R, Linderkamp, C, Flotho, C, Petit, A, Micalizzi, C, Zeng, Y, Desai, R, Kormany, W, Eckert, C, Moricke, A, Sartor, M, Hrusak, O, Peters, C, Saha, V, Vinti, L, von Stackelberg, A, Locatelli F., Zugmaier G., Rizzari C., Morris J. D., Gruhn B., Klingebiel T., Parasole R., Linderkamp C., Flotho C., Petit A., Micalizzi C., Zeng Y., Desai R., Kormany W. N., Eckert C., Moricke A., Sartor M., Hrusak O., Peters C., Saha V., Vinti L., von Stackelberg A., Locatelli, F, Zugmaier, G, Rizzari, C, Morris, J, Gruhn, B, Klingebiel, T, Parasole, R, Linderkamp, C, Flotho, C, Petit, A, Micalizzi, C, Zeng, Y, Desai, R, Kormany, W, Eckert, C, Moricke, A, Sartor, M, Hrusak, O, Peters, C, Saha, V, Vinti, L, von Stackelberg, A, Locatelli F., Zugmaier G., Rizzari C., Morris J. D., Gruhn B., Klingebiel T., Parasole R., Linderkamp C., Flotho C., Petit A., Micalizzi C., Zeng Y., Desai R., Kormany W. N., Eckert C., Moricke A., Sartor M., Hrusak O., Peters C., Saha V., Vinti L., and von Stackelberg A.

Published

2023

2. Incidence and Characteristics of Hypersensitivity Reactions to PEG-asparaginase Observed in 6136 Children with Acute Lymphoblastic Leukemia Enrolled in the AIEOP-BFM ALL 2009 Study Protocol

Author

Rizzari, C, Möricke, A, Valsecchi, M, Conter, V, Zimmermann, M, Silvestri, D, Attarbaschi, A, Niggli, F, Barbaric, D, Stary, J, Elitzur, S, Cario, G, Vinti, L, Boos, J, Zucchetti, M, Lanvers-Kaminsky, C, Von Stackelberg, A, Biondi, A, Schrappe, M, Rizzari C., Möricke A., Valsecchi M. G., Conter V., Zimmermann M., Silvestri D., Attarbaschi A., Niggli F., Barbaric D., Stary J., Elitzur S., Cario G., Vinti L., Boos J., Zucchetti M., Lanvers-Kaminsky C., Von Stackelberg A., Biondi A., Schrappe M., Rizzari, C, Möricke, A, Valsecchi, M, Conter, V, Zimmermann, M, Silvestri, D, Attarbaschi, A, Niggli, F, Barbaric, D, Stary, J, Elitzur, S, Cario, G, Vinti, L, Boos, J, Zucchetti, M, Lanvers-Kaminsky, C, Von Stackelberg, A, Biondi, A, Schrappe, M, Rizzari C., Möricke A., Valsecchi M. G., Conter V., Zimmermann M., Silvestri D., Attarbaschi A., Niggli F., Barbaric D., Stary J., Elitzur S., Cario G., Vinti L., Boos J., Zucchetti M., Lanvers-Kaminsky C., Von Stackelberg A., Biondi A., and Schrappe M.

Abstract

The incidence of hypersensitivity reactions (HSRs) to PEG-asparaginase (PEG-ASNase) was evaluated in 6136 children with ALL enrolled in the AIEOP-BFM ALL 2009 study. Patients with B-cell precursor-acute lymphoblastic leukemia (BCP-ALL) were stratified as standard-risk/medium-risk (MR)/high-risk (HR) and those with T-ALL as non-High/HR. PEG-ASNase was administered intravenously at 2500 IU/sqm/dose. All patients received 2 PEG-ASNase doses in induction; thereafter non-HR versus HR patients received 1 versus 6 PEG-ASNase doses, respectively. After the single regular dose of PEG-ASNase at the beginning of delayed intensification, BCP-ALL-MR patients were randomized to receive 9 additional PEG-ASNase doses every 2 weeks (experimental arm [EA]) versus none (standard arm [SA]); HR patients were randomized to receive, in consolidation, 4 weekly PEG-ASNase doses (EA) versus none (SA). The HSR cumulative incidence (CI) was estimated adjusting for competing risks. An HSR occurred in 472 of 6136 (7.7%) patients. T-non- HR/BCP-Standard-Risk, BCP-MR-SA, BCP-MR-EA, HR-SA and HR-EA patients had 1-year-CI-HSR (±SE) rates of 5.2% (0.5), 5.2% (0.5), 4.0% (0.8), 20.2% (1.2), and 6.4% (1.3), respectively. The randomized intensification of PEG-ASNase did not significantly impact on HSR incidence in BCP-MR patients (1-y-CI-HSR 3.8% [0.8] versus 3.2% [0.6] in MR-EA versus MR-SA; P = 0.55), while impacted significantly in HR patients (1-y-CI-HSR 6.4% [1.3] versus 17.9% [1.8] in HR-EA and HR-SA, respectively; P < 0.001). The CI-HSR was comparable among non-HR groups and was not increased by a substantial intensification of PEG-ASNase in the BCP-MR-EA group whilst it was markedly higher in HR-SA than in HR-EA patients, suggesting that, in such a chemotherapy context, a continuous exposure to PEG-ASNase reduces the risk of developing an HSR.

Published

2023

3. Inotuzumab ozogamicin as single agent in pediatric patients with relapsed and refractory acute lymphoblastic leukemia: results from a phase II trial

Author

Pennesi, E, Michels, N, Brivio, E, van der Velden, V, Jiang, Y, Thano, A, Ammerlaan, A, Boer, J, Beverloo, H, Sleight, B, Chen, Y, Vormoor-Burger, B, Rives, S, Bielorai, B, Rossig, C, Petit, A, Rizzari, C, Engstler, G, Stary, J, Bautista Sirvent, F, Chen-Santel, C, Bruno, B, Bertrand, Y, Rialland, F, Plat, G, Reinhardt, D, Vinti, L, Von Stackelberg, A, Locatelli, F, Zwaan, C, Pennesi E., Michels N., Brivio E., van der Velden V. H. J., Jiang Y., Thano A., Ammerlaan A. J. C., Boer J. M., Beverloo H. B., Sleight B., Chen Y., Vormoor-Burger B., Rives S., Bielorai B., Rossig C., Petit A., Rizzari C., Engstler G., Stary J., Bautista Sirvent F. J., Chen-Santel C., Bruno B., Bertrand Y., Rialland F., Plat G., Reinhardt D., Vinti L., Von Stackelberg A., Locatelli F., Zwaan C. M., Pennesi, E, Michels, N, Brivio, E, van der Velden, V, Jiang, Y, Thano, A, Ammerlaan, A, Boer, J, Beverloo, H, Sleight, B, Chen, Y, Vormoor-Burger, B, Rives, S, Bielorai, B, Rossig, C, Petit, A, Rizzari, C, Engstler, G, Stary, J, Bautista Sirvent, F, Chen-Santel, C, Bruno, B, Bertrand, Y, Rialland, F, Plat, G, Reinhardt, D, Vinti, L, Von Stackelberg, A, Locatelli, F, Zwaan, C, Pennesi E., Michels N., Brivio E., van der Velden V. H. J., Jiang Y., Thano A., Ammerlaan A. J. C., Boer J. M., Beverloo H. B., Sleight B., Chen Y., Vormoor-Burger B., Rives S., Bielorai B., Rossig C., Petit A., Rizzari C., Engstler G., Stary J., Bautista Sirvent F. J., Chen-Santel C., Bruno B., Bertrand Y., Rialland F., Plat G., Reinhardt D., Vinti L., Von Stackelberg A., Locatelli F., and Zwaan C. M.

Abstract

Inotuzumab Ozogamicin is a CD22-directed antibody conjugated to calicheamicin, approved in adults with relapsed or refractory (R/R) B cell acute lymphoblastic leukemia (BCP-ALL). Patients aged 1–18 years, with R/R CD22 + BCP-ALL were treated at the RP2D of 1.8 mg/m2. Using a single-stage design, with an overall response rate (ORR) ≤ 30% defined as not promissing and ORR > 55% as expected, 25 patients needed to be recruited to achieve 80% power at 0.05 significance level. Thirty-two patients were enrolled, 28 were treated, 27 were evaluable for response. The estimated ORR was 81.5% (95%CI: 61.9–93.7%), and 81.8% (18/22) of the responding subjects were minimal residual disease (MRD) negative. The study met its primary endpoint. Median follow up of survivors was 16 months (IQR: 14.49–20.07). One year Event Free Survival was 36.7% (95% CI: 22.2–60.4%), and Overall Survival was 55.1% (95% CI: 39.1−77.7%). Eighteen patients received consolidation (with HSCT and/or CAR T-cells therapy). Sinusoidal obstructive syndrome (SOS) occurred in seven patients. MRD negativity seemed correlated to calicheamicin sensitivity in vitro, but not to CD22 surface expression, saturation, or internalization. InO was effective in this population. The most relevant risk was the occurrence of SOS, particularly when InO treatment was followed by HSCT.

