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4. Premature aging of the immune system affects the response to SARS-CoV-2 mRNA vaccine in β-thalassemia: role of an additional dose

Author

Rita Carsetti, Chiara Agrati, Valeria Maria Pinto, Barbara Gianesin, Rita Gamberini, Monica Fortini, Susanna Barella, Rita Denotti, Silverio Perrotta, Maddalena Casale, Aurelio Maggio, Lorella Pitrolo, Eleonora Tartaglia, Eva Piano Mortari, Francesca Colavita, Vincenzo Puro, Massimo Francalancia, Valeria Marini, Marco Caminati, Filippo Mazzi, Lucia De Franceschi, Gian Luca Forni, Franco Locatelli, Carsetti, Rita, Agrati, Chiara, Pinto, Valeria Maria, Gianesin, Barbara, Gamberini, Rita, Fortini, Monica, Barella, Susanna, Denotti, Rita, Perrotta, Silverio, Casale, Maddalena, Maggio, Aurelio, Pitrolo, Lorella, Tartaglia, Eleonora, Mortari, Eva Piano, Colavita, Francesca, Puro, Vincenzo, Francalancia, Massimo, Marini, Valeria, Caminati, Marco, Mazzi, Filippo, De Franceschi, Lucia, Forni, Gian Luca, and Locatelli, Franco

Subjects
thalassemia, Vaccines, Synthetic, COVID-19 Vaccines, SARS-CoV-2, beta-Thalassemia, Immunology, COVID-19, Aging, Premature, Cell Biology, Hematology, Antibodies, Viral, Biochemistry, Settore MED/38 - PEDIATRIA GENERALE E SPECIALISTICA, Immune System, Humans, mRNA Vaccines
Abstract

Patients with beta-thalassemia show 5-fold increase in agestandardized lethality due to SARS-CoV-2 infection, representing a high-risk population compared with age- and sex-matched healthy subjects.(1) Vaccination against SARS-CoV-2 is crucial to reduce mortality and morbidity of frail patients.(2) Up to now, limited data have been available on the responses of patients with beta-thalassemia immunized with anti-SARS-CoV-2 mRNA vaccines.(3)

Published
2022

9. Identification of the Proteasome Subunits PSMB4 and PSMD4 As Novel Targets in Multiple Myeloma Patients Carrying 1q21 Amplification

Author

Burroughs Garcia, Jessica, primary, Storti, Paola, additional, Iannozzi, Nicolas Thomas, additional, Notarfranchi, Laura, additional, Toscani, Denise, additional, Marchica, Valentina, additional, Raimondi, Vincenzo, additional, Agnelli, Luca, additional, Franceschi, Valentina, additional, Todaro, Giannalisa, additional, Lungu, Oxana, additional, Bernardi, Matia, additional, Scita, Matteo, additional, Sammarelli, Gabriella, additional, Donofrio, Gaetano, additional, Dalla Palma, Anna Benedetta, additional, and Giuliani, Nicola, additional

Published
2022
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10. Colchicine Protects Against Cardiomyopathy in Humanized Mouse Model for Sickle Cell Disease

Author

Federti, Enrica, primary, Iatcenko, Iana, additional, Ghigo, Alessandra, additional, Mattè, Alessandro, additional, Riccardi, Veronica, additional, Andolfo, Immacolata, additional, Siciliano, Angela, additional, Mazzi, Filippo, additional, Stella, Manuela, additional, Robbiano, Luigi, additional, Pinto, Valeria, additional, Iolascon, Achille, additional, Forni, Gian Luca, additional, and De Franceschi, Lucia, additional

Published
2022
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11. Resolvins Modulate Netosis and Autoimmunity in Sickle Cell Disease

Author

Mattè, Alessandro, primary, Recchiuti, Antonio, additional, Federti, Enrica, additional, Mazzi, Filippo, additional, Ceolan, Jacopo, additional, Porreca, Annamaria, additional, Di Nicola, Marta, additional, Menotti, Sofia, additional, Alivernini, Stefano, additional, Brugnara, Carlo, additional, and De Franceschi, Lucia, additional

Published
2022
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12. Premature aging of the immune system affects the response to SARS-CoV-2 mRNA vaccine in β-thalassemia: role of an additional dose

Author

Carsetti, Rita, primary, Agrