Your search keyword '"Stefania Girlanda"' showing total 31 results

1. A real‐world retrospective–prospective analysis of efficacy and safety of combined ixazomib, lenalidomide, and dexamethasone in relapsed/refractory multiple myeloma: The northern Italy experience

Author

Anna Furlan, Michele Cea, Laura Pavan, Monica Galli, Cristina Clissa, Silvia Mangiacavalli, Anna Maria Cafro, Stefania Girlanda, Francesca Patriarca, Claudia Minotto, Giovanni Bertoldero, Gregorio Barilà, Anna Pascarella, Albana Lico, Rossella Paolini, Nicholas Rabassi, Norbert Pescosta, Marika Porrazzo, Giovanni De Sabbata, Alessandra Pompa, Giulia Bega, Stefania Cavallin, Francesca Guidotti, Magda Marcatti, Maurizio Rupolo, Angelo Belotti, Filippo Gherlinzoni, and Renato Zambello

Subjects

efficacy, ixazomib–lenalidomide–dexamethasone, lenalidomide‐exposed, lenalidomide‐refractory, real‐life, relapsed/refractory multiple myeloma, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Introduction Ixazomib, lenalidomide, and dexamethasone (IRd) have been approved for the treatment of relapsed/refractory multiple myeloma (RRMM) based on the results of the TOURMALINE‐MM1. Objectives and Methods We conducted a retrospective–prospective analysis of 106 RRMM patients (pts) treated with IRd in 21 centers in Northern Italy, with the aim to evaluate the efficacy and safety of IRd in real life. Results At IRd initiation, 34% of pts were aged ≥75 (median 72.5), 8.5% had an ECOG performance status ≥2, 54.7% of evaluable pts carried high‐risk cytogenetic abnormalities [del17p and/or t(4;14) and/or t(14;16) and/or 1 g gain/amp], 60.2% had received ≥2 prior lines of therapy (pLoT), 57.5% were lenalidomide (Len)‐exposed (including both Len‐sensitive and Len‐refractory pts), and 22% were Len‐refractory. Main G ≥3 adverse events (AEs) were thrombocytopenia (16%) and neutropenia (12.3%). G ≥3 non‐hematologic AEs included infections (9.4%) and GI toxicity (diarrhea 5.7%, hepatotoxicity 2.8%), VTE, skin rash, and peripheral neuropathy were mainly G1‐2. The overall response rate was 56.4% (≥VGPR 30%). With a median follow‐up of 38 m, median PFS (mPFS) was 16 m and the 1‐year OS rate was 73%. By subgroup analysis, an extended PFS was observed for pts achieving ≥VGPR (mPFS 21.2 m), time from diagnosis to IRd ≥5 years (26.2 m), 1 pLoT (34.4 m), Len‐naïve (NR), age ≥70 (20 m). In pts exposed to Len, non‐refractory in any prior line and immediately prior to IRd, mPFS was 16 and 18 m, respectively. An inferior PFS was seen in Len‐refractory pts (4.6 m). By multivariate analysis, independent predictors of PFS were age ≥70 (HR 0.6), time from diagnosis ≥5 years (HR 0.32), refractoriness to Len in any prior line (HR 3.33), and immediately prior (HR 4.31). Conclusion IRd might be effective and safe in RRMM pts with an indolent disease, in early lines of treatment, and who proved Len‐sensitive, independent of age, and cytogenetic risk.

Published

2024

2. P970: A REAL-WORLD RETROSPECTIVE-PROSPECTIVE ANALYSIS OF EFFICACY AND SAFETY OF COMBINED IXAZOMIB, LENALIDOMIDE AND DEXAMETHASONE IN RELAPSED/REFRACTORY MULTIPLE MYELOMA: THE NORTHERN ITALY EXPERIENCE

Author

Anna Furlan, Michele Cea, Renato Zambello, Laura Pavan, Monica Galli, Cristina Clissa, Silvia Mangiacavalli, Anna Maria Cafro, Stefania Girlanda, Francesca Patriarca, Claudia Minotto, Giovanni Bertoldero, Gregorio Barilà, Anna Pascarella, Albana Lico, Rossella Paolini, Nicholas Rabassi, Norbert Pescosta, Marika Porrazzo, and Filippo Gherlinzoni

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Published

2023

3. Immune Reconstitution-Based Score for Risk Stratification of Chronic Graft-Versus-Host Disease Patients

Author

Fabio Serpenti, Francesca Lorentino, Sarah Marktel, Raffaella Milani, Carlo Messina, Raffaella Greco, Stefania Girlanda, Daniela Clerici, Fabio Giglio, Carmine Liberatore, Francesca Farina, Sara Mastaglio, Simona Piemontese, Elena Guggiari, Francesca Lunghi, Magda Marcatti, Matteo G. Carrabba, Massimo Bernardi, Chiara Bonini, Andrea Assanelli, Consuelo Corti, Jacopo Peccatori, Fabio Ciceri, and Maria Teresa Lupo-Stanghellini

Subjects

chronic GvHD, immune reconstitution, biomarker, prognostic score, overall survival, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

IntroductionAllogeneic stem cell transplantation survivors are at a relevant risk of developing chronic GvHD (cGvHD), which importantly affects quality of life and increases morbidity and mortality. Early identification of patients at risk of cGvHD-related morbidity could represent a relevant tool to tailor preventive strategies. The aim of this study was to evaluate the prognostic power of immune reconstitution (IR) at cGvHD onset through an IR-based score.MethodsWe analyzed data from 411 adult patients consecutively transplanted between January 2011 and December 2016 at our Institution: 151 patients developed cGvHD (median follow-up 4 years). A first set of 111 consecutive patients with cGvHD entered the test cohort while an additional consecutive 40 patients represented the validation cohort. A Cox multivariate model for OS (overall survival) in patients with cGvHD of any severity allowed the identification of six variables independently predicting OS and TRM (transplant-related mortality). A formula for a prognostic risk index using the β coefficients derived from the model was designed. Each patient was assigned a score defining three groups of risk (low, intermediate, and high).ResultsOur multivariate model defined the variables independently predicting OS at cGvHD onset: CD4+ >233 cells/mm3, NK 3.09 and ≤6.9, and high-risk patients >6.9. By ROC analysis, we identified a cut-off of 6.310 for both TRM and overall mortality.In the training cohort, the 6-year OS and TRM from cGvHD occurrence were 85% (95% CI, 70-92) and 13% (95% CI, 5-25) for low-risk, 64% (95% CI, 44-89) and 30% (95% CI, 15-47) for intermediate-risk, 26% (95% CI, 10-47), and 42% (95% CI, 19-63) for high-risk patients (OS p

Published

2021

4. ATR addiction in multiple myeloma: synthetic lethal approaches exploiting established therapies

Author

Oronza A. Botrugno, Silvia Bianchessi, Desirée Zambroni, Michela Frenquelli, Daniela Belloni, Lucia Bongiovanni, Stefania Girlanda, Simona Di Terlizzi, Marina Ferrarini, Elisabetta Ferrero, Maurilio Ponzoni, Magda Marcatti, and Giovanni Tonon

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Therapeutic strategies designed to tinker with cancer cell DNA damage response have led to the widespread use of PARP inhibitors for BRCA1/2-mutated cancers. In the haematological cancer multiple myeloma, we sought to identify analogous synthetic lethality mechanisms that could be leveraged upon established cancer treatments. The combination of ATR inhibition using the compound VX-970 with a drug eliciting interstrand cross-links, melphalan, was tested in in vitro, ex vivo, and most notably in vivo models. Cell proliferation, induction of apoptosis, tumor growth and animal survival were assessed. The combination of ATM inhibition with a drug triggering double strand breaks, doxorucibin, was also probed. We found that ATR inhibition is strongly synergistic with melphalan, even in resistant cells. The combination was dramatically effective in targeting myeloma primary patient cells and cell lines reducing cell proliferation and inducing apoptosis. The combination therapy significantly reduced tumor burden and prolonged survival in animal models. Conversely, ATM inhibition only marginally impacted on myeloma cell survival, even in combination with doxorucibin at high doses. These results indicate that myeloma cells extensively rely on ATR, but not on ATM, for DNA repair. Our findings posit that adding an ATR inhibitor such as VX-970 to established therapeutic regimens may provide a remarkably broad benefit to myeloma patients.

Published

2019

5. Modeling multiple myeloma-bone marrow interactions and response to drugs in a 3D surrogate microenvironment

Author

Daniela Belloni, Silvia Heltai, Maurilio Ponzoni, Antonello Villa, Barbara Vergani, Lorenza Pecciarini, Magda Marcatti, Stefania Girlanda, Giovanni Tonon, Fabio Ciceri, Federico Caligaris-Cappio, Marina Ferrarini, and Elisabetta Ferrero

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Multiple myeloma develops primarily inside the bone marrow microenvironment, that confers pro-survival signals and drug resistance. 3D cultures that reproduce multiple myeloma-bone marrow interactions are needed to fully investigate multiple myeloma pathogenesis and response to drugs. To this purpose, we exploited the 3D Rotary Cell Culture System bioreactor technology for myeloma-bone marrow co-cultures in gelatin scaffolds. The model was validated with myeloma cell lines that, as assessed by histochemical and electron-microscopic analyses, engaged contacts with stromal cells and endothelial cells. Consistently, pro-survival signaling and also cell adhesion-mediated drug resistance were significantly higher in 3D than in 2D parallel co-cultures. The contribution of the VLA-4/VCAM1 pathway to resistance to bortezomib was modeled by the use of VCAM1 transfectants. Soluble factor-mediated drug resistance could be also demonstrated in both 2D and 3D co-cultures. The system was then successfully applied to co-cultures of primary myeloma cells-primary myeloma bone marrow stromal cells from patients and endothelial cells, allowing the development of functional myeloma-stroma interactions and MM cell long-term survival. Significantly, genomic analysis performed in a high-risk myeloma patient demonstrated that culture in bioreactor paralleled the expansion of the clone that ultimately dominated in vivo. Finally, the impact of bortezomib on myeloma cells and on specialized functions of the microenvironment could be evaluated. Our findings indicate that 3D dynamic culture of reconstructed human multiple myeloma microenvironments in bioreactor may represent a useful platform for drug testing and for studying tumor-stroma molecular interactions.