Published

2022

4. Improved survival and MRD remission with blinatumomab vs. chemotherapy in children with first high-risk relapse B-ALL

Author

Locatelli, Franco, Zugmaier, G., Rizzari, C., Morris, J. D., Gruhn, B., Klingebiel, T., Parasole, R., Linderkamp, C., Flotho, C., Petit, A., Micalizzi, C., Zeng, Y., Desai, R., Kormany, W. N., Eckert, C., Moricke, A., Sartor, M., Hrusak, O., Peters, C., Saha, V., Vinti, L., von Stackelberg, A., Locatelli F. (ORCID:0000-0002-7976-3654), Locatelli, Franco, Zugmaier, G., Rizzari, C., Morris, J. D., Gruhn, B., Klingebiel, T., Parasole, R., Linderkamp, C., Flotho, C., Petit, A., Micalizzi, C., Zeng, Y., Desai, R., Kormany, W. N., Eckert, C., Moricke, A., Sartor, M., Hrusak, O., Peters, C., Saha, V., Vinti, L., von Stackelberg, A., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

NO ABSTRACT

Published

2023

5. Impact of Pregnancy on Weight Loss After Endoscopic Sleeve Gastroplasty

Author

Carlino, Giorgio, Benson, A. A., Bove, Vincenzo, Pontecorvi, Valerio, De Siena, Martina, Matteo, Maria Valeria, Farina, A., Polidori, G., Vinti, L., Giannetti, Giulia, Costamagna, Guido, Spada, Cristiano, Boskoski, Ivo, Carlino G., Bove V., Pontecorvi V., De Siena M., Matteo M. V., Giannetti G., Costamagna G. (ORCID:0000-0002-8100-2731), Spada C. (ORCID:0000-0002-5692-0960), Boskoski I. (ORCID:0000-0001-8194-2670), Carlino, Giorgio, Benson, A. A., Bove, Vincenzo, Pontecorvi, Valerio, De Siena, Martina, Matteo, Maria Valeria, Farina, A., Polidori, G., Vinti, L., Giannetti, Giulia, Costamagna, Guido, Spada, Cristiano, Boskoski, Ivo, Carlino G., Bove V., Pontecorvi V., De Siena M., Matteo M. V., Giannetti G., Costamagna G. (ORCID:0000-0002-8100-2731), Spada C. (ORCID:0000-0002-5692-0960), and Boskoski I. (ORCID:0000-0001-8194-2670)

Abstract

Purpose: Obesity and pregnancy are strictly related: on the one hand, obesity—one of the most common comorbidities in women of reproductive age—contributes to infertility and obesity-related pregnancy complications, whereas pregnancy is a condition in which, physiologically, the pregnant woman undergoes weight gain. Endoscopic sleeve gastroplasty (ESG) may be used for the treatment of obesity in women of childbearing age. Materials and Methods: A retrospective analysis was conducted to evaluate weight trajectories, the evolution of obesity-related comorbidities, and lifestyle modification in women who became pregnant after ESG. A comparison was made between childbearing-age women who became pregnant after ESG and non-pregnant women. Results: A total of 150 childbearing-age women underwent ESG at a large tertiary medical center. Of these, 11 patients (33.4 ± 6.2 years) became pregnant after the procedure, following a mean time interval of 5.5 ± 3.9 months. Three women (two affected by polycystic ovary syndrome) reported difficulty getting pregnant before undergoing ESG. The mean preconception BMI was 31.9±4.0 kg/m2 (−7.24 ± 4.0 kg/m2 after ESG). Total body weight loss (TBWL, %) was 18.08 ± 8.00, 11.00 ± 11.08, and 12.08 ± 8.49, at the beginning of pregnancy, at the delivery, and at the first follow-up (19.6 ± 7.8 months after ESG). TBWL of at least 5% was achieved before pregnancy in all patients (73% reached a TBWL ≥ 10%). No significant differences in weight loss and QoL were found between the pregnancy and non-pregnancy groups up to 24 months after ESG. Conclusions: Endoscopic sleeve gastroplasty allows for adequate weight loss before and after pregnancy in patients with obesity. Graphical Abstract: [Figure not available: see fulltext.]

Published

2023

6. Achievement of operational tolerance in a pediatric liver transplant recipient following successful hematopoietic stem cell transplantation from a different donor

Author

Algeri, M., Velardi, E., Spada, M., Galaverna, F., Carta, R., Vinti, L., Palumbo, G., Gaspari, S., Pietrobattista, A., Boccieri, E., Becilli, M., Francalanci, P., Bertaina, V., Merli, P., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Algeri, M., Velardi, E., Spada, M., Galaverna, F., Carta, R., Vinti, L., Palumbo, G., Gaspari, S., Pietrobattista, A., Boccieri, E., Becilli, M., Francalanci, P., Bertaina, V., Merli, P., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Hematopoietic stem cell transplantation (HSCT)–based approaches are increasingly investigated strategies to induce tolerance in recipients of solid allografts. However, in the majority of cases, these approaches rely on the infusion of hematopoietic stem cells recovered from the same solid organ donor. In this report, we describe the case of a boy who received liver transplantation from a deceased donor, who had successfully underwent allogeneic HSCT from an unrelated donor for hepatitis-associated aplastic anemia. In this patient, it was possible to permanently withdraw post-HSCT immune suppression without causing any sign of liver graft dysfunction. To the best of our knowledge, this is the first case of operational tolerance documented in a patient who received combined liver transplantation and HSCT from different donors.

Published

2023

7. 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

8. Musculoskeletal manifestations of childhood cancer and differential diagnosis with juvenile idiopathic arthritis (ONCOREUM): a multicentre, cross-sectional study

Author

Civino, A, Alighieri, G, Prete, E, Caroleo, A, Magni-Manzoni, S, Vinti, L, Romano, M, Santoro, N, Filocamo, G, Belotti, T, Santarelli, F, Gorio, C, Ricci, F, Colombini, A, Pastore, S, Cesaro, S, Barone, P, Verzegnassi, F, Olivieri, A, Ficara, M, Miniaci, A, Russo, G, Gallizzi, R, Pericoli, R, Breda, L, Mura, R, Podda, R, Onofrillo, D, Lattanzi, B, Tirtei, E, Maggio, M, De Santis, R, Consolini, R, Arlotta, A, La Torre, F, Mainardi, C, Pelagatti, M, Coassin, E, Capolsini, I, Burnelli, R, Tornesello, A, Soscia, F, De Fanti, A, Rigante, D, Pizzato, C, De Fusco, C, Abate, M, Roncadori, A, Rossi, E, Stabile, G, Biondi, A, Lepore, L, Conter, V, Rondelli, R, Pession, A, Ravelli, A, Amatruda, M, Atzeni, C, Bertolini, P, Bigucci, B, Caniglia, M, Cappella, M, Cattalini, M, Cefalo, M, Cellini, M, Cortis, E, Davi, S, De Benedetti, F, Di Cataldo, A, Fabbri, E, Fagioli, F, Fontanili, I, Garaventa, A, Gicchino, M, Ladogana, S, Locatelli, F, Magnolato, A, Marsili, M, Martino, S, Mascarin, M, Messina, C, Micalizzi, C, Porta, F, Rizzari, C, Civino A., Alighieri G., Prete E., Caroleo A. M., Magni-Manzoni S., Vinti L., Romano M., Santoro N., Filocamo G., Belotti T., Santarelli F., Gorio C., Ricci F., Colombini A., Pastore S., Cesaro S., Barone P., Verzegnassi F., Olivieri A. N., Ficara M., Miniaci A., Russo G., Gallizzi R., Pericoli R., Breda L., Mura R., Podda R. A., Onofrillo D., Lattanzi B., Tirtei E., Maggio M. C., De Santis R., Consolini R., Arlotta A., La Torre F., Mainardi C., Pelagatti M. A., Coassin E., Capolsini I., Burnelli R., Tornesello A., Soscia F., De Fanti A., Rigante D., Pizzato C., De Fusco C., Abate M. E., Roncadori A., Rossi E., Stabile G., Biondi A., Lepore L., Conter V., Rondelli R., Pession A., Ravelli A., Amatruda M., Atzeni C., Bertolini P., Bigucci B., Caniglia M., Cappella M., Cattalini M., Cefalo M. G., Cellini M., Cortis E., Davi S., De Benedetti F., Di Cataldo A., Fabbri E., Fagioli F., Fontanili I., Garaventa A., Gicchino M. F., Ladogana S., Locatelli F., Magnolato A., Marsili M., Martino S., Mascarin M., Messina C., Micalizzi C., Porta F., Rizzari C., Civino, A, Alighieri, G, Prete, E, Caroleo, A, Magni-Manzoni, S, Vinti, L, Romano, M, Santoro, N, Filocamo, G, Belotti, T, Santarelli, F, Gorio, C, Ricci, F, Colombini, A, Pastore, S, Cesaro, S, Barone, P, Verzegnassi, F, Olivieri, A, Ficara, M, Miniaci, A, Russo, G, Gallizzi, R, Pericoli, R, Breda, L, Mura, R, Podda, R, Onofrillo, D, Lattanzi, B, Tirtei, E, Maggio, M, De Santis, R, Consolini, R, Arlotta, A, La Torre, F, Mainardi, C, Pelagatti, M, Coassin, E, Capolsini, I, Burnelli, R, Tornesello, A, Soscia, F, De Fanti, A, Rigante, D, Pizzato, C, De Fusco, C, Abate, M, Roncadori, A, Rossi, E, Stabile, G, Biondi, A, Lepore, L, Conter, V, Rondelli, R, Pession, A, Ravelli, A, Amatruda, M, Atzeni, C, Bertolini, P, Bigucci, B, Caniglia, M, Cappella, M, Cattalini, M, Cefalo, M, Cellini, M, Cortis, E, Davi, S, De Benedetti, F, Di Cataldo, A, Fabbri, E, Fagioli, F, Fontanili, I, Garaventa, A, Gicchino, M, Ladogana, S, Locatelli, F, Magnolato, A, Marsili, M, Martino, S, Mascarin, M, Messina, C, Micalizzi, C, Porta, F, Rizzari, C, Civino A., Alighieri G., Prete E., Caroleo A. M., Magni-Manzoni S., Vinti L., Romano M., Santoro N., Filocamo G., Belotti T., Santarelli F., Gorio C., Ricci F., Colombini A., Pastore S., Cesaro S., Barone P., Verzegnassi F., Olivieri A. N., Ficara M., Miniaci A., Russo G., Gallizzi R., Pericoli R., Breda L., Mura R., Podda R. A., Onofrillo D., Lattanzi B., Tirtei E., Maggio M. C., De Santis R., Consolini R., Arlotta A., La Torre F., Mainardi C., Pelagatti M. A., Coassin E., Capolsini I., Burnelli R., Tornesello A., Soscia F., De Fanti A., Rigante D., Pizzato C., De Fusco C., Abate M. E., Roncadori A., Rossi E., Stabile G., Biondi A., Lepore L., Conter V., Rondelli R., Pession A., Ravelli A., Amatruda M., Atzeni C., Bertolini P., Bigucci B., Caniglia M., Cappella M., Cattalini M., Cefalo M. G., Cellini M., Cortis E., Davi S., De Benedetti F., Di Cataldo A., Fabbri E., Fagioli F., Fontanili I., Garaventa A., Gicchino M. F., Ladogana S., Locatelli F., Magnolato A., Marsili M., Martino S., Mascarin M., Messina C., Micalizzi C., Porta F., and Rizzari C.

Abstract

Background: Presenting symptoms of childhood cancers might mimic those of rheumatic diseases. However, the evidence available to guide differential diagnosis remains scarce. Preventing wrong or delayed diagnosis is therefore important to avoid incorrect administration of glucocorticoid or immunosuppressive therapy and worsening of prognosis. As such, we aimed to assess the prevalence and characteristics of presenting musculoskeletal manifestations in patients at cancer onset and to identify the factors that differentiate childhood malignancies with arthropathy from juvenile idiopathic arthritis. Methods: We did a multicentre, cross-sectional study at 25 paediatric haemato-oncology centres and 22 paediatric rheumatology centres in Italy. We prospectively recruited patients who were younger than 16 years that were newly diagnosed with cancer or juvenile idiopathic arthritis. We excluded patients with glucocorticoid pre-treatment (>1 mg/kg per day of oral prednisone or equivalent for ≥2 consecutive weeks). We collected data for patients with a new diagnosis of cancer or juvenile idiopathic arthritis using an electronic case report form on a web-based platform powered by the Cineca Interuniversity Consortium. The primary outcome was to describe the frequency and characteristics of musculoskeletal manifestations at cancer onset; and the secondary outcome was to identify factors that could discriminate malignancies presenting with arthropathy, with or without other musculoskeletal symptoms, from juvenile idiopathic arthritis using multivariable logistic regression analysis. Findings: Between May 1, 2015, and May 31, 2018, 1957 patients were eligible, of which 1277 (65%) had cancer and 680 (35%) had juvenile idiopathic arthritis. Musculoskeletal symptoms occurred in 324 (25% [95% CI 23·0–27·8]) of 1277 patients with cancer, of whom 207 had arthropathy. Patients with malignant bone tumours had the highest frequency of musculoskeletal symptoms (53 [80%] of 66), followed b

Published

2021

9. Recurrent genetic fusions redefine MLL germ line acute lymphoblastic leukemia in infants

Author

Fazio, G, Bardini, M, De Lorenzo, P, Grioni, A, Quadri, M, Pedace, L, Corral Abascal, L, Palamini, S, Palmi, C, Buldini, B, Vinti, L, Parasole, R, Barisone, E, Zecca, M, Favre, C, Locatelli, F, Conter, V, Rizzari, C, Valsecchi, M, Biondi, A, Cazzaniga, G, Fazio G., Bardini M., De Lorenzo P., Grioni A., Quadri M., Pedace L., Corral Abascal L., Palamini S., Palmi C., Buldini B., Vinti L., Parasole R., Barisone E., Zecca M., Favre C., Locatelli F., Conter V., Rizzari C., Valsecchi M. G., Biondi A., Cazzaniga G., Fazio, G, Bardini, M, De Lorenzo, P, Grioni, A, Quadri, M, Pedace, L, Corral Abascal, L, Palamini, S, Palmi, C, Buldini, B, Vinti, L, Parasole, R, Barisone, E, Zecca, M, Favre, C, Locatelli, F, Conter, V, Rizzari, C, Valsecchi, M, Biondi, A, Cazzaniga, G, Fazio G., Bardini M., De Lorenzo P., Grioni A., Quadri M., Pedace L., Corral Abascal L., Palamini S., Palmi C., Buldini B., Vinti L., Parasole R., Barisone E., Zecca M., Favre C., Locatelli F., Conter V., Rizzari C., Valsecchi M. G., Biondi A., and Cazzaniga G.

Abstract

B-cell precursor (BCP) acute lymphoblastic leukemia (BCP-ALL) in infants (ie, children age <1 year) is a rare disease traditionally subdivided into MLL-rearranged (alias KMT2A; MLL-R) and MLL germ line (MLL-G) subtypes. MLL gene rearrangements occur in ∼75% of infants with BCP-ALL1-3 and are typically associated with a mixed-lineage phenotype.4 MLL rearrangements originate prenatally in utero5 and play a role in transcription factor dysregulation.6 MLL-R BCP-ALL in infants is associated with dismal outcomes.1-3 Infants with MLL-G ALL treated with intensive therapies in the Interfant-06 protocol may have a relatively favorable prognosis, with a 6-year event-free survival (EFS) rate of 73.9%,2 slightly inferior to that observed in older children with BCP-ALL.1,2 Of interest, a recent study from the Japanese Pediatric Leukemia/Lymphoma Study Group MLL-10 trial reported more favorable outcomes in infants

Published

2021

10. P359: IMPROVED OVERALL SURVIVAL AND MRD CLEARANCE WITH BLINATUMOMAB VS CHEMOTHERAPY AS PRE-TRANSPLANT CONSOLIDATION IN PEDIATRIC HIGH-RISK FIRST-RELAPSE B-CELL PRECURSOR ACUTE LYMPHOBLASTIC LEUKEMIA (B-ALL)

Author

Locatelli, F., primary, Zugmaier, G., additional, Rizzari, C., additional, Morris, J., additional, Gruhn, B., additional, Klingebiel, T., additional, Parasole, R., additional, Linderkamp, C., additional, Flotho, C., additional, Petit, A., additional, Micalizzi, C., additional, Zeng, Y., additional, Desai, R., additional, Kormany, W., additional, Eckert, C., additional, Möricke, A., additional, Sartor, M., additional, Hrusak, O., additional, Peters, C., additional, Saha, V., additional, Vinti, L., additional, and von Stackelberg, A., additional

Published

2022

11. S204: PEMBROLIZUMAB IN CHILDREN AND YOUNG ADULTS WITH NEWLY DIAGNOSED CLASSICAL HODGKIN LYMPHOMA WITH SLOW EARLY RESPONSE TO FRONTLINE CHEMOTHERAPY: THE PHASE 2, OPEN-LABEL, KEYNOTE-667 STUDY

Author

Vinti, L., primary, Daw, S., additional, Sabado Alvarez, C., additional, Fagioli, F., additional, Beishuizen, A., additional, Michel, G., additional, Moleti, M. L., additional, Cepelova, M., additional, Thorwarth, A., additional, Rigaud, C., additional, Plaza Lopez de Sabando, D., additional, Landman Parker, J., additional, Zhu, Y., additional, Pillai, P., additional, Nahar, A., additional, and Mauz-Koerholz, C., additional

Published

2022

12. P521: TREATMENT OF BLASTIC PLASMACYTOID DENDRITIC CELL NEOPLASM IN PEDIATRIC PATIENTS WITH TAGRAXOFUSP, A CD123-TARGETED THERAPY

Author

Pemmaraju, N., primary, Cuglievan, B., additional, Lasky, J., additional, Kheradpour, A., additional, Hijiya, N., additional, Stein, A. S., additional, Meshinchi, S., additional, Mullen, C., additional, Angelucci, E., additional, Vinti, L., additional, Mughal, T. I., additional, and Pawlowska, A., additional

Published

2022

13. 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

14. Inotuzumab ozogamicin as single agent in pediatric patients with relapsed and refractory acute lymphoblastic leukemia: results from a phase II trial

Author

Pennesi, E., Michels, N., Brivio, E., van der Velden, V. H. J., Jiang, Y., Thano, A., Ammerlaan, A. J. C., Boer, J. M., Beverloo, H. B., Sleight, B., Chen, Y., Vormoor-Burger, B., Rives, S., Bielorai, B., Rossig, C., Petit, A., Rizzari, C., Engstler, G., Stary, J., Bautista Sirvent, F. J., Chen-Santel, C., Bruno, B., Bertrand, Y., Rialland, F., Plat, G., Reinhardt, D., Vinti, L., Von Stackelberg, A., Locatelli, Franco, Zwaan, C. M., Locatelli F. (ORCID:0000-0002-7976-3654), Pennesi, E., Michels, N., Brivio, E., van der Velden, V. H. J., Jiang, Y., Thano, A., Ammerlaan, A. J. C., Boer, J. M., Beverloo, H. B., Sleight, B., Chen, Y., Vormoor-Burger, B., Rives, S., Bielorai, B., Rossig, C., Petit, A., Rizzari, C., Engstler, G., Stary, J., Bautista Sirvent, F. J., Chen-Santel, C., Bruno, B., Bertrand, Y., Rialland, F., Plat, G., Reinhardt, D., Vinti, L., Von Stackelberg, A., Locatelli, Franco, Zwaan, C. M., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Inotuzumab Ozogamicin is a CD22-directed antibody conjugated to calicheamicin, approved in adults with relapsed or refractory (R/R) B cell acute lymphoblastic leukemia (BCP-ALL). Patients aged 1–18 years, with R/R CD22 + BCP-ALL were treated at the RP2D of 1.8 mg/m2. Using a single-stage design, with an overall response rate (ORR) ≤ 30% defined as not promissing and ORR > 55% as expected, 25 patients needed to be recruited to achieve 80% power at 0.05 significance level. Thirty-two patients were enrolled, 28 were treated, 27 were evaluable for response. The estimated ORR was 81.5% (95%CI: 61.9–93.7%), and 81.8% (18/22) of the responding subjects were minimal residual disease (MRD) negative. The study met its primary endpoint. Median follow up of survivors was 16 months (IQR: 14.49–20.07). One year Event Free Survival was 36.7% (95% CI: 22.2–60.4%), and Overall Survival was 55.1% (95% CI: 39.1−77.7%). Eighteen patients received consolidation (with HSCT and/or CAR T-cells therapy). Sinusoidal obstructive syndrome (SOS) occurred in seven patients. MRD negativity seemed correlated to calicheamicin sensitivity in vitro, but not to CD22 surface expression, saturation, or internalization. InO was effective in this population. The most relevant risk was the occurrence of SOS, particularly when InO treatment was followed by HSCT.