Published

2018

6. Ex-vivo dynamic 3-D culture of human tissues in the RCCS™ bioreactor allows the study of Multiple Myeloma biology and response to therapy.

Author

Marina Ferrarini, Nathalie Steimberg, Maurilio Ponzoni, Daniela Belloni, Angiola Berenzi, Stefania Girlanda, Federico Caligaris-Cappio, Giovanna Mazzoleni, and Elisabetta Ferrero

Subjects

Medicine, Science

Abstract

Three-dimensional (3-D) culture models are emerging as invaluable tools in tumor biology, since they reproduce tissue-specific structural features and cell-cell interactions more accurately than conventional 2-D cultures. Multiple Myeloma, which depends on myeloma cell-Bone Marrow microenvironment interactions for development and response to drugs, may particularly benefit from such an approach. An innovative 3-D dynamic culture model based on the use of the RCCS™ Bioreactor was developed to allow long-term culture of myeloma tissue explants. This model was first validated with normal and pathological explants, then applied to tissues from myeloma patients. In all cases, histological examination demonstrated maintenance of viable myeloma cells inside their native microenvironment, with an overall well preserved histo-architecture including bone lamellae and vessels. This system was then successfully applied to evaluate the cytotoxic effects exerted by the proteasome inhibitor Bortezomib not only on myeloma cells but also on angiogenic vessels. Moreover, as surrogate markers of specialized functions expressed by myeloma cells and microenvironment, β2 microglobulin, VEGF and Angiopoietin-2 levels, as well as Matrix Metalloproteases activity, were evaluated in supernatants from 3D cultures and their levels reflected the effects of Bortezomib treatment. Notably, determination of β2 microglobulin levels in supernatants from Bortezomib-treated samples and in patients'sera following Bortezomib-based therapies disclosed an overall concordance in the response to the drug ex vivo and in vivo. Our findings indicate, as a proof of principle, that 3-D, RCCS™ bioreactor-based culture of tissue explants can be exploited for studying myeloma biology and for a pre-clinical approach to patient-targeted therapy.

Published

2013

7. Correction: Dynamic 3-D Culture of Human Tissues in the RCCS™ Bioreactor Allows the Study of Multiple Myeloma Biology and Response to Therapy.

Author

Marina Ferrarini, Nathalie Steimberg, Maurilio Ponzoni, Daniela Belloni, Angiola Berenzi, Stefania Girlanda, Federico Caligaris-Cappio, Giovanna Mazzoleni, and Elisabetta Ferrero

Subjects

Medicine, Science

Published

2013

8. Supplementary Figure Legends from Chromogranin A Is Preferentially Cleaved into Proangiogenic Peptides in the Bone Marrow of Multiple Myeloma Patients

Author

Angelo Corti, Federico Caligaris-Cappio, Magda Marcatti, Fabio Ciceri, Giovanni Tonon, Matteo Bellone, P. Leif Bergsagel, Marta Chesi, Marina Ferrarini, Elisabetta Ferrero, Angelina Sacchi, Arianna Calcinotto, Maria Teresa Sabrina Bertilaccio, Maurilio Ponzoni, Stefania Girlanda, Flavio Curnis, Barbara Colombo, Anna Maria Gasparri, and Mimma Bianco

Abstract

Legend for Supplementary Figures S1-S5.

Published

2023

9. Supplementary Methods from Chromogranin A Is Preferentially Cleaved into Proangiogenic Peptides in the Bone Marrow of Multiple Myeloma Patients

Author

Angelo Corti, Federico Caligaris-Cappio, Magda Marcatti, Fabio Ciceri, Giovanni Tonon, Matteo Bellone, P. Leif Bergsagel, Marta Chesi, Marina Ferrarini, Elisabetta Ferrero, Angelina Sacchi, Arianna Calcinotto, Maria Teresa Sabrina Bertilaccio, Maurilio Ponzoni, Stefania Girlanda, Flavio Curnis, Barbara Colombo, Anna Maria Gasparri, and Mimma Bianco

Abstract

Description of additional methods and procedures used in the study.

Published

2023

10. Data from Chromogranin A Is Preferentially Cleaved into Proangiogenic Peptides in the Bone Marrow of Multiple Myeloma Patients

Author

Angelo Corti, Federico Caligaris-Cappio, Magda Marcatti, Fabio Ciceri, Giovanni Tonon, Matteo Bellone, P. Leif Bergsagel, Marta Chesi, Marina Ferrarini, Elisabetta Ferrero, Angelina Sacchi, Arianna Calcinotto, Maria Teresa Sabrina Bertilaccio, Maurilio Ponzoni, Stefania Girlanda, Flavio Curnis, Barbara Colombo, Anna Maria Gasparri, and Mimma Bianco

Abstract

Angiogenesis has been postulated to be critical for the pathogenesis of multiple myeloma, a neoplastic disease characterized by abnormal proliferation of malignant plasma cells in the bone marrow (BM). Cleavage of the N- and C-terminal regions of circulating chromogranin A (CgA, CHGA), classically an antiangiogenic protein, can activate latent antiangiogenic and proangiogenic sites, respectively. In this study, we investigated the distribution of CgA-derived polypeptides in multiple myeloma patients and the subsequent implications for disease progression. We show that the ratio of pro/antiangiogenic forms of CgA is altered in multiple myeloma patients compared with healthy subjects and that this ratio is higher in BM plasma compared with peripheral plasma, suggesting enhanced local cleavage of the CgA C-terminal region. Enhanced cleavage correlated with increased VEGF and FGF2 BM plasma levels and BM microvascular density. Using the Vk*MYC mouse model of multiple myeloma, we further demonstrate that exogenously administered CgA was cleaved in favor of the proangiogenic form and was associated with increased microvessel density. Mechanistic studies revealed that multiple myeloma and proliferating endothelial cells can promote CgA C-terminal cleavage by activating the plasminogen activator/plasmin system. Moreover, cleaved and full-length forms could also counter balance the pro/antiangiogenic activity of each other in in vitro angiogenesis assays. These findings suggest that the CgA-angiogenic switch is activated in the BM of multiple myeloma patients and prompt further investigation of this CgA imbalance as a prognostic or therapeutic target. Cancer Res; 76(7); 1781–91. ©2016 AACR.

Published

2023

11. Supplementary Figures S1-S5 from Chromogranin A Is Preferentially Cleaved into Proangiogenic Peptides in the Bone Marrow of Multiple Myeloma Patients

Author

Angelo Corti, Federico Caligaris-Cappio, Magda Marcatti, Fabio Ciceri, Giovanni Tonon, Matteo Bellone, P. Leif Bergsagel, Marta Chesi, Marina Ferrarini, Elisabetta Ferrero, Angelina Sacchi, Arianna Calcinotto, Maria Teresa Sabrina Bertilaccio, Maurilio Ponzoni, Stefania Girlanda, Flavio Curnis, Barbara Colombo, Anna Maria Gasparri, and Mimma Bianco

Abstract

Characterization of the new α-373 antibody and *373-ELISA (S1); Levels of different CgA-related analytes in peripheral-blood and bone marrow plasma samples obtained from normal subjects and MM patients stratified according to renal failure and treatment with proton pump inhibitors (S2); BM plasma levels of different CgA forms in MM patients at diagnosis in different disease stages (S3); MM and endothelial cells produce the urinary-type plasminogen activator (S4); Alignment of CgA sequence from different species (S5).

Published

2023

12. Supplementary Tables S1-S4 from Chromogranin A Is Preferentially Cleaved into Proangiogenic Peptides in the Bone Marrow of Multiple Myeloma Patients

Author

Angelo Corti, Federico Caligaris-Cappio, Magda Marcatti, Fabio Ciceri, Giovanni Tonon, Matteo Bellone, P. Leif Bergsagel, Marta Chesi, Marina Ferrarini, Elisabetta Ferrero, Angelina Sacchi, Arianna Calcinotto, Maria Teresa Sabrina Bertilaccio, Maurilio Ponzoni, Stefania Girlanda, Flavio Curnis, Barbara Colombo, Anna Maria Gasparri, and Mimma Bianco

Abstract

Demographic and clinical data regarding the study population (S1); ELISAs used for the characterization of CgA and its fragments in MM plasma samples (S2); Correlation between BM plasma levels of different CgA analytes and clinical variables in MM patients at diagnosis (S3); Correlation between BM plasma levels of different CgA analytes and FGF2 or VEGF in MM patients at diagnosis (S4).