Published

2022

15. PACSIN2 rs2413739 influence on thiopurine pharmacokinetics: validation studies in pediatric patients

Author

Franca, R, Stocco, G, Favretto, D, Giurici, N, del Rizzo, I, Locatelli, F, Vinti, L, Biondi, A, Colombini, A, Fagioli, F, Barisone, E, Pelin, M, Martellossi, S, Ventura, A, Decorti, G, Rabusin, M, Franca R., Stocco G., Favretto D., Giurici N., del Rizzo I., Locatelli F., Vinti L., Biondi A., Colombini A., Fagioli F., Barisone E., Pelin M., Martellossi S., Ventura A., Decorti G., Rabusin M., Franca, R, Stocco, G, Favretto, D, Giurici, N, del Rizzo, I, Locatelli, F, Vinti, L, Biondi, A, Colombini, A, Fagioli, F, Barisone, E, Pelin, M, Martellossi, S, Ventura, A, Decorti, G, Rabusin, M, Franca R., Stocco G., Favretto D., Giurici N., del Rizzo I., Locatelli F., Vinti L., Biondi A., Colombini A., Fagioli F., Barisone E., Pelin M., Martellossi S., Ventura A., Decorti G., and Rabusin M.

Abstract

The aim of the study was to validate the impact of the single-nucleotide polymorphism rs2413739 (T > C) in the PACSIN2 gene on thiopurines pharmacological parameters and clinical response in an Italian cohort of pediatric patients with acute lymphoblastic leukemia (ALL) and inflammatory bowel disease (IBD). In ALL, PACSIN2 rs2413739 T allele was associated with a significant reduction of TPMT activity in erythrocytes (p = 0.0094, linear mixed-effect model, multivariate analysis considering TPMT genotype) and increased severe gastrointestinal toxicity during consolidation therapy (p = 0.049). A similar trend was present also for severe hematological toxicity during maintenance. In IBD, no significant effect of rs2413739 could be found on TPMT activity, however azathioprine effectiveness was reduced in patients carrying the T allele (linear mixed effect, p = 0.0058). In PBMC from healthy donors, a positive correlation between PACSIN2 and TPMT protein concentration could be detected (linear mixed effect, p = 0.045). These results support the role of PACSIN2 polymorphism on TPMT activity and mercaptopurine adverse effects in patients with ALL. Further evidence on PBMC and pediatric patients with IBD supports an association between PACSIN2 variants, TPMT activity, and thiopurines effects, even if more studies are needed since some of these effects may be tissue specific.

Published

2020

16. 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

17. A phase 1 study of inotuzumab ozogamicin in pediatric relapsed/refractory acute lymphoblastic leukemia (ITCC-059 study)

Author

Brivio, E., Locatelli, Franco, Lopez-Yurda, M., Malone, A., Diaz-de-Heredia, C., Bielorai, B., Rossig, C., van der Velden, V. H. J., Ammerlaan, A. C. J., Thano, A., van der Sluis, I. M., den Boer, M. L., Chen, Y., Sleight, B., Brethon, B., Nysom, K., Sramkova, L., Ora, I., Vinti, L., Chen-Santel, C., Zwaan, C. M., Locatelli F. (ORCID:0000-0002-7976-3654), Brivio, E., Locatelli, Franco, Lopez-Yurda, M., Malone, A., Diaz-de-Heredia, C., Bielorai, B., Rossig, C., van der Velden, V. H. J., Ammerlaan, A. C. J., Thano, A., van der Sluis, I. M., den Boer, M. L., Chen, Y., Sleight, B., Brethon, B., Nysom, K., Sramkova, L., Ora, I., Vinti, L., Chen-Santel, C., Zwaan, C. M., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

This phase 1 study investigated the recommended phase 2 dose (RP2D) of inotuzumab ozogamicin (InO), a CD22-directed antibody-drug conjugate, in pediatric patients with multiple relapsed/refractory (R/R) CD22+ acute lymphoblastic leukemia (ALL). Patients (age ≥1 year or <18 years) received 3 doses of InO (days 1, 8, and 15) per course. Dose escalation was based on dose-limiting toxicities (DLTs) during course 1. Dose level 1 (DL1) was 1.4 mg/m2 (0.6, 0.4, 0.4 mg/m2) and DL2 was 1.8 mg/m2 (0.8, 0.5, 0.5 mg/m2). Secondary end points included safety, antileukemic activity, and pharmacokinetics. Twenty-five patients (23 evaluable for DLTs) were enrolled. In course 1, the first cohort had 1 of 6 (DL1) and 2 of 5 (DL2) patients who experienced DLTs; subsequent review considered DL2 DLTs to be non–dose-limiting. Dose was de-escalated to DL1 while awaiting protocol amendment to re-evaluate DL2 in a second cohort, in which 0 of 6 (DL1) and 1 of 6 (DL2) patients had a DLT. Twenty-three patients experienced grade 3 to 4 adverse events; hepatic sinusoidal obstruction syndrome was reported in 2 patients after subsequent chemotherapy. Overall response rate after course 1 was 80% (95% confidence interval [CI], 59% to 93%) (20 of 25 patients; DL1: 75% [95% CI, 43% to 95%], DL2: 85% [95% CI, 55% to 98%]). Of the responders, 84% (95% CI, 60% to 97%) achieved minimal residual disease (MRD)-negative complete response, and 12-month overall survival was 40% (95% CI, 25% to 66%). Nine patients received hematopoietic stem cell transplantation or chimeric antigen receptor T cells after InO. InO median maximum concentrations were comparable to simulated adult concentrations. InO was well tolerated, demonstrating antileukemic activity in heavily pretreated children with CD22+ R/R ALL. RP2D was established as 1.8 mg/m2 per course, as in adults. This trial was registered at https://www.clinicaltrialsregister.eu as EUDRA-CT 2016-000227-71. Key Points: • The recommended phase 2 dose of InO for

Published

2021

18. Recurrent genetic fusions redefine MLL germ line acute lymphoblastic leukemia in infants

Author

Fazio, G., Bardini, M., De Lorenzo, P., Grioni, A., Quadri, M., Pedace, L., Corral Abascal, L., Palamini, S., Palmi, C., Buldini, B., Vinti, L., Parasole, R., Barisone, E., Zecca, M., Favre, C., Locatelli, Franco, Conter, V., Rizzari, C., Valsecchi, M. G., Biondi, A., Cazzaniga, G., Locatelli F. (ORCID:0000-0002-7976-3654), Fazio, G., Bardini, M., De Lorenzo, P., Grioni, A., Quadri, M., Pedace, L., Corral Abascal, L., Palamini, S., Palmi, C., Buldini, B., Vinti, L., Parasole, R., Barisone, E., Zecca, M., Favre, C., Locatelli, Franco, Conter, V., Rizzari, C., Valsecchi, M. G., Biondi, A., Cazzaniga, G., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

NO ABSTRACT

Published

2021

19. PACSIN2 rs2413739 influence on thiopurine pharmacokinetics: validation studies in pediatric patients

Author

Franca, R., Stocco, G., Favretto, D., Giurici, N., del Rizzo, I., Locatelli, Franco, Vinti, L., Biondi, A., Colombini, A., Fagioli, F., Barisone, E., Pelin, M., Martellossi, S., Ventura, A., Decorti, G., Rabusin, M., Locatelli F. (ORCID:0000-0002-7976-3654), Franca, R., Stocco, G., Favretto, D., Giurici, N., del Rizzo, I., Locatelli, Franco, Vinti, L., Biondi, A., Colombini, A., Fagioli, F., Barisone, E., Pelin, M., Martellossi, S., Ventura, A., Decorti, G., Rabusin, M., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

The aim of the study was to validate the impact of the single-nucleotide polymorphism rs2413739 (T > C) in the PACSIN2 gene on thiopurines pharmacological parameters and clinical response in an Italian cohort of pediatric patients with acute lymphoblastic leukemia (ALL) and inflammatory bowel disease (IBD). In ALL, PACSIN2 rs2413739 T allele was associated with a significant reduction of TPMT activity in erythrocytes (p = 0.0094, linear mixed-effect model, multivariate analysis considering TPMT genotype) and increased severe gastrointestinal toxicity during consolidation therapy (p = 0.049). A similar trend was present also for severe hematological toxicity during maintenance. In IBD, no significant effect of rs2413739 could be found on TPMT activity, however azathioprine effectiveness was reduced in patients carrying the T allele (linear mixed effect, p = 0.0058). In PBMC from healthy donors, a positive correlation between PACSIN2 and TPMT protein concentration could be detected (linear mixed effect, p = 0.045). These results support the role of PACSIN2 polymorphism on TPMT activity and mercaptopurine adverse effects in patients with ALL. Further evidence on PBMC and pediatric patients with IBD supports an association between PACSIN2 variants, TPMT activity, and thiopurines effects, even if more studies are needed since some of these effects may be tissue specific.

Published

2020

20. Blinatumomab versus historical standard therapy in pediatric patients with relapsed/refractory Ph-negative B-cell precursor acute lymphoblastic leukemia

Author

Locatelli, Franco, Whitlock, J. A., Peters, C., Chen-Santel, C., Chia, V., Dennis, R. M., Heym, K. M., Katz, A. J., Kelsh, M. A., Sposto, R., Tu, H., Tuglus, C. A., Verma, A., Vinti, L., Wilkes, J. J., Zubarovskaja, N., Zugmaier, G., von Stackelberg, A., Sun, W., Locatelli F. (ORCID:0000-0002-7976-3654), Locatelli, Franco, Whitlock, J. A., Peters, C., Chen-Santel, C., Chia, V., Dennis, R. M., Heym, K. M., Katz, A. J., Kelsh, M. A., Sposto, R., Tu, H., Tuglus, C. A., Verma, A., Vinti, L., Wilkes, J. J., Zubarovskaja, N., Zugmaier, G., von Stackelberg, A., Sun, W., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

NO ABSTRACT

Published

2020

21. 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

22. Repurposing anthelmintic agents to eradicate resistant leukemia

Author

Mezzatesta, C., Abduli, L., Guinot, A., Eckert, C., Schewe, D., Zaliova, M., Vinti, L., Marovca, B., Tsai, Y. -C., Jenni, S., Aguade-Gorgorio, J., von Stackelberg, A., Schrappe, M., Locatelli, Franco, Stanulla, M., Cario, G., Bourquin, J. -P., Bornhauser, B. C., Locatelli F. (ORCID:0000-0002-7976-3654), Mezzatesta, C., Abduli, L., Guinot, A., Eckert, C., Schewe, D., Zaliova, M., Vinti, L., Marovca, B., Tsai, Y. -C., Jenni, S., Aguade-Gorgorio, J., von Stackelberg, A., Schrappe, M., Locatelli, Franco, Stanulla, M., Cario, G., Bourquin, J. -P., Bornhauser, B. C., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Despite rapid progress in genomic profiling in acute lymphoblastic leukemia (ALL), identification of actionable targets and prediction of response to drugs remains challenging. To identify specific vulnerabilities in ALL, we performed a drug screen using primary human ALL samples cultured in a model of the bone marrow microenvironment combined with high content image analysis. Among the 2487 FDA-approved compounds tested, anthelmintic agents of the class of macrocyclic lactones exhibited potent anti-leukemia activity, similar to the already known anti-leukemia agents currently used in induction chemotherapy. Ex vivo validation in 55 primary ALL samples of both precursor B cell and T-ALL including refractory relapse cases confirmed strong anti-leukemia activity with IC50 values in the low micromolar range. Anthelmintic agents increased intracellular chloride levels in primary leukemia cells, inducing mitochondrial outer membrane depolarization and cell death. Supporting the notion that simultaneously targeting cell death machineries at different angles may enhance the cell death response, combination of anthelmintic agents with the BCL-2 antagonist navitoclax or with the chemotherapeutic agent dexamethasone showed synergistic activity in primary ALL. These data reveal anti-leukemia activity of anthelmintic agents and support exploiting drug repurposing strategies to identify so far unrecognized anti-cancer agents with potential to eradicate even refractory leukemia.

Published

2020

23. 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

24. PS952 NELARABINE AS SALVAGE THERAPY FOR PEDIATRIC PATIENTS WITH RELAPSED T-ALL

Author

Vinti, L., primary, Strocchio, L., additional, Girardi, K., additional, Antonetti, L., additional, and Locatelli, F., additional

Published

2019

25. 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

26. Durable remissions in TCF3-HLF positive acute lymphoblastic leukemia with blinatumomab and stem cell transplantation

Author

Mouttet, B., Vinti, L., Ancliff, P., Bodmer, N., Brethon, B., Cario, G., Chen-Santel, C., Elitzur, S., Hazar, V., Kunz, J., Moricke, A., Stein, J., Vora, A., Yaman, Y., Schrappe, M., Anak, S., Baruchel, A., Locatelli, Franco, Stackelberg, A. V., Stanulla, M., Bourquin, J. -P., Locatelli F. (ORCID:0000-0002-7976-3654), Mouttet, B., Vinti, L., Ancliff, P., Bodmer, N., Brethon, B., Cario, G., Chen-Santel, C., Elitzur, S., Hazar, V., Kunz, J., Moricke, A., Stein, J., Vora, A., Yaman, Y., Schrappe, M., Anak, S., Baruchel, A., Locatelli, Franco, Stackelberg, A. V., Stanulla, M., Bourquin, J. -P., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

no abstract

Published

2019

27. Applicazione dell’international pediatric Non Hodgkin Lymphoma staging system (IPNHLSS) ai pazienti pediatrici con nuova diagnosi di linfoma non Hodgkin (LNH) Barruolati nel protocollo AIEOP-LNH-97

Author

Onofrillo, D., Pascale, S., Carraro, E., Massano, D., Mussolin, L., Mura, R., Vinti, L., Buffardi, S., Farruggia, P., Cesaro, S., Zecca, M., Bertolini, P., Piglione, M., Tondo, A., Santoro, N., Garaventa, A., Lo-Nigro, L., and M. Pillon.

Subjects

pediatria, LNH, LNH, score prognostico, pediatria, score prognostico

Published

2018

28. Complicanze infettive gravi nei pazienti affetti da leucemia linfoblastica acuta (LLA) arruolati nel protocollo AIEOP-BFM ALL 2009: incidenza ed esito. Hematology Reports 2018; 10 (s1): 67

Author

Colombini, A., Brivio, E., Barisone, E., Barone, A., Cellini, M., Kiren, V., La-Spina, M., Mina, T., Muggeo, P., Mura, R., Parasole, R., Putti, M. C., Rizzari, C., Silvestri, D., Vinti, L., Conter, V., and Cesaro, S.

Subjects

leucemia linfoblastica acuta, pediatria, infezioni batteriche, leucemia linfoblastica acuta, pediatria, infezioni batteriche

Published

2018

29. Incidenza delle infezioni fungine e sopravvivenza nei pazienti aieop trattati per leucemia linfoblastica acuta nel protocollo AIEOP-BFM ALL 2009

Author

Cesaro, S., Barisone, E., Colombini, A., Putti, M. C., Vinti, L., Parasole, R., La-Spina, M., Muggeo, P., Mina, T., Mura, R., Kiren, V., Barone, A., Silvestri, D., and V. Conter.

Subjects

leucemia linfoblastica acuta, pediatria, infezioni fungine, infezioni fungine, leucemia linfoblastica acuta, pediatria

Published

2018

30. Bone marrow failure may be caused by chromosome anomalies exerting effects on RUNX1T1 gene

Author

Valli, R., Vinti, L., Frattini, A., Fabbri, M., Montalbano, G., Olivieri, C., Minelli, A., Locatelli, Franco, Pasquali, F., Maserati, E., Locatelli F. (ORCID:0000-0002-7976-3654), Valli, R., Vinti, L., Frattini, A., Fabbri, M., Montalbano, G., Olivieri, C., Minelli, A., Locatelli, Franco, Pasquali, F., Maserati, E., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Background: The majority of the cases of bone marrow failure syndromes/aplastic anaemias (BMFS/AA) are non-hereditary and considered idiopathic (80-85%). The peripheral blood picture is variable, with anaemia, neutropenia and/or thrombocytopenia, and the patients with idiopathic BMFS/AA may have a risk of transformation into a myelodysplastic syndrome (MDS) and/or an acute myeloid leukaemia (AML), as ascertained for all inherited BMFS. We already reported four patients with different forms of BMFS/AA with chromosome anomalies as primary etiologic event: the chromosome changes exerted an effect on specific genes, namely RUNX1, MPL, and FLI1, leading to the disease. Results: We report two further patients with non-hereditary BM failure, with diagnosis of severe aplastic anaemia and pancytopenia caused by two different constitutional structural anomalies involving chromosome 8, and possibly leading to the disorder due to effects on the RUNX1T1 gene, which was hypo-expressed and hyper-expressed, respectively, in the two patients. The chromosome change was unbalanced in one patient, and balanced in the other one. Conclusions: We analyzed the sequence of events in the pathogenesis of the disease in the two patients, including a number of non-haematological signs present in the one with the unbalanced anomaly. We demonstrated that in these two patients the primary event causing BMFS/AA was the constitutional chromosome anomaly. If we take into account the cohort of 219 patients with a similar diagnosis in whom we made cytogenetic studies in the years 2003-2017, we conclude that cytogenetic investigations were instrumental to reach a diagnosis in 52 of them. We postulate that a chromosome change is the primary cause of BMFS/AA in a not negligible proportion of cases, as it was ascertained in 6 of these patients.

Published

2018

31. Rischio di recidiva nel linfoma di Hodgkin pediatrico: dalla esperienza AIEOP ad una strategia europea

Author

Mascarin, M., Bernasconi, S., Bertolini, P., Bianchi, M., Buffardi, S., Casale, F., Casini, T., Cellini, M., Cesaro, S., Civino, A., Consarino, C., Cosmi, C., D’Amico, S., De Santis, R., Facchini, E., Fagioli, F., Farruggia, P., Favre, C., Felici, L., Galimberti, D., Garaventa, A., Iaria, G., Indolfi, P., Locatelli, F., Moleti, M. L., Muggeo, P., Mura, R. M., Pericoli, R., Perruccio, K., Pierani, P., Pillon, M., Porta, F., Provenzi, M., Rinieri, S., Rondelli, R., Russo, G., Sala, A., Santoro, N., Sau, A., Sperli, D., Todesco, A., Tolva, A., Varasso, G., Verzegnassi, F., Vinti, L., Zecca, M., Lopci, E., Elia, C., Birri, S., Sabattini, E., D’Amore, E., and Burnelli, R.