Published

2023

13. Ibrutinib Alone or in Combination with R-CHOP Chemoimmunotherapy in Relapsed or Refractory Primary Central Nervous System Lymphoma (rrPCNSL): A «Real-Life» Study

Author

Teresa Calimeri, Federico Erbella, Lorella Orsucci, Teresa Aloisi, Annalisa Arcari, Cirino Botta, Annarosa Cuccaro, Pio Manlio Mirko Frascione, Stefania Girlanda, Manuel Gotti, Sabrina Mariani, Luca Nassi, Fioravante Ronconi, Luana Schiattone, Alessandra Tucci, Luisa Verga, Vincenzo Mercurio, Paolo Fiore, Sara Steffanoni, Fabio Ciceri, and Andrés J.M. Ferreri

Subjects

Immunology, Cell Biology, Hematology, Biochemistry

Published

2022

14. R-CHOP preceded by blood-brain barrier permeabilization with engineered tumor necrosis factor-α in primary CNS lymphoma

Author

C. Cecchetti, Salvatore Perrone, Angelo Corti, Claudio Bordignon, Flavio Curnis, Marianna Sassone, Giovanni Citterio, Maurilio Ponzoni, Andrés J.M. Ferreri, Teresa Calimeri, Letterio S. Politi, Gian Marco Conte, Dario Cattaneo, Marco Foppoli, Eloise Scarano, Fabio Ciceri, Federico Fallanca, Alessandro Nonis, Stefania Girlanda, Nicoletta Anzalone, Paolo Lopedote, Ferreri, Andrés J M, Calimeri, Teresa, Conte, Gian Marco, Cattaneo, Dario, Fallanca, Federico, Ponzoni, Maurilio, Scarano, Eloise, Curnis, Flavio, Nonis, Alessandro, Lopedote, Paolo, Citterio, Giovanni, Politi, Letterio, Foppoli, Marco, Girlanda, Stefania, Sassone, Marianna, Perrone, Salvatore, Cecchetti, Caterina, Ciceri, Fabio, Bordignon, Claudio, Corti, Angelo, and Anzalone, Nicoletta

Subjects

Male, Oncology, Vincristine, medicine.medical_specialty, Cell Membrane Permeability, Cyclophosphamide, Recombinant Fusion Proteins, medicine.medical_treatment, Immunology, Neuroimaging, Vascular permeability, CD13 Antigens, Blood–brain barrier, Biochemistry, Central Nervous System Neoplasms, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Doxorubicin, Tomography, Emission-Computed, Single-Photon, Chemotherapy, Tumor Necrosis Factor-alpha, business.industry, Lymphoma, Non-Hodgkin, Primary central nervous system lymphoma, Cell Biology, Hematology, medicine.disease, Immunohistochemistry, Treatment Outcome, medicine.anatomical_structure, Blood-Brain Barrier, Research Design, Prednisone, Female, Rituximab, business, Biomarkers, medicine.drug

Abstract

Patients with primary central nervous system lymphoma (PCNSL) are treated with high-dose methotrexate-based chemotherapy, which requires hospitalization and extensive expertise to manage related toxicity. The use of R-CHOP (rituximab, cyclophosphamide, doxorubicin, vincristine, and prednisone) could overcome these difficulties, but blood-brain barrier (BBB) penetration of related drugs is poor. Tumor necrosis factor-α coupled with NGR (NGR-hTNF), a peptide targeting CD13+ vessels, induces endothelial permeabilization and improves tumor access of cytostatics. We tested the hypothesis that NGR-hTNF can break the BBB, thereby improving penetration and activity of R-CHOP in patients with relapsed/refractory PCNSL (NCT03536039). Patients received six R-CHOP21 courses, alone at the first course and preceded by NGR-hTNF (0.8 μg/m2) afterward. This trial included 2 phases: an “explorative phase” addressing the effect of NGR-hTNF on drug pharmacokinetic parameters and on vessel permeability, assessed by dynamic contrast-enhanced magnetic resonance imaging and 99mTc-diethylene-triamine-pentacetic acid–single-photon emission computed tomography, and the expression of CD13 on tumor tissue; and an “expansion phase” with overall response rate as the primary end point, in which the 2-stage Simon Minimax design was used. At the first stage, if ≥4 responses were observed among 12 patients, the study accrual would have continued (sample size, 28). Herein, we report results of the explorative phase and the first-stage analysis (n = 12). CD13 was expressed in tumor vessels of all cases. NGR-hTNF selectively increased vascular permeability in tumoral/peritumoral areas, without interfering with drug plasma/cerebrospinal fluid concentrations. The NGR-hTNF/R-CHOP combination was well tolerated: there were only 2 serious adverse events, and grade 4 toxicity was almost exclusively hematological, which were resolved without dose reductions or interruptions. NGR-hTNF/R-CHOP was active, with 9 confirmed responses (75%; 95% confidence interval, 51-99), 8 of which were complete. In conclusion, NGR-hTNF/R-CHOP was safe in these heavily pretreated patients. NGR-hTNF enhanced vascular permeability specifically in tumoral/peritumoral areas, which resulted in fast and sustained responses.

Published

2019

15. COVID-19 in recipients of allogeneic stem cell transplantation: favorable outcome

Author

Carlo Messina, Raffaella Greco, Jacopo Peccatori, Sarah Marktel, Sara Mastaglio, Maria Teresa Lupo-Stanghellini, Francesca Farina, Raffaella Milani, Fabio Ciceri, Lorenzo Lazzari, Andrea Assanelli, Elisabetta Xue, Piera Angelillo, Federico Erbella, Maria Pia Cicalese, Stefania Girlanda, Chiara Oltolini, Simona Piemontese, Consuelo Corti, Massimo Locatelli, Lupo-Stanghellini, M. T., Xue, E., Mastaglio, S., Oltolini, C., Angelillo, P., Messina, C., Piemontese, S., Girlanda, S., Farina, F., Lazzari, L., Cicalese, M. P., Erbella, F., Greco, R., Locatelli, M., Milani, R., Peccatori, J., Corti, C., Marktel, S., Assanelli, A., and Ciceri, F.

Subjects

Transplantation, 2019-20 coronavirus outbreak, Bone marrow transplantation, Coronavirus disease 2019 (COVID-19), business.industry, SARS-CoV-2, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), MEDLINE, Hematopoietic Stem Cell Transplantation, COVID-19, Hematology, Virology, Text mining, Correspondence, Infectious diseases, Medicine, Humans, Transplantation, Homologous, Favorable outcome, Stem cell, business

Published

2021

16. CTIM-24. AUTOLOGOUS CD34+ ENRICHED HEMATOPOIETIC PROGENITOR CELLS GENETICALLY MODIFIED FOR HUMAN INTERFERON-α2, ARE WELL TOLERATED & RAPIDLY ENGRAFT IN PATIENTS WITH GLIOBLASTOMA MULTIFORME (TEM-GBM_001 STUDY)

Author

Matteo Carrabba, Fabio Ciceri, Marica Eoli, Gaetano Finocchiaro, Andrew Zambanini, Stefania Mazzoleni, Alessia Capotondo, Bianca Pollo, Bernhard Gentner, Maria Grazia Bruzzone, Francesco DiMeco, Federico G. Legnani, Mariagrazia Garramone, Paolo Ferroli, Stefania Girlanda, Valeria Cuccarini, Luigi Naldini, Rosina Paterra, Farina Francesca, Carlo Russo, Elena Anghileri, and Marco Saini

Subjects

Cancer Research, Carmustine, medicine.medical_specialty, Hematology, Angiogenesis, business.industry, CD34, O-6-methylguanine-DNA methyltransferase, Clinical Trials: Immunologic, Genetically modified organism, medicine.anatomical_structure, Immune system, Oncology, Internal medicine, medicine, Cancer research, Neurology (clinical), Bone marrow, business, medicine.drug

Abstract

GBM with an unmethylated MGMT gene promoter is associated with very poor prognosis. A subset of tumor associated macrophages expressing the angiopoietin receptor Tie2 (TEMs) can be genetically modified for local & tumor restricted release of interferon-α2 (IFN). IFN has antitumor effects, inhibits angiogenesis & modulates the immune system. Temferon consists of autologous HSPCs transduced ex-vivo with an LVV encoding an IFN gene & expression control sequences for TEMs. TEM-GBM is an open-label, Phase I/IIa study (Part A: 3x3x3 dose escalation; Part B: n=12), & Temferon (single dose) is given to patients with first diagnosis of GBM & unmethylated MGMT promoter. Part A 3rd cohort is ongoing & completes dosing in September 2020. Eight patients completed screening; one patient died (disease progression) before Temferon was administered. Six patients received Temferon (3 women, 3 men, mean age 52.3 years). Cohort 1 received Temferon 0.5x106 cells/kg & Cohort 2, 1x106 cells/kg. Neutropenia & thrombocytopenia occurred as expected following conditioning & hematologic recovery (HR) occurred median D+13. Transduced PBMCs were identified by vector copy number (VCN) on myeloid cells at HR & at later timepoints. In general, a dose-ordered increase in VCN was observed (mean VCN D+30 CD14+ Cohort 1: 0.094, cohort 2: 0.125); 1 patient in each cohort had low VCNs. VCN remained detectable up to recent follow up visits (≤ D+180). No dose-limiting toxicities have been reported. Four SAEs occurred in 3 patients who received Temferon (pneumonia, pulmonary embolism, febrile neutropenia, fatigue) but these events were not attributed to Temferon, resolved, & may have been related to the conditioning regimen (carmustine & thiotepa). Disease progression has been confirmed in 3 patients who received Temferon. These preliminary results indicate feasibility of engrafting a pre-determined fraction of Temferon cells in the bone marrow of GBM patients without, so far, causing dose-limiting toxicity.

Published

2020

17. ATR addiction in multiple myeloma: synthetic lethal approaches exploiting established therapies

Author

Michela Frenquelli, Simona Di Terlizzi, Marina Ferrarini, Giovanni Tonon, Oronza A. Botrugno, Silvia Bianchessi, Elisabetta Ferrero, Lucia Bongiovanni, Daniela Belloni, Maurilio Ponzoni, Stefania Girlanda, Desirée Zambroni, and Magda Marcatti

Subjects

0301 basic medicine, Melphalan, Combination therapy, DNA Repair, DNA repair, Cell Survival, Apoptosis, Synthetic lethality, Ataxia Telangiectasia Mutated Proteins, Article, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, medicine, Animals, Humans, Multiple myeloma, business.industry, Cell growth, Cancer, Hematology, medicine.disease, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, business, Multiple Myeloma, medicine.drug, DNA Damage

Abstract

Therapeutic strategies designed to tinker with cancer cell DNA damage response have led to the widespread use of PARP inhibitors for BRCA1/2-mutated cancers. In the haematological cancer multiple myeloma, we sought to identify analogous synthetic lethality mechanisms that could be leveraged upon established cancer treatments. The combination of ATR inhibition using the compound VX-970 with a drug eliciting interstrand cross-links, melphalan, was tested in in vitro, ex vivo, and most notably in vivo models. Cell proliferation, induction of apoptosis, tumor growth and animal survival were assessed. The combination of ATM inhibition with a drug triggering double strand breaks, doxorucibin, was also probed. We found that ATR inhibition is strongly synergistic with melphalan, even in resistant cells. The combination was dramatically effective in targeting myeloma primary patient cells and cell lines reducing cell proliferation and inducing apoptosis. The combination therapy significantly reduced tumor burden and prolonged survival in animal models. Conversely, ATM inhibition only marginally impacted on myeloma cell survival, even in combination with doxorucibin at high doses. These results indicate that myeloma cells extensively rely on ATR, but not on ATM, for DNA repair. Our findings posit that adding an ATR inhibitor such as VX-970 to established therapeutic regimens may provide a remarkably broad benefit to myeloma patients.