Subjects

pediatria, linfoma hodgkin, risultati, linfoma hodgkin, pediatria, risultati

Published

2017

32. Bone marrow failure may be caused by chromosome anomalies exerting effects on RUNX1T1 gene

Author

Valli, R., primary, Vinti, L., additional, Frattini, A., additional, Fabbri, M., additional, Montalbano, G., additional, Olivieri, C., additional, Minelli, A., additional, Locatelli, F., additional, Pasquali, F., additional, and Maserati, E., additional

Published

2018

33. Infezioni Clinicamente rilevanti durante la terapia di induzione sono associate con un aumento del rischio di recidiva. Studio di 1999 pazienti arruolati nel protocollo AIEOP-LLA-2000

Author

Caselli, D., Colombini, A., Silvestri, D., Vinti, L., Parasole, R., Putti, M. C., Barisone, E., Lo Nigro, L., Santoro, N., Ziino, O., Decembrino, N., Castagnola, E., Cesaro, Simone, Aricò, M., and Conter, V. .

Subjects

leucemia linfoblastica acuta, chemioterapia, Infezioni, Infezioni, chemioterapia, leucemia linfoblastica acuta

Published

2016

34. Studio Multicentrico prospettico osserva zionale sui sintomi muscolo scheletrici all’esordio in oncologia pediatrica e i fattori predittivi nella diagnosi differenziale con l’atrite idiopatica giovanile. Analisi preliminare

Author

Civino, A., Alighieri, G., Davi, S., Pession, A., Ravelli, A., Santoro, N., Belotti, T, Martino, S., Cesaro, Simone, Filocamo, G., Marino, S., Magnolato, A., Colombini, A., Ricci, F., Suffia, C., Galizzi, R., Palmisani, E., Verzegnassi, F., Olivieri, A. N., Tirtei, E., Gerloni, V, Gorio, C., Lattanzi, B., Pizzati, C., Soscia, F., Vinti, L., De Fanti, A., Ficara, M., Magni Manzoni, S., Boaro, M. P., Prete, E., Quartulli, L., La Torre, F., Onofrillo, D., Rigante, D., Capolsini, I., Maggio, C., Ladogana, S., Marsali, M., Burnelli, R., Coassin, E., Pelegatti, M. A., Arlotta, A., Lepore, L., Conter, V., Biondi, A., Fagioli, F., and Rondelli, R.

Subjects

diagnosi, leucemia acuta, sintomi, diagnosi, sintomi, leucemia acuta

Published

2016

35. Report sulle modalità organizzative e sugli effetti della somministrazione in regime di Day-Hospital della ciclofosfamide (1 gr/mq) effettuata in 11 centri AIEOP-BFM ALL 2009

Author

Bettini, L., Colombini, A., Spinelli, M., Silvestri, D., Cannata, E., Casini, T., Cesaro, Simone, Giagnuolo, G., Mohamed, S., Melchionda, F., Mosa, C., Pierri, F., Varotto, E., Vinti, L., Conter, V., and Rizzari, C.

Subjects

terapia ambulatoriale, ciclofosfamide, leucemia acuta, terapia ambulatoriale, leucemia acuta, ciclofosfamide

Published

2016

36. The combination of bortezomib with chemotherapy to treat relapsed/refractory acute lymphoblastic leukaemia of childhood

Author

Bertaina, A., Vinti, L., Strocchio, L., Gaspari, S., Caruso, R., Algeri, M., Coletti, V., Gurnari, C., Romano, M., Cefalo, M. G., Girardi, K., Trevisan, V., Bertaina, V., Merli, P., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Bertaina, A., Vinti, L., Strocchio, L., Gaspari, S., Caruso, R., Algeri, M., Coletti, V., Gurnari, C., Romano, M., Cefalo, M. G., Girardi, K., Trevisan, V., Bertaina, V., Merli, P., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Achieving complete remission (CR) in childhood relapsed/refractory acute lymphoblastic leukaemia (ALL) is a difficult task. Bortezomib, a proteasome inhibitor, has in vitro activity against ALL blasts. A phase I-II trial, reported by the Therapeutic Advances in Childhood Leukaemia and Lymphoma (TACL) consortium, demonstrated that bortezomib with chemotherapy has acceptable toxicity and remarkable activity in patients with relapsed ALL failing 2–3 previous regimens. We evaluated bortezomib in combination with chemotherapy in 30 and 7 children with B-cell precursor (BCP) and T-cell ALL, respectively. Bortezomib (1·3 mg/m2/dose) was administered intravenously on days 1, 4, 8, and 11. Chemotherapy agents were the same as those used in the TACL trial, consisting of dexamethasone, doxorubicin, vincristine and pegylated asparaginase. Three patients (8·1%) died due to infections. Twenty-seven patients (72·9%) achieved CR or CR with incomplete platelet recovery (CRp). Fourteen had minimal residual disease (MRD) lower than 0·1%. Twenty-two of 30 BCP-ALL patients (73·3%) and 5/7 patients (71%) with T-cell ALL achieved CR/CRp. The 2-year overall survival (OS) is 31·3%; CR/CRp patients with an MRD response had a remarkable 2-year OS of 68·4%. These data confirm that the combination of bortezomib with chemotherapy is a suitable/effective option for childhood relapsed/refractory ALL.

Published

2017

37. Protocol II vs protocol III given twice during reinduction therapy in children with medium-risk ALL

Author

Locatelli, Franco, Valsecchi, M. G., Moricke, A., Zimmermann, M., Gruhn, B., Biondi, A., Kulozik, A. E., Silvestri, D., Bodmer, N., Putti, M. C., Burdach, S., Micalizzi, C., Teigler-Schlegel, A., Ritter, J., Pession, A., Cario, G., Bielack, S., Basso, G., Klingebiel, T., Vinti, L., Rizzari, C., Attarbaschi, A., Santoro, N., Parasole, R., Mann, G., Karawajew, L., Haas, O. A., Conter, V., Schrappe, M., Locatelli F. (ORCID:0000-0002-7976-3654), Locatelli, Franco, Valsecchi, M. G., Moricke, A., Zimmermann, M., Gruhn, B., Biondi, A., Kulozik, A. E., Silvestri, D., Bodmer, N., Putti, M. C., Burdach, S., Micalizzi, C., Teigler-Schlegel, A., Ritter, J., Pession, A., Cario, G., Bielack, S., Basso, G., Klingebiel, T., Vinti, L., Rizzari, C., Attarbaschi, A., Santoro, N., Parasole, R., Mann, G., Karawajew, L., Haas, O. A., Conter, V., Schrappe, M., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

NO ABSTRACT

Published

2017

38. Imatinib and nilotinib off-target effects on human NK cells, monocytes, and M2 macrophages

Author

Bellora, F., Dondero, A., Corrias, M. V., Casu, B., Regis, S., Caliendo, F., Moretta, A., Cazzola, M., Elena, C., Vinti, L., Locatelli, Franco, Bottino, C., Castriconi, R., Locatelli F. (ORCID:0000-0002-7976-3654), Bellora, F., Dondero, A., Corrias, M. V., Casu, B., Regis, S., Caliendo, F., Moretta, A., Cazzola, M., Elena, C., Vinti, L., Locatelli, Franco, Bottino, C., Castriconi, R., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Tyrosine kinase inhibitors (TKIs) are used in the clinical management of hematological neoplasms. Moreover, in solid tumors such as stage 4 neuroblastomas (NB), imatinib showed benefits that might depend on both on-target and immunological off-target effects. We investigated the effects of imatinib and nilotinib on human NK cells, monocytes, and macrophages. High numbers of monocytes died upon exposure to TKI concentrations similar to those achieved in patients. Conversely,NKcells were highly resistant to the TKI cytotoxic effect, were properly activated by immunostimulatory cytokines, and degranulated in the presence of NB cells. In NB, neither drug reduced the expression of ligands for activating NK receptors or upregulated that of HLA class I, B7-H3, PD-L1, and PD-L2, molecules that might limit NK cell function. Interestingly, TKIs modulated the chemokine receptor repertoire of immune cells. Acting at the transcriptional level, they increased the surface expression of CXCR4, an effect observed also in NK cells and monocytes of patients receiving imatinib for chronic myeloid leukemia. Moreover, TKIs reduced the expression of CXCR3 (in NK cells) and CCR1 (in monocytes). Monocytes also decreased the expression of M-CSFR, and low numbers of cells underwent differentiation toward macrophages. M0 and M2 macrophages were highly resistant to TKIs and maintained their phenotypic and functional characteristics. Importantly, also in the presence of TKIs, the M2 immunosuppressive polarization was reverted by TLR engagement, and M1-oriented macrophages fully activated autologous NK cells. Our results contribute to better interpreting the offtarget efficacy of TKIs in tumors and to envisaging strategies aimed at facilitating antitumor immune responses.

Published

2017

39. Protocol II vs protocol III given twice during reinduction therapy in children with medium-risk ALL

Author

Locatelli, F, Valsecchi, M, Möricke, A, Zimmermann, M, Gruhn, B, Biondi, A, Kulozik, A, Silvestri, D, Bodmer, N, Putti, M, Burdach, S, Micalizzi, C, Teigler-Schlegel, A, Ritter, J, Pession, A, Cario, G, Bielack, S, Basso, G, Klingebiel, T, Vinti, L, Rizzari, C, Attarbaschi, A, Santoro, N, Parasole, R, Mann, G, Karawajew, L, Haas, O, Conter, V, Schrappe, M, Valsecchi, MG, Kulozik, AE, Putti, MC, Locatelli, F, Valsecchi, M, Möricke, A, Zimmermann, M, Gruhn, B, Biondi, A, Kulozik, A, Silvestri, D, Bodmer, N, Putti, M, Burdach, S, Micalizzi, C, Teigler-Schlegel, A, Ritter, J, Pession, A, Cario, G, Bielack, S, Basso, G, Klingebiel, T, Vinti, L, Rizzari, C, Attarbaschi, A, Santoro, N, Parasole, R, Mann, G, Karawajew, L, Haas, O, Conter, V, Schrappe, M, Valsecchi, MG, Kulozik, AE, and Putti, MC

Published

2017

40. Comprehensive characterization of mesenchymal stromal cells from patients with Fanconi anaemia

Author

Mantelli, M., Avanzini, M. A., Rosti, V., Ingo, D. M., Conforti, A., Novara, F., Arrigo, G., Boni, M., Zappatore, R., Lenta, E., Moretta, A., Acquafredda, G., de Silvestri, A., Cirillo, V., Cicchetti, E., Algeri, M., Strocchio, L., Vinti, L., Starc, N., Biagini, S., Sirleto, P., Bernasconi, P., Zuffardi, O., Maserati, E., Maccario, R., Zecca, M., Locatelli, Franco, Bernardo, M. E., Locatelli F. (ORCID:0000-0002-7976-3654), Mantelli, M., Avanzini, M. A., Rosti, V., Ingo, D. M., Conforti, A., Novara, F., Arrigo, G., Boni, M., Zappatore, R., Lenta, E., Moretta, A., Acquafredda, G., de Silvestri, A., Cirillo, V., Cicchetti, E., Algeri, M., Strocchio, L., Vinti, L., Starc, N., Biagini, S., Sirleto, P., Bernasconi, P., Zuffardi, O., Maserati, E., Maccario, R., Zecca, M., Locatelli, Franco, Bernardo, M. E., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Fanconi anaemia (FA) is an inherited disorder characterized by pancytopenia, congenital malformations and a predisposition to develop malignancies. Alterations in the haematopoietic microenvironment of FA patients have been reported, but little is known regarding the components of their bone marrow (BM) stroma. We characterized mesenchymal stromal cells (MSCs) isolated from BM of 18 FA patients both before and after allogeneic haematopoietic stem cell transplantation (HSCT). Morphology, fibroblast colony-forming unit (CFU-F) ability, proliferative capacity, immunophenotype, differentiation potential, ability to support long-term haematopoiesis and immunomodulatory properties of FA-MSCs were analysed and compared with those of MSCs expanded from 15 age-matched healthy donors (HD-MSCs). FA-MSCs were genetically characterized through conventional karyotyping, diepoxybutane-test and array-comparative genomic hybridization. FA-MSCs generated before and after HSCT were compared. Morphology, immunophenotype, differentiation potential, ability in vitro to inhibit mitogen-induced T-cell proliferation and to support long-term haematopoiesis did not differ between FA-MSCs and HD-MSCs. CFU-F ability and proliferative capacity of FA-MSCs isolated after HSCT were significantly lower than those of HD-MSCs. FA-MSCs reached senescence significantly earlier than HD-MSCs and showed spontaneous chromosome fragility. Our findings indicate that FA-MSCs are defective in their ability to survive in vitro and display spontaneous chromosome breakages; whether these defects are involved in pathophysiology of BM failure syndromes deserves further investigation.

Published

2015

41. Treosulfan-based conditioning regimen for allogeneic haematopoietic stem cell transplantation in children with sickle cell disease

Author

Strocchio, L., Zecca, M., Comoli, P., Mina, T., Giorgiani, G., Giraldi, E., Vinti, L., Merli, P., Regazzi, M., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Strocchio, L., Zecca, M., Comoli, P., Mina, T., Giorgiani, G., Giraldi, E., Vinti, L., Merli, P., Regazzi, M., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Although allogeneic haematopoietic stem cell transplantation (HSCT) still represents the only consolidated possibility of cure for sickle cell disease (SCD) patients, its use has been limited by the risk of morbidity and mortality associated with conventional myeloablative therapy. The introduction of treosulfan to replace busulfan in conditioning regimens has recently been explored by virtue of its lower toxicity profile. We report our experience with a treosulfan/thiotepa/fludarabine conditioning for human leucocyte antigen (HLA)-matched sibling or unrelated donor-HSCT in 15 children with SCD, and compare patient outcomes with those of a historical cohort (15 patients) given a busulfan-based regimen. Engraftment was achieved in 28 out of 30 patients (93%), with one case of graft failure in either group. The conditioning regimen was well tolerated in both groups, with no cases of grade III-IV regimen-related toxicity. The 7-year overall survival (OS) and disease-free survival (DFS) for the whole cohort were 100% and 93%, respectively, with a 93% DFS in both busulfan and treosulfan groups. No SCD-related adverse events occurred after engraftment in patients with complete or mixed donor chimerism. This retrospective analysis suggests that a treosulfan-based conditioning regimen is able to ensure engraftment with excellent OS/DFS and low regimen-related toxicity in patients with SCD.

Published

2015

42. Cord blood transplantation in children with hemoglobinopathies

Author

Strocchio, L., Romano, M., Cefalo, M. G., Vinti, L., Gaspari, S., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Strocchio, L., Romano, M., Cefalo, M. G., Vinti, L., Gaspari, S., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Introduction: Current challenges in the field of hematopoietic stem cell transplantation (HSCT) for hemoglobinopathies include the possibility of using alternative donors to expand the number of candidates to an allograft. Umbilical cord blood transplantation (UCBT) have extended the access to HSCT in patients lacking matched related or unrelated adult donors, and appears particularly appealing in non-malignant diseases by virtue of the associated low incidence of graft-versus-host disease (GVHD).Areas covered: Outcomes of patients with thalassemia or sickle cell disease given related UCBT is at least as good as that of patients receiving bone marrow (BM) allograft from human leucocyte antigen (HLA)-identical siblings, provided the UCB unit contains adequate cell dose. The experience with unrelated UCBT has been less encouraging, primarily due to low engraftment rates and delayed hematopoietic recovery. New promising approaches of ex vivo graft manipulation aimed at overcoming the drawback of cell dose limitation are under investigation.Expert opinion: We suggest that HSCT should be pursued whenever an HLA-identical CB unit is available, employing it either alone or in combination with BM from the same donor. Based on currently reported data, unrelated UCBT appears to be a suboptimal strategy for patients with hemoglobinopathies, unless it is performed in the context of clinical trials aimed at exploring specific treatment platforms of ex vivo UCB-graft manipulation.

Published

2015

43. Eltrombopag for treatment of thrombocytopenia-associated disorders

Author

Merli, P., Strocchio, L., Vinti, L., Palumbo, G., Locatelli, Franco, Locatelli F. (ORCID:0000-0002-7976-3654), Merli, P., Strocchio, L., Vinti, L., Palumbo, G., Locatelli, Franco, and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

Introduction: Eltrombopag is an orally bioavailable, non-peptide thrombopoietin receptor agonist capable of stimulating platelet production through the differentiation of CD34+ hematopoietic progenitor cells into committed CD41+ megakaryocyte precursors and proliferation of megakaryocyte progenitor cells.Areas covered: This drug has been tested in several clinical trials in adult patients with chronic immune thrombocytopenia (ITP), demonstrating the ability of the drug to reduce the burden of thrombocytopenia and its associated side effects. Two multicenter trials on eltrombopag in chronic ITP of childhood have been recently completed, showing that the drug is effective also in pediatric patients. Recent studies have suggested a potential role of eltrombopag in the treatment of thrombocytopenia associated with hepatitis-C virus infection. These studies have documented that adjunct treatment with eltrombopag can help avoid either dose reductions or withdrawal of pegylated interferon due to development of thrombocytopenia. Eltrombopag has shown efficacy also in patients with acquired severe aplastic anemia and myelodysplastic syndromes.Expert opinion: Eltrombopag plays an important therapeutic role in many different conditions characterized by persistent thrombocytopenia. A more comprehensive definition of both long-term safety and benefits deriving from the use of eltrombopag will be obtained through prolonged observation of patients already enrolled in the different studies conducted so far and from future prospective controlled trials.

Published

2015

44. Co-infusion of ex vivo-expanded, parental MSCs prevents life-threatening acute GVHD, but does not reduce the risk of graft failure in pediatric patients undergoing allogeneic umbilical cord blood transplantation

Author

Bernardo, M E, Ball, L M, Cometa, A M, Roelofs, H, Zecca, M, Avanzini, M A, Bertaina, A, Vinti, L, Lankester, A, Maccario, R, Ringden, O, Le Blanc, K, Egeler, R M, Fibbe, W E, Locatelli, Franco, Locatelli, F (ORCID:0000-0002-7976-3654), Bernardo, M E, Ball, L M, Cometa, A M, Roelofs, H, Zecca, M, Avanzini, M A, Bertaina, A, Vinti, L, Lankester, A, Maccario, R, Ringden, O, Le Blanc, K, Egeler, R M, Fibbe, W E, Locatelli, Franco, and Locatelli, F (ORCID:0000-0002-7976-3654)