Published

2019

18. Clinical presentation and management practice of systemic mastocytosis. A survey on 460 Italian patients

Author

Omar Perbellini, Giuditta Corbizzi Fattori, Marina Mauro, Valerio Pravettoni, Fabio Almerigogna, Giovanni Martinelli, Chiara Elena, Francesca Gesullo, Lisa Pieri, Roberto Salerno, Roberta Zanotti, Cristina Papayannidis, Tiziana Fanelli, Federica Scarfì, Agostino Cortelezzi, Vittoria Cova, Patrizia Bonadonna, Anna Artuso, Diomira Magliacane, Fabio Ciceri, Simona Soverini, Massimiliano Bonifacio, Massimo Triggiani, Caterina De Benedittis, Serena Merante, G Cortellini, Federica Irene Grifoni, Maria Loredana Iorno, Simona Muratori, Stefania Girlanda, Elena Maria Elli, Michela Rondoni, and Alessandro M. Vannucchi

Subjects

medicine.medical_specialty, Acute leukemia, Hematology, business.industry, Retrospective cohort study, medicine.disease, Mast cell leukemia, Dermatology, 03 medical and health sciences, 0302 clinical medicine, 030220 oncology & carcinogenesis, Internal medicine, medicine, Clinical significance, Systemic mastocytosis, Intensive care medicine, business, Survival rate, Myeloproliferative neoplasm, 030215 immunology

Abstract

Systemic mastocytosis is a rare heterogeneous myeloproliferative neoplasm characterized by abnormal proliferation and activation of mast cells. We describe a large multicentre series of 460 adult patients with systemic mastocytosis, with a diagnosis based on WHO 2008 criteria, in a "real-life" setting of ten Italian centers with dedicated multidisciplinary programs. We included indolent forms with (n = 255) and without (n = 165) skin lesions, smouldering (n = 20), aggressive (n = 28), associated with other hematological diseases mastocytosis (n = 21) and mast cell leukemia (n = 1). This series was uniquely characterized by a substantial proportion of patients with low burden of neoplastic mast cells; notably, 38% of cases were diagnosed using only minor diagnostic criteria according to WHO 2008 classification, underlying the feasibility of early diagnosis where all diagnostic approaches are made available. This has particular clinical relevance for prevention of anaphylaxis manifestations, that were typically associated with indolent forms. In multivariate analysis, the most important features associated with shortened overall survival were disease subtype and age at diagnosis >60 years. Disease progression was correlated with mastocytosis subtype and thrombocytopenia. As many as 32% of patients with aggressive mastocytosis suffered from early evolution into acute leukemia. Overall, this study provides novel information about diagnostic approaches and current presentation of patients with SM and underlines the importance of networks and specialized centers to facilitate early diagnosis and prevent disease-associated manifestations. Am. J. Hematol. 91:692-699, 2016. © 2016 Wiley Periodicals, Inc.

Published

2016

19. Modeling multiple myeloma-bone marrow interactions and response to drugs in a 3d surrogate microenvironment

Author

Stefania Girlanda, Marina Ferrarini, Lorenza Pecciarini, Elisabetta Ferrero, Federico Caligaris-Cappio, Magda Marcatti, Giovanni Tonon, Maurilio Ponzoni, Antonello Villa, Silvia Heltai, Barbara Vergani, Fabio Ciceri, Daniela Belloni, Belloni, D, Heltai, S, Ponzoni, M, Villa, A, Vergani, B, Pecciarini, L, Marcatti, M, Girlanda, S, Tonon, G, Ciceri, F, Caligaris-Cappio, F, Ferrarini, M, Ferrero, E, Belloni, Daniela, Heltai, Silvia, Ponzoni, Maurilio, Villa, Antonello, Vergani, Barbara, Pecciarini, Lorenza, Marcatti, Magda, Girlanda, Stefania, Tonon, Giovanni, Ciceri, Fabio, Caligaris-Cappio, Federico, Ferrarini, Marina, and Ferrero, Elisabetta

Subjects

0301 basic medicine, 3D model, medicine.medical_specialty, Stromal cell, Cell Survival, Cell Culture Techniques, Drug Resistance, Cell Communication, Models, Biological, Article, Plasma Cell Disorders, Bortezomib, 03 medical and health sciences, Bioreactors, 0302 clinical medicine, Bone Marrow, immune system diseases, hemic and lymphatic diseases, Internal medicine, Cell Adhesion, Tumor Microenvironment, medicine, Humans, Multiple myeloma, Tumor microenvironment, Hematology, Chemistry, Endothelial Cells, medicine.disease, Coculture Techniques, Bone Marrow Microenvironment, 030104 developmental biology, medicine.anatomical_structure, Cell culture, 030220 oncology & carcinogenesis, Cancer research, Gelatin, Bone marrow, Stromal Cells, Clone (B-cell biology), Multiple Myeloma, medicine.drug

Abstract

Multiple myeloma develops primarily inside the bone marrow microenvironment, that confers pro-survival signals and drug resistance. 3D cultures that reproduce multiple myeloma-bone marrow interactions are needed to fully investigate multiple myeloma pathogenesis and response to drugs. To this purpose, we exploited the 3D Rotary Cell Culture System bioreactor technology for myeloma-bone marrow co-cultures in gelatin scaffolds. The model was validated with myeloma cell lines that, as assessed by histochemical and electron-microscopic analyses, engaged contacts with stromal cells and endothelial cells. Consistently, pro-survival signaling and also cell adhesion-mediated drug resistance were significantly higher in 3D than in 2D parallel co-cultures. The contribution of the VLA-4/VCAM1 pathway to resistance to bortezomib was modeled by the use of VCAM1 transfectants. Soluble factor-mediated drug resistance could be also demonstrated in both 2D and 3D co-cultures. The system was then successfully applied to co-cultures of primary myeloma cells-primary myeloma bone marrow stromal cells from patients and endothelial cells, allowing the development of functional myeloma-stroma interactions and MM cell long-term survival. Significantly, genomic analysis performed in a high-risk myeloma patient demonstrated that culture in bioreactor paralleled the expansion of the clone that ultimately dominated in vivo. Finally, the impact of bortezomib on myeloma cells and on specialized functions of the microenvironment could be evaluated. Our findings indicate that 3D dynamic culture of reconstructed human multiple myeloma microenvironments in bioreactor may represent a useful platform for drug testing and for studying tumor-stroma molecular interactions.

Published

2018

20. R-CHOP preceded by blood-brain barrier permeabilization (BBBp) by NGR-tumor necrosis factor (NGR-hTNF) in patients with relapsed or refractory primary CNS lymphoma (rrPCNSL): First results of the 'INGRID' phase II trial

Author

Nicoletta Anzalone, Andrés J.M. Ferreri, Federico Fallanca, Giovanni Citterio, Dario Cattaneo, Gian Marco Conte, Salvatore Perrone, Marco Foppoli, Alessandro Nonis, Fabio Ciceri, Marianna Sassone, Stefania Girlanda, Caterina Cecchetti, Letterio S. Politi, Maurilio Ponzoni, Angelo Corti, Teresa Calimeri, Paolo Lopedote, and Claudio Bordignon

Subjects

Cancer Research, business.industry, Blood–brain barrier, medicine.anatomical_structure, Oncology, NGR-hTNF, Refractory, Primary CNS Lymphoma, Toxicity, Cancer research, Medicine, In patient, Tumor necrosis factor alpha, business

Abstract

7575Background: PCNSL pts are treated with HDMTX-based chemo, which requires hospitalization and extensive expertise to manage toxicity. R-CHOP could overcome these troubles, but CNS access of rela...

Published

2018

21. Erdheim-Chester disease: report on a case and new insights on its immunopathogenesis

Author

Lorenzo Dagna, Stefania Girlanda, Marina Ferrarini, Maria Grazia Sabbadini, Nathalie Rizzo, Enrica Bozzolo, Silvia Langheim, Dagna, Lorenzo, Girlanda, S, Langheim, S, Rizzo, N, Bozzolo, Ep, Sabbadini, Mg, and Ferrarini, M.

Subjects

medicine.medical_specialty, Rheumatology, business.industry, Erdheim–Chester disease, medicine, Pharmacology (medical), medicine.disease, business, Dermatology

Abstract

In this paper, we describe the release of cyto-chemokines potentially relevant to Erdheim-Chester disease pathogenesis by intra-lesional cells from a patient with skeletal and multiorgan involvements.

Published

2010

22. Chromogranin A Is Preferentially Cleaved into Proangiogenic Peptides in the Bone Marrow of Multiple Myeloma Patients

Author

Elisabetta Ferrero, Angelina Sacchi, Arianna Calcinotto, Giovanni Tonon, Mimma Bianco, Maurilio Ponzoni, Marina Ferrarini, Flavio Curnis, Marta Chesi, Maria Teresa Sabrina Bertilaccio, Matteo Bellone, Stefania Girlanda, Fabio Ciceri, Federico Caligaris-Cappio, Magda Marcatti, P. Leif Bergsagel, Anna Gasparri, Barbara Colombo, and Angelo Corti

Subjects

0301 basic medicine, Male, endocrine system, Cancer Research, medicine.medical_specialty, Plasmin, Angiogenesis, Pathogenesis, Neovascularization, 03 medical and health sciences, Mice, 0302 clinical medicine, Bone Marrow, Internal medicine, medicine, Animals, Humans, Multiple myeloma, biology, Neovascularization, Pathologic, Chemistry, Chromogranin A, Middle Aged, medicine.disease, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Female, Bone marrow, medicine.symptom, Multiple Myeloma, Peptides, Plasminogen activator, medicine.drug

Abstract

Angiogenesis has been postulated to be critical for the pathogenesis of multiple myeloma, a neoplastic disease characterized by abnormal proliferation of malignant plasma cells in the bone marrow (BM). Cleavage of the N- and C-terminal regions of circulating chromogranin A (CgA, CHGA), classically an antiangiogenic protein, can activate latent antiangiogenic and proangiogenic sites, respectively. In this study, we investigated the distribution of CgA-derived polypeptides in multiple myeloma patients and the subsequent implications for disease progression. We show that the ratio of pro/antiangiogenic forms of CgA is altered in multiple myeloma patients compared with healthy subjects and that this ratio is higher in BM plasma compared with peripheral plasma, suggesting enhanced local cleavage of the CgA C-terminal region. Enhanced cleavage correlated with increased VEGF and FGF2 BM plasma levels and BM microvascular density. Using the Vk*MYC mouse model of multiple myeloma, we further demonstrate that exogenously administered CgA was cleaved in favor of the proangiogenic form and was associated with increased microvessel density. Mechanistic studies revealed that multiple myeloma and proliferating endothelial cells can promote CgA C-terminal cleavage by activating the plasminogen activator/plasmin system. Moreover, cleaved and full-length forms could also counter balance the pro/antiangiogenic activity of each other in in vitro angiogenesis assays. These findings suggest that the CgA-angiogenic switch is activated in the BM of multiple myeloma patients and prompt further investigation of this CgA imbalance as a prognostic or therapeutic target. Cancer Res; 76(7); 1781–91. ©2016 AACR.

Published

2015

23. MICA Expressed by Multiple Myeloma and Monoclonal Gammopathy of Undetermined Significance Plasma Cells Costimulates Pamidronate-Activated γδ Lymphocytes

Author

Thomas Spies, Marina Ferrarini, Paolo Ticozzi, Daniela Belloni, Elisabetta Ferrero, Aurelio Vicari, Stefania Girlanda, Clara Sciorati, Moreno Tresoldi, Claudio Fortis, Federico Caligaris-Cappio, and Veronika Groh

Subjects

Male, Cancer Research, Myeloma protein, T-Lymphocytes, Lymphocyte, Plasma Cells, Paraproteinemias, Mevalonic Acid, Pamidronate, Antineoplastic Agents, Biology, Lymphocyte Activation, Antigen, immune system diseases, hemic and lymphatic diseases, Gammopathy, medicine, Humans, Multiple myeloma, Aged, Aged, 80 and over, Diphosphonates, Histocompatibility Antigens Class I, Receptors, Antigen, T-Cell, gamma-delta, Middle Aged, medicine.disease, NKG2D, stomatognathic diseases, medicine.anatomical_structure, Oncology, Immunology, Cancer research, Female, Bone marrow, Multiple Myeloma, Monoclonal gammopathy of undetermined significance

Abstract

Amino-biphosphonates (like pamidronate) activate human Vγ9/Vδ2 T lymphocytes and promote their cytotoxicity against multiple myeloma cells. T-cell receptor (TCR)–mediated effector functions of γδ cells are enhanced upon triggering of the activating receptor NKG2D by MICA, a stress-inducible antigen expressed by epithelial and some hematopoietic tumors, including multiple myeloma. Here we show that MICA was expressed not only by myeloma cell lines and by 6 of 10 primary multiple myeloma cells from patients but also by bone marrow plasma cells from all (six of six) patients with preneoplastic gammopathy (monoclonal gammopathy of undetermined significance, MGUS), a direct precursor of multiple myeloma. Moreover, compared with multiple myeloma plasma cells, MICA was expressed by MGUS plasma cells at significantly (P < 0.05) higher levels. MICA expressed by myeloma cell lines contributed to killing and IFN-γ production by Vγ9/Vδ2 cells only upon pamidronate treatment, suggesting a dual interaction between Vγ9/Vδ2 lymphocytes and multiple myeloma plasma cells involving both TCR triggering and NKG2D-mediated signals. Finally, MICA enhanced killing of freshly derived, pamidronate-treated multiple myeloma cells from patients by γδ cells, as indicated by the significantly (P < 0.05) higher γδ cytotoxicity against MICA-positive rather than MICA-negative multiple myeloma cells. Our results indicate that MICA expressed by monoclonal plasma cells is functional and correlates with disease stages, suggesting a role for the molecule in the immune surveillance against multiple myeloma. Moreover, pamidronate-activated Vγ9/Vδ2 lymphocytes can be exploited in the immune therapy of early stages multiple myeloma and possibly of premalignant disease.

Published

2005

24. Voriconazole and Non-Melanoma Skin Cancer after Allogeneic HSCT: Results of a Prospective Dedicated Follow-up Program in 302 Patients

Author

Sarah Marktel, Francesca Lunghi, Fabio Ciceri, Mara Morelli, Elena Guggiari, Magda Marcatti, Sara Mastaglio, Chiara Bonini, Serena Dalto, Fabio Giglio, Elisa Sala, Matteo Carrabba, Massimo Bernardi, Jacopo Peccatori, Andrea Assanelli, Francesca Pavesi, Luca Vago, Raffaella Greco, Tommaso Perini, Simona Piemontese, Francesca Lorentino, Consuelo Corti, Stefania Girlanda, Gabriele Antonarelli, Carlo Messina, and Maria Teresa Lupo-Stanghellini

Subjects

Voriconazole, medicine.medical_specialty, business.industry, medicine.medical_treatment, Immunology, Actinic keratosis, Retrospective cohort study, Cell Biology, Hematology, Hematopoietic stem cell transplantation, medicine.disease, Biochemistry, Surgery, Transplantation, Internal medicine, medicine, Basal cell carcinoma, Cumulative incidence, Skin cancer, business, medicine.drug

Abstract

Introduction Voriconazoleis a second-generationtriazolebroad-spectrum antifungal agent indicated in adults and children aged 2 years and above as treatment of invasive aspergillosis, treatment ofcandidaemiain non-neutropenic patients (pts), treatment of fluconazole-resistant serious invasive Candida infections, treatment of serious fungal infections caused byScedosporiumspp. and Fusarium spp. Voriconazoleis associated with a broad spectrum of dermatologically adverse reactions: it seems to be responsible for a multistep process beginning with acute and chronicphototoxicity, followed by actinic keratosis (AK), and finally skin squamous cell carcinoma (SCC), especially if therapy is maintained. Strictphotoprotectionis mandatory; drug replacement by anothertriazolemust be discussed in case of acutephototoxicity.Voriconazolemust be stopped in pts with chronicphototoxicity, and a long-term dermatologic follow-up of skin lesions is required even after withdrawal. It is now established thatvoriconazoleis an independent risk factor for the development of cutaneous malignancy in lung transplant recipients. Recently, a retrospective study from the Mayo Clinic (WojenskiDJ et al, Transplant Infectious Disease 2015, 17, 250-58) confirmed the association betweenvoriconazoleand SCC also after allo-HSCT (allogeneic hematopoietic stem cell transplantation) and identified cumulative days ofvoriconazoleas a risk factor for SCC. Methods The current study seeks to analyze the correlation betweenvoriconazoleexposure and non-melanoma skin cancer (NMSC) in our Center, where it is available an intensive dedicated follow-up after allo-HSCT to prevent and early detect second solid tumors. Results We analyze data prospectively collected at our Long-Term Follow-Up clinic between 2011 and 2016 including 302 adult pts with a minimum follow-up of 24 months. A written consent was given by pts allowing the use of medical records for research in accordance with the Declaration of Helsinki. Baseline characteristics of the 302 pts are outlined in table 1. In total, 25 pts developed NMSC - median time from allo-HSCT 42 months (range, 9 months - 20 years) - median follow-up after NMSC diagnosis 2 years (range, 2 months - 12 years). The estimated cumulative incidence of NMSC at 3 years was 3.2% and at 5 years 6.2%. At the dermatological annual evaluation 3 pts were presenting AK, only one progress to basal cell carcinoma (BCC), the 2 pts with AK are under dermatological follow-up. All pts were treated withvoriconazolefor more than 180 days. In total 19 pts were diagnosed with BCC and 6 pts with SCC. Five pts with SCC and 17 with BCC were treated withvoriconazole, overall 16/22 (4 SCC) for more than 180 days. All pts were treated according to standard practice for NMSC, unfortunately 1 pts deceased due to SCC progression. Only 2 pts were diagnosed and treated for NMSC before transplantation. Six pts had antecedent acute GvHD and 8 pts had antecedent moderate to severe chronic GvHD. History ofvoriconazoleexposure, cumulative days ofvoriconazoleuse, gender, age at transplant, TBI based conditioning regimen, acute/chronic GvHD and skin cancer pre-transplant were considered for analysis. Age at transplant above 48 years (p Conclusions Our experience confirms the correlation betweenvoriconazoleand occurrence of NMSC after allo-HSCT. Incidence of NMSC is higher than previously reported in registry reports, and the occurrence of NMSC in pts exposed tovoriconazoleseems to be precocious. This observation confirms the relevance of counseling and prevention of NMSC in patients benefiting fromvoriconazoleas a crucialmold-active antifungal prophylaxis and treatment. Disclosures Bonini: Molmed SpA: Consultancy; TxCell: Membership on an entity's Board of Directors or advisory committees. Ciceri:MolMed SpA: Consultancy.

Published

2016

25. Ex-vivo dynamic 3-D culture of human tissues in the RCCS™ bioreactor allows the study of Multiple Myeloma biology and response to therapy

Author

Nathalie Steimberg, Elisabetta Ferrero, Maurilio Ponzoni, Angiola Berenzi, Daniela Belloni, Marina Ferrarini, Stefania Girlanda, Federico Caligaris-Cappio, Giovanna Mazzoleni, Ferrarini, M, Steimberg, N, Ponzoni, Maurilio, Belloni, D, Berenzi, A, Girlanda, S, Caligaris Cappio, F, Mazzoleni, G, and Ferrero, E.