Abstract

When compared with BMT, umbilical cord blood transplantation (UCBT) is associated with a lower rate of engraftment and delayed hematological/immunological recovery. This leads to increased risk of TRM in the early post transplantation period due to infection. Acute GVHD, although occurring less frequently in UCBT compared with BMT, is also significantly associated with increased rate of early TRM. BM MSCs are known to support normal in vivo hematopoiesis, and co-transplantation of MSCs has been shown to enhance engraftment of human cord blood hematopoietic cells in nonobese diabetic/SCID mice. In 13 children with hematological disorders (median age 2 years) undergoing UCBT, we co-transplanted paternal, HLA-disparate MSCs with the aim of improving hematological recovery and reducing rejection. We observed no differences in hematological recovery or rejection rates compared with 39 matched historical controls, most of whom received G-CSF after UCBT. However, the rate of grade III and IV acute GVHD was significantly decreased in the study cohort when compared with controls (P = 0.05), thus resulting in reduced early TRM. Although these data do not support the use of MSCs in UCBT to support hematopoietic engraftment, they suggest that MSCs, possibly because of their immunosuppressive effect, may abrogate life-threatening acute GVHD and reduce early TRM. Bone Marrow Transplantation (2011) 46, 200-207; doi: 10.1038/bmt.2010.87; published online 19 April 2010

Published

2011

45. The role of killer immunoglobulin-like receptor haplotypes on the outcome of unrelated donor haematopoietic SCT for thalassaemia

Author

Littera, R, Orrù, N, Vacca, A, Bertaina, A, Caocci, G, Mulargia, M, Giardini, C, Piras, E, Mastronuzzi, A, Vinti, L, Orrù, S, Locatelli, Franco, Carcassi, C, La Nasa, G, Locatelli, F (ORCID:0000-0002-7976-3654), Littera, R, Orrù, N, Vacca, A, Bertaina, A, Caocci, G, Mulargia, M, Giardini, C, Piras, E, Mastronuzzi, A, Vinti, L, Orrù, S, Locatelli, Franco, Carcassi, C, La Nasa, G, and Locatelli, F (ORCID:0000-0002-7976-3654)

Abstract

Recent insight into the pathophysiology of acute GVHD after allogeneic haematopoietic SCT has led to a growing interest in the role of natural killer (NK) cells. NK cell cytotoxicity is mainly regulated by the interaction of activating and inhibitory killer immunoglobulin-like receptors (KIRs) with their respective ligands. To investigate the impact of KIRs and their ligands on haematopoietic SCT outcome, we performed a retrospective study of 78 transfusion-dependent thalassaemia patients (median age 10 years, range 1-29 years) transplanted from an unrelated donor selected using high-resolution molecular typing for both class I and II loci after a myeloablative conditioning regimen. GVHD prophylaxis consisted of CsA, short-term MTX and anti-thymocyte globulin in all patients. We found that patients transplanted from donors homozygous for KIR haplotype A had a greater risk of developing grade II-IV acute GVHD compared with those transplanted from a donor carrying at least one B haplotype (hazard ratio 4.5, 99% confidence interval = 1.2-17.1, P = 0.003). Our study suggests that KIR genotyping of donor and recipient pairs could contribute to the identification of patients at high risk for developing severe complications of haematopoietic SCT and thus may help with the choice of intensity of GVHD prophylaxis. Bone Marrow Transplantation (2010) 45, 1618-1624; doi:10.1038/bmt.2010.24; published online 22 February 2010

Published

2010

46. High frequency of ribosomal protein gene deletions in Italian Diamond-Blackfan anemia patients detected by multiplex ligation-dependent probe amplification assay

Author

Quarello, P., primary, Garelli, E., additional, Brusco, A., additional, Carando, A., additional, Mancini, C., additional, Pappi, P., additional, Vinti, L., additional, Svahn, J., additional, Dianzani, I., additional, and Ramenghi, U., additional

Published

2012

47. Possible correlation between food allergies and enuresis

Author

Ferrara, Pietro, Schiavino, A., D'Aleo, C. M., Rigante, Donato, Petrucci, S., Paolini Paoletti, F., Vinti, L., Pardeo, M., Crea, F., Marietti, G., Ferrara P. (ORCID:0000-0001-9449-3464), Rigante D. (ORCID:0000-0001-7032-7779), Ferrara, Pietro, Schiavino, A., D'Aleo, C. M., Rigante, Donato, Petrucci, S., Paolini Paoletti, F., Vinti, L., Pardeo, M., Crea, F., Marietti, G., Ferrara P. (ORCID:0000-0001-9449-3464), and Rigante D. (ORCID:0000-0001-7032-7779)

Abstract

Food allergies in children, in addition to most common symptoms, can be associated with less common but likewise significant organic disorders. Many studies demonstrate some children have behaviour disorders when they fall in with an allergen, towards which they are particularly sensitive, and they normalize themselves just removing that allergen from the diet. Moreover, in some children, to eat a particular food allergen can cause enuresis, that heals with the removal of foods from the diet. The best theory is that urinary bladder smooth muscle acts as target organ for the allergen, causing a spasm, with consequent pressure increase, bladder capacity decrease and so enuresis. Most frequently involved foods are chocolate, milk, tomato, spices, citrus fruits, grapes, apple and melon. Thus, it's important, in children affected by enuresis and food allergies, removal of foods from the diet, that, in association with a possible desensitizing treatment, may cure completly enuretic symptomatology too.

Published

2002

48. Possibili correlazioni tra allergie alimentari ed enuresi

Author

Ferrara, Pietro, Schiavino, A., D’Aleo, C. M., Rigante, Donato, Petrucci, S., Paolini Paoletti, F., Vinti, L., Pardeo, M., Crea, F., Marietti, G., Ferrara, P. (ORCID:0000-0001-9449-3464), Rigante, Donato (ORCID:0000-0001-7032-7779), Ferrara, Pietro, Schiavino, A., D’Aleo, C. M., Rigante, Donato, Petrucci, S., Paolini Paoletti, F., Vinti, L., Pardeo, M., Crea, F., Marietti, G., Ferrara, P. (ORCID:0000-0001-9449-3464), and Rigante, Donato (ORCID:0000-0001-7032-7779)

Abstract

La possibile correlazione tra allergie alimentari ed enuresi nell'età pediatrica viene discussa in questo articolo.

Published

2002

49. Diamond-Blackfan anemia: genotype-phenotype correlations in Italian patients with RPL5 and RPL11 mutations

Author

Quarello, P., primary, Garelli, E., additional, Carando, A., additional, Brusco, A., additional, Calabrese, R., additional, Dufour, C., additional, Longoni, D., additional, Misuraca, A., additional, Vinti, L., additional, Aspesi, A., additional, Biondini, L., additional, Loreni, F., additional, Dianzani, I., additional, and Ramenghi, U., additional

Published

2009

50. PACSIN2 rs2413739 influence on thiopurine pharmacokinetics: validation studies in pediatric patients

Author

Nagua Giurici, Diego Favretto, Antonella Colombini, Raffaella Franca, Irene Del Rizzo, Andrea Biondi, Franco Locatelli, Alessandro Ventura, Giuliana Decorti, Gabriele Stocco, S. Martellossi, Marco Pelin, Franca Fagioli, Elena Barisone, Marco Rabusin, Luciana Vinti, Franca, R, Stocco, G, Favretto, D, Giurici, N, del Rizzo, I, Locatelli, F, Vinti, L, Biondi, A, Colombini, A, Fagioli, F, Barisone, E, Pelin, M, Martellossi, S, Ventura, A, Decorti, G, Rabusin, M, Franca, R., Stocco, G., Favretto, D., Giurici, N., del Rizzo, I., Locatelli, F., Vinti, L., Biondi, A., Colombini, A., Fagioli, F., Barisone, E., Pelin, M., Martellossi, S., Ventura, A., Decorti, G., and Rabusin, M.

Subjects

Male, 0301 basic medicine, genotype, Pediatric patients, population, Thiopurine pharmacokinetic, 030226 pharmacology & pharmacy, Gastroenterology, Inflammatory bowel disease, polymorphism, Cohort Studies, 0302 clinical medicine, Polymorphism (computer science), Azathioprine, Genotype, Child, pharmacogenetics, Thiopurine methyltransferase, biology, tpmt, Mercaptopurine, implementation consortium guidelines, s-methyltransferase, therapy, azathioprine, determinant, Middle Aged, Precursor Cell Lymphoblastic Leukemia-Lymphoma, TPMT, thiopurine, Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA, Italy, Child, Preschool, Cohort, Molecular Medicine, Female, PACSIN2 rs2413739, pediatric patients, acute lymphoblastic leukemia, inflammatory bowel disease, pediatric patient, medicine.drug, thiopurine pharmacokinetics, Adult, medicine.medical_specialty, Adolescent, Polymorphism, Single Nucleotide, 03 medical and health sciences, Pharmacokinetics, thiopurine, Internal medicine, Genetics, medicine, Humans, Adverse effect, Adaptor Proteins, Signal Transducing, Pharmacology, business.industry, Inflammatory Bowel Diseases, medicine.disease, 030104 developmental biology, biology.protein, business

Abstract

The aim of the study was to validate the impact of the single-nucleotide polymorphism rs2413739 (T > C) in the PACSIN2 gene on thiopurines pharmacological parameters and clinical response in an Italian cohort of pediatric patients with acute lymphoblastic leukemia (ALL) and inflammatory bowel disease (IBD). In ALL, PACSIN2 rs2413739 T allele was associated with a significant reduction of TPMT activity in erythrocytes (p = 0.0094, linear mixed-effect model, multivariate analysis considering TPMT genotype) and increased severe gastrointestinal toxicity during consolidation therapy (p = 0.049). A similar trend was present also for severe hematological toxicity during maintenance. In IBD, no significant effect of rs2413739 could be found on TPMT activity, howeverazathioprine effectiveness was reduced in patients carrying the T allele (linear mixed effect, p = 0.0058). In PBMC from healthy donors, a positive correlation between PACSIN2 and TPMT protein concentration could be detected (linear mixed effect, p = 0.045). These results support the role of PACSIN2 polymorphism on TPMT activity and mercaptopurine adverse effects in patients with ALL. Further evidence on PBMC and pediatric patients with IBD supports an association between PACSIN2 variants, TPMT activity, and thiopurines effects, even if more studies are needed since some of these effects may be tissue specific.

Published

2019