Subjects

Male, Vascular Endothelial Growth Factor A, Pathology, Cell Culture Techniques, Cancer Treatment, Cell Communication, Plasma Cell Disorders, Bortezomib, Rats, Sprague-Dawley, Hematologic Cancers and Related Disorders, Tissue culture, Bioreactors, Engineering, hemic and lymphatic diseases, Tumor Cells, Cultured, Multiple myeloma, Multidisciplinary, Neovascularization, Pathologic, Hematology, Middle Aged, Boronic Acids, Immunohistochemistry, Oncology, Pyrazines, Medicine, Female, Antiangiogenesis Therapy, Multiple Myeloma, Proteasome Inhibitors, Research Article, Biotechnology, medicine.drug, Adult, Genetic Markers, medicine.medical_specialty, Histology, Science, Bone Marrow Cells, Bioengineering, Biology, Bone and Bones, Angiopoietin-2, In vivo, medicine, Animals, Humans, Aged, Tibia, Beta-2 microglobulin, Chemotherapy and Drug Treatment, medicine.disease, Rats, Cell culture, Proteasome inhibitor, Cancer research, beta 2-Microglobulin, Ex vivo

Abstract

Three-dimensional (3-D) culture models are emerging as invaluable tools in tumor biology, since they reproduce tissue-specific structural features and cell-cell interactions more accurately than conventional 2-D cultures. Multiple Myeloma, which depends on myeloma cell-Bone Marrow microenvironment interactions for development and response to drugs, may particularly benefit from such an approach. An innovative 3-D dynamic culture model based on the use of the RCCS™ Bioreactor was developed to allow long-term culture of myeloma tissue explants. This model was first validated with normal and pathological explants, then applied to tissues from myeloma patients. In all cases, histological examination demonstrated maintenance of viable myeloma cells inside their native microenvironment, with an overall well preserved histo-architecture including bone lamellae and vessels. This system was then successfully applied to evaluate the cytotoxic effects exerted by the proteasome inhibitor Bortezomib not only on myeloma cells but also on angiogenic vessels. Moreover, as surrogate markers of specialized functions expressed by myeloma cells and microenvironment, β2 microglobulin, VEGF and Angiopoietin-2 levels, as well as Matrix Metalloproteases activity, were evaluated in supernatants from 3D cultures and their levels reflected the effects of Bortezomib treatment. Notably, determination of β2 microglobulin levels in supernatants from Bortezomib-treated samples and in patients'sera following Bortezomib-based therapies disclosed an overall concordance in the response to the drug ex vivo and in vivo. Our findings indicate, as a proof of principle, that 3-D, RCCS™ bioreactor-based culture of tissue explants can be exploited for studying myeloma biology and for a pre-clinical approach to patient-targeted therapy.

Published

2013

26. Facing the Rising Tide of Multidrug Resistant Gram-Negative Pathogens in Allogeneic HSCT with Nanosphere's Verigene® System

Author

Renée Pasciuta, Massimo Bernardi, Maria Chiara Barbanti, Maria Teresa Lupo Stanghellini, Massimo Clementi, Raffaella Greco, Laura Infurnari, Sarah Marktel, Carlo Messina, Fabio Giglio, Andrea Assanelli, Fabio Ciceri, Stefania Girlanda, Mara Morelli, Tommaso Perini, Matteo Carrabba, Jacopo Peccatori, Alessandra Forcina, Nicasio Mancini, Luca Vago, and Consuelo Corti

Subjects

medicine.medical_specialty, Hematology, medicine.diagnostic_test, business.industry, medicine.drug_class, medicine.medical_treatment, Immunology, Antibiotics, Cell Biology, Hematopoietic stem cell transplantation, medicine.disease, Biochemistry, Multiple drug resistance, Sepsis, Antibiotic resistance, Internal medicine, Medicine, Infection control, Blood culture, business

Abstract

Infections are the major cause of treatment-related morbidity and mortality in hematological patients, mostly after allogeneic hematopoietic stem cell transplantation (HSCT). Although the proportion of infection-related deaths has decreased in the past two decades, the alarming emergence of multidrug resistant (MDR) gram-negative pathogens, increasingly reported from various cancer treatment centers, represents a significant challenge. Dramatic infection-related mortality (64.4%) have been observed in allogeneic HSCT, due to carbapenem-resistant Klebsiella pneumoniae (CRKp). Timely microbiological diagnosis, active surveillance and early therapeutic strategies represent critical aspects for the management of MDR infections after allogeneic HSCT. In this study, we investigated whether a new molecular tool could be clinically relevant in the management of high-risk hematological patients, particularly in allogeneic HSCT. At San Raffaele Hematology and BMT Unit, all blood cultures positive for gram-negative bacteria in the last year, were prospectively collected and in parallel tested with Verigene® Gram-negative blood culture (BC-GN) test (Nanosphere, Northbrook, IL, USA), a microarray-based system allowing a rapid identification of genus, species, and genetic resistance determinants for a broad panel of gram-negative bacteria directly from positive blood cultures. Initially, we evaluated the reliability of the BC-GN test on 50 consecutive patients undergoing chemotherapy (n=16), autologous (n=4) or allogeneic (n=30) HSCT. The concordance with the standard blood culture was 100% considering the bacteria detectable by the system. Resistance genes (CTX-M or carbapenemases, as KPC and VIM) were detected in 15% of the isolates, and 100% were associated to the same phenotypic antibiotic resistance. We observed only 8% of phenotypic resistances not detected by the test, belonging to other kinds of resistance mechanisms not related to the genes included in the panel. Overall, Verigene BC-GN assay correctly identified 40/50 of all the gram-negative pathogens (3 Klebsiella pneumonia, 25 Escherichia coli, 5 Pseudomonas aeruginosa, 4 Acinetobacter spp, 1 Enterobacter spp, 2 Citrobacter spp), yielding a general sensitivity of 80%, which increased to 100% if only the genera and species included in the panel were considered. Then, we examined the potential clinical impact of this molecular approach in allogeneic HSCT recipients (n=30), either in an inpatient (n=24) or outpatient (n=6) management. As far as transplanted patients' care is concerned, the BC-GN test strongly influenced clinical practice. In the majority of cases we were able to early start targeted antibiotic therapy (78%), sparing or interrupting non-specific antimicrobial therapy (56%), thus reducing useless and/or potentially more toxic antibiotics and their potential impact in favouring antimicrobial resistance. Moreover, in 5/8 cases the 'triple therapy', recommended at fever onset for all CRKp-colonized patients, was spared thanks to BC-GN test results, showing the absence of resistance markers. In 95% of patients immunosuppressive prophylaxis was not reduced, thanks to a rapid control of sepsis, avoiding the risk of undesired GVHD. Early contact isolation was possible in 32% of patients, preventing the spread of infections from a patient to the others and allowing infection control. Infection-related mortality was reported only in one patient. An outpatient management was continued in 3/6 haemodynamically stable patients, avoiding unnecessary hospitalization. While conventional microbiological methods required 2-4 days, BC-GN test provided detailed results within 2 hours from blood culture positivity. The mean gain in time comparing BC-GN test to fast blood cultures was reported to be about 20 hours. In our experience, this new microarray test has provided highly accurate identification results and earlier potentially important information on antibiotic susceptibility, both confirming and excluding the presence of an MDR phenotype. The contribution to a rapid diagnosis and an earlier targeted antimicrobial therapy of Verigene BC-GN test is of high clinical relevance for the infections by MDR bacteria, a significant public health challenge worldwide, particularly in allogeneic HSCT recipients. Disclosures No relevant conflicts of interest to declare.

Published

2015

27. ELISPOT-IFN-gamma assay instead of tuberculin skin test for detecting latent Mycobacterium tuberculosis infection in rheumatic patients candidate to anti-TNF-alpha treatment

Author

Manuela Ratti, Elena Baldissera, Claudio Fortis, Maria Grazia Sabbadini, Patrizia Aiello, Paola Mantegani, and Stefania Girlanda

Subjects

Adult, Male, medicine.medical_specialty, Enzyme-Linked Immunospot Assay, Tuberculosis, Tuberculin, Sensitivity and Specificity, Mycobacterium tuberculosis, Rheumatology, Latent Tuberculosis, Internal medicine, Rheumatic Diseases, medicine, Humans, biology, Latent tuberculosis, business.industry, Tuberculin Test, Tumor Necrosis Factor-alpha, ELISPOT, Isoniazid, Antibodies, Monoclonal, General Medicine, Middle Aged, bacterial infections and mycoses, medicine.disease, biology.organism_classification, Immunology, biology.protein, Female, Antibody, business, medicine.drug

Abstract

In rheumatic patients candidate to anti-TNF-alpha treatment, there is an increased risk of developing tuberculosis (TB). The tuberculin skin test (TST), the standard diagnostic test for latent tuberculosis infection (LTBI), suffers low specificity and sensitivity. Here, we compared the performance characteristics of an in-house ELISPOT-IFN-gamma assay (using a restricted pool of Mycobacterium tuberculosis-specific peptides or MTP) to TST for the diagnosis of LTBI in 69 rheumatic patients candidate to anti-TNF-alpha treatment and in 60 healthy LTBI individuals. Among the 69 patients enrolled, 17 (25%) had a positive TST response and 15 (22%) a positive ELISPOT-MTP response. Among the patients with a positive TST result, eight had a positive and nine a negative ELISPOT-MTP response, whereas among the 49 patients with a negative TST result, 42 were ELISPOT-MTP negative, but seven (14%) were ELISPOT-MTP positive, with three indeterminate results. The agreement between the two tests was poor (k = 0.341, 95% CI = 0.060 to 0.622) and the test of symmetry was not significant (P = 0.8). Considering the ELISPOT assay, rheumatic patients had a reduced number of spot-forming cells after stimulation of lymphocytes with PHA or PPD when compared with healthy LTBI individuals. Thus, the ELISPOT-IFN-gamma assay performs better than the TST in recognizing patients with LTBI, on one hand reducing the number of patients submitted to isoniazid prophylaxis, and on the other hand, since the assay is less biased by immunosuppressive regimens than TST, recognizing LTBI patients among those with a negative TST response.

Published

2010

28. Graft-Versus-Host Disease after Haploidentical Stem Cell Transplantation in High Risk Haematological Diseases: A 10-Years Evaluation at San Raffaele Scientific Institute

Author

Sarah Marktel, Raffaella Greco, Roberto Crocchiolo, Lara Crucitti, Massimo Bernardi, Claudio Bordignon, Francesca Lunghi, Alessandra Forcina, Fabio Giglio, Francesca Pavesi, Fabio Ciceri, Magda Marcatti, Tommaso Perini, Jacopo Peccatori, Alessia Orsini, Elena Guggiari, Stefania Girlanda, Andrea Assanelli, Chiara Bonini, Maria Teresa Lupo-Stanghellini, Matteo Carrabba, and Consuelo Corti

Subjects

education.field_of_study, medicine.medical_specialty, business.industry, Mortality rate, Immunology, Population, Cell Biology, Hematology, medicine.disease, Biochemistry, Comorbidity, Transplantation, surgical procedures, operative, Graft-versus-host disease, immune system diseases, Prednisone, Internal medicine, medicine, Complication, education, business, medicine.drug, Cause of death

Abstract

Introduction Haematopoietic stem cell transplantation (HSCT) is the only curative option for patients (pts) affected by high-risk haematological diseases (HRHD). However, the availability of a match donor is still an unmet-medical need. Recently alternative donor transplantations have been broadly exploited, reaching results similar to transplants from a well match donor. Anyway, whoever the donor is, the most important complication remains Graft-versus-Host Disease (GvHD). Aim of the study We evaluated incidence, characterization, stratification, treatment, treatment response and outcome at medium and long-term follow-up for both acute (a-) and chronic (c-) GvHD in haploidentical setting. We also evaluated the impact of the NIH consensus criteria on GvHD in a routine clinical application to confirm their feasibility in daily practice and not only in clinical trials use. Methods A population of 257 pts was selected from our Institutional database on the basis of their having an HRHD with indication to allogeneic HSCT and having received a HSCT from an haploidentical family donor without exclusion. HSCT were performed between January 2004 and December 2013 at our Center. No distinction between first HSCT or subsequent one was made, all consecutive haploidentical HSCT were captured. Results Time of median follow-up was 10 months; 1-year overall-survival (OS) was 46%, with better outcome for pts transplanted in complete remission (p 0.0001) confirming disease status as the leading factor for overall outcome. Transplant related mortality was estimated to be 30% at 1 year and the leading cause of death was infections. The 6-months a-GvHD incidence was 45% (119/257) - median day of presentation 21 post HSCT (range 8-89). Late-onset a-GvHD was documented in 15 pts. Grade I GvHD was documented in 33 pts (27.7%), grade II in 44 (37%), grade III-IV in 36 (30.3%) – 6 not evaluable. Skin was the most frequently involved organ (77.3%), both as single manifestation or combined. One-hundred and five pts received a first line therapy based on high-dose prednisone (2mg/Kg) and 37/105 completely abrogated the a-GvHD. At a 3-months evaluation 46% of affected pts showed complete resolution of a-GvHD, while the mortality rate was 29%. C-GvHD affected 69/257 pts and 1-year risk of onset was 25% - median day of presentation was 139 post HSCT (range 40-809) and 36/69 pts were off immunosuppressive therapy (52.3%) at presentation. According to onset presentation 53.7% were de novo, 24.6% progressive and 18.8% quiescent GvHD. Forty-one pts (59.5%) presented at declaration with overlap features. The most frequent involved organ was skin (grade I to III), as reported in 53 pts (76.8%). Skin lesions were usually accompanied with mouth lesions (35 pts – 50.7%), liver (23 pts – 33.3%) or eyes (27 pts – 39.1%) dysfunctions. The median number of involved organs was 3 (range 1-7). Mild c-GvHD was diagnosed in 10 pts (14.5%), who received topical therapy. Fifty-nine pts – diagnosed with moderate (32, 46.4%) or severe (27, 39.1%) - received a systemic treatment for c-GvHD: prednisone 1 mg/Kg alone or 0,5 mg/kg plus mTOR- or calcineurin-inhibitor for pts that were not likely to tolerate high dose steroid due to comorbidity (namely active infections, diabetes, cardiovascular diseases). At a 12-months evaluation the overall response was 48% (complete resolution 25%, partial resolution 23%), while the mortality rate was 36%. The Landmark analysis of OS at 3 months after HSCT shows that a-GvHD affected pts had a worse outcome (p= 0,068), on the contrary the Landmark analysis of OS at 18 months shows that c-GvHD did not associate with a worse outcome (p ns) but the follow up is still short. Confirming previous reports, overlap c-GvHD was related to worse survival in comparison with classic c-GvHD (p 0.0098). Conclusion Haploidentical HSCT is a valid and feasible option for pts in need of a transplant. GvHD is manageable after haploidentical HSCT, as in full matched setting. Better knowledge and insight in a/c-GvHD are providing advance in improving pts outcome. The NIH-consensus criteria are manageable in daily clinical practice and able to translate in a tailored approach to GvHD with benefit on general outcome. Further advance in the development of specific biomarkers for GvHD will provide additional crucial information for management, diagnosis and prognostication in GvHD. Figure 1 Figure 1. Disclosures Bonini: MolMed S.p.A.: Consultancy. Bordignon:MolMed: Employment.

Published

2014

29. WT1 Transcripts Is a Powerful Leukemia Marker to Predict Early Relapse After Allogeneic Haematopoietic Stem Cell Transplantation

Author

Francesca Lunghi, Cristina Tresoldi, Chiara Bonini, Magda Marcatti, Simona Malato, Fabio Giglio, Elena Guggiari, Matteo Carrabba, Alessandro Crotta, Barbara Forno, Jacopo Peccatori, Maria Teresa Lupo Stanghellini, Claudio Bordignon, Stefania Girlanda, Milena Coppola, Massimo Bernardi, Katharina Fleischhauer, Raffaella Greco, Marta Bruno Ventre, Simona Piemontese, Fabio Ciceri, Andrea Assanelli, Daniela Clerici, Consuelo Corti, Carlo Messina, and Sara Mastaglio

Subjects

Oncology, medicine.medical_specialty, business.industry, medicine.medical_treatment, Immunology, Cell Biology, Hematology, Hematopoietic stem cell transplantation, Treosulfan, medicine.disease, Biochemistry, Donor lymphocyte infusion, Fludarabine, Transplantation, Leukemia, medicine.anatomical_structure, Graft-versus-host disease, Internal medicine, medicine, Bone marrow, business, medicine.drug

Abstract

Abstract 4488 Introduction Definition of leukemia remission requires the lack of disease markers at sub-microscopic level. This is highly important after a potentially curative approach as allogeneic hematopoietic stem cell transplant (HSCT), where early detection of relapse at molecular level may lead to modulation of immunosuppressive therapy or donor lymphocyte infusion (DLI). In AML various approaches has been used to define MRD, but still the majority of AML cases do not have a useful and sensitive MRD marker. Over-expression of Wilms' tumor gene 1 (WT1) in leukemic blasts has been reported in >80% of AML and >40% of MDS. Physiologic hematopoietic stem cell compartments also express WT1, however, a ‘malignant’ WT1 expression can be clearly distinguished based on quantitative detection methods such as semiquantitative RT-PCR. Quantification of WT1 expression levels can detect frequencies of leukemic cells in bone marrow (BM) and peripheral blood (PB) as low as 10-3 and 10-5, respectively. Therefore WT1 expression levels provide a new marker for leukemic blast cells regardless of the type of leukemia especially in the relevant percentage of patients that lacks a specific molecular marker of their disease and thus may be a useful marker MRD and may predict the relapse after allogeneic HSCT. Materials and methods We measured quantitative expression of WT1 at diagnosis, before and after allogeneic transplant monthly for the first six months and then every three months. The quantitative assessment of the WT1 transcript amount was performed by real-time quantitative polymerase chain reaction (RQ-PCR). Results Our study included 19 AML and 6 MDS pts who underwent allogeneic HSCT in our Institute between 12/2007 and 6/2009. Median age at diagnosis was 49 years (range 22-68). Bone marrow samples at diagnosis showed a WT1 median expression level of 5851.66 copies (range 77.98-31203.57). Fifteen pts (60%) had a specific cytogenetic marker that could allow MRD monitoring. At HSCT 17 pts (68%) were in CR, 5 (20%) had a refractory or relapsed disease, while 3 (12%) were transplanted upfront. Six pts (24%) received grafts from a matched sibling donors, 6 (24%) were transplanted from a matched unrelated donor (MUD), 10 (40%) from a familiar haploidentical donor and 3 (12%) received a cord blood unit. Myeloablative conditioning regimen consisted of Treosulfan 42 g/sqm, Fludarabine 150 mg/sqm, ALG 30 mg/kg and Rituximab 500 mg (last two drugs only for alternative donors). After HSCT a rapid decline of WT1 expression levels was observed in all pts that obtained or maintained a condition of CR. Two pts (8%) relapsed and both had an increase in WT1 expression before relapse. In the first relapsed pt, analysis of WT1 showed a dramatically increase between pre transplant level and day +28, while STR showed 100% donor chimerism. Relapse occurred on day +43, still on IST, with 69% of blast at AM evaluation and 40% donor chimerism. This pt was successfully reinduced with chemotherapy followed by allogeneic PBSC infusion without GvHD profilaxys obtaining a rapid reduction of WT1 (43.66). The pt developed GvHD that required a new IST, confirming a strong immune-surveillance of HSCT. The second pt was still on immunosuppressive treatment (IST) at the time of relapse (+136). WT1 in BM on day +30 was 30 cp and then increased gradually to 167 and 190 cp on day +67 and +102, respectively. Cytogenetic analysis and STR chimerism still showed a cCR with 100% donor chimerism. At relapse AM showed 10% blasts, WT1 expression level was 7447 cp with >95% donor chimerism. IST was discontinued and one month later WT1 expression level decreased to 1640 with >95% donor chimerism. In this situation we reasoned that DLI was the best available treatment. The total dose of donor T cell infused was 5 ×105 CD3/Kg. This procedure allowed an immune-mediated leukemia control with reduction of WT1 (1.58), cCR and 100% donor chimerism. Conclusions These data show that WT1 may be useful as a non-specific leukemia marker for monitoring MRD in AML and MDS after allogeneic HSCT and should enable the detection of early relapse allowing intervention at a more favourable stage than at overt relapse. We observed a complete concordance between WT1 expression levels and status of AML before and after allogeneic HSCT. Based on these results cases with increase of WT1 levels after HSCT and without GVHD may be candidate to immune intervention such as discontinuation of immunosuppression and/or DLI. Disclosures: Bonini: MolMed S.p.A.: Consultancy.

Published

2009

30. Allogeneic Transplantation with a Treosulfan-Fludarabine Conditioning Regimen Is Feasible and Effective in Elderly Patients with Refractory or Relapsed Acute Myeloid Leukaemia (AML) and Myelodysplastic Syndrome (MDS); Preliminary Results From a Single Center Experience

Author

Maria Teresa Lupo Stanghellini, Sara Mastaglio, Massimo Bernardi, Michela Tassara, Consuelo Corti, Fabio Giglio, Alessandro Crotta, Elena Guggiari, Stefania Girlanda, Fabio Ciceri, Carlo Messina, Andrea Assanelli, Daniela Clerici, Simona Malato, Barbara Forno, Jacopo Peccatori, Matteo Carrabba, Chiara Bonini, and Annalisa Ruggeri

Subjects

medicine.medical_specialty, Performance status, business.industry, medicine.medical_treatment, Immunology, Induction chemotherapy, Cell Biology, Hematology, Hematopoietic stem cell transplantation, Treosulfan, Single Center, Biochemistry, Gastroenterology, Surgery, Fludarabine, Transplantation, hemic and lymphatic diseases, Internal medicine, medicine, Cytarabine, business, medicine.drug

Abstract

Abstract 4318 Background the majority of AML and poor risk MDS cases in the elderly (>60 years) are resistant to induction chemotherapy or relapse after initial response; thereafter, most of these patients (pts) receive only supportive treatments, with an expected survival of few weeks. Allogeneic (allo) stem cell transplantation (SCT) could be the only potentially salvage strategy; actually, for the high probability of letal toxicites due to the conditioning regimen, acute graft-versus-host disease (aGvHD) and infections, these pts are rarely offered this procedure. Since 2005, we have transplanted 12 pts, age>60, with refractory or relapsed AML/MDS, from an allogeneic donor. Data on feasibility and outcome are here reported. Aim to retrospectively evaluate data on alloSCT in elderly pts with refractory or relapsed AML and MDS, transplanted at our Institute. Patients and Methods period 9/2005 to 4/2009, 12 pts, median age 65 (61-72). Performance status (Karnofsky): median 90% (80-100), HCT-CI: median score 1 (0-4). Diagnosis (WHO): AML 3, AMLMD 4, RAEB2 2, MDS/MPD 2, therapy-related AML 1. Median number of chemo cycles before SCT: 2 (1-7), all pts received at least 1 cycle with intermediate or high-dose cytarabine, 2 pts also received an autologous SCT. Donors: matched sibling 2, matched unrelated 2, related haploidentical 7, cord blood 1. Disease status at SCT: primary refractory 7, relapsed 5. Conditioning regimen: treosulfan (TREO) 14 g/sqm for 3 days, fludarabine (FLU) 30 mg/sqm for 5 days, ATG 10 mg/kg for 3 days for SCT from alternative donors. GvHD prophylaxis: T-cell depletion in 2 cases, cyclosporine (CSA)/methotrexate in 7, rapamycin/mycophenolate mofetil (MMF) in 3. Results 11/12 (92%) pts engrafted and were in CR at day +30, with 95-100% donor chimerism (VNTR). Deaths within day 30 and day 100 were 0 and 3 (25%), respectively. Acute GvHD: 6 pts (55%), grade II (3) or III (3), only of skin in 3 cases, skin+liver in 1, only intestinal in 2. Relapses were 4 (36%). Overall TRM was 25% (3 pts), with all deaths due to infections during immunosuppression for aGVHD; 5 more pts died because of disease progression. Median OS from SCT of all 12 pts was 180 (56-1150) days, DFS (11 pts) was 128 (24-1114) days. At last follow-up (FU) 4 pts (33%) are alive, all in CR with a median FU of 406 (128-1150) days. Conclusions alloSCT proved to be feasible in our elderly pts with AML/MDS refractory to induction or relapsed after initial complete remission. Early letal toxicities, due to the conditioning treatment, were absent; aGVHD, infections and relapses were the principal causes of mortality. Up to now, prolonged survival (>1 year) free from disease has been obtained in 25% of pts; of the 4 pts alive in CR, only 1 is receiving immunosuppression (CSA), for chronic GVHD. In conclusion, the TREO-FLU association showed a reduced-toxicity profile in these frail pts and a substantial anti-leukemic effect. Better prevention of aGVHD should be obtained, expecially after SCT from alternative donors, possibly with the rapamycin/MMF combination, which we are currently investigating at our Institute. AlloSCT after TREO-FLU conditioning can be considered an effective option for AML/MDS elderly pts with active disease after failure of previous intensive treatments. Disclosures: bonini: MolMed S.p.A.: Consultancy.

Published

2009

31. A Survey on Clinical and Biological Characteristic and Therapy Management of an Italian Series of 455 Adult Patients with Systemic Mastocytosis on Behalf of Italian Registry of Mastocytosis

Author

Roberta Zanotti, Vittoria Cova, Alberto Bosi, Anna Artuso, Chiara Elena, Simona Muratori, Federica Irene Grifoni, Massimo Triggiani, Omar Perbellini, Serena Merante, Elena Maria Elli, Fabio Almerigogna, Diomira Magliacane, Marina Mauro, Giovanni Martinelli, Cristina Papayannidis, Massimiliano Bonifacio, Lisa Pieri, G Cortellini, L. Lunardon, Caterina De Benedittis, Patrizia Bonadonna, Maurizio Severino, Stefania Girlanda, Agostino Cortelezzi, Simona Soverini, Federica Scarfì, Maria Loredana Iorno, Alessandro M. Vannucchi, Michela Rondoni, and Lisa Pieri, Patrizia Bonadonna, Chiara Elena, Cristina Papayannidis, Federica Irene Grifoni, Michela Rondoni, Stefania Girlanda, Marina Mauro, Diomira Magliacane, Elena Maria Elli, Maria Loredana Iorno, Maurizio Severino, Fabio Almerigogna, Federica Scarfì, Massimiliano Bonifacio, Omar Perbellini, Anna Artuso, Simona Soverini, Caterina De Benedittis, Simona Muratori, Luisa Lunardon, Vittoria Cova, Gabriele Cortellini, Alberto Bosi, Agostino Cortelezzi, Giovanni Martinelli, Massimo Triggiani, Serena Merante, Alessandro Maria Vannucchi, Roberta Zanotti

Subjects

medicine.medical_specialty, Pathology, Thrombocytosis, business.industry, Cutaneous Mastocytosis, Immunology, Retrospective cohort study, Cell Biology, Hematology, systemic mastocytosis, medicine.disease, Biochemistry, Gastroenterology, Imatinib mesylate, epidemiology, Internal medicine, Medicine, Systemic mastocytosis, business, Myelofibrosis, Myeloproliferative neoplasm, Multiple myeloma, Mastocytosis

Abstract

Systemic mastocytosis (SM) is a rare myeloproliferative neoplasm characterized by proliferation and hyperactivation of clonal mast cells. Clinical manifestations are heterogeneous and encompass cutaneous lesions, gastrointestinal alterations, osteoporosis, anaphylaxis and involvement of bone marrow and other organs due to neoplastic mast cells (MC) infiltration. As consequence, diagnosis may be difficult and patients (pts) are often evaluated by different specialists before the disease is recognized. To date, only few studies (Lim 2009, Escribano 2009, Cohen 2014) described relatively large series of pts with SM. We performed a multicentre retrospective study to evaluate clinical and biological features and therapeutic management in a large series of pts from 10 Italian centres experienced in management of SM and organized in multidisciplinary groups of specialists. We collected 455 pts diagnosed with SM according to WHO criteria. Additionally 26 pts with mastocytosis in the skin (MIS) evaluated with BM examination did not fulfil criteria for SM, leading to diagnosis of Cutaneous Mastocytosis (CM); however 2/26 pts with CM had both cKITD816V mutation and CD2/CD25 expression on MC in BM, additional 3 showed either cKITD816V or CD2/CD25. Moreover, we found 22 pts without MIS but with features of monoclonal mast cell activation syndrome. Of the 455 pts with WHO-SM (male 56%), 252 (55%) had MIS: median age at MIS diagnosis (dg) was 37 years (y) (range 0-79), while at SM dg it was 46.5 (range 18-82). Time from onset of MIS to dg of SM was 9 y (range 0-43). In 18/252 pts (7%) MIS occurred before age of 18 y (median 9, range 0-17) and persisted over childhood. Median age at dg of SM without MIS (203/455 pts, 45%) was older: 54 y, range 19-79 (p Disclosures Martinelli: Novartis: Consultancy, Speakers Bureau; BMS: Consultancy, Speakers Bureau; Pfizer: Consultancy; ARIAD: Consultancy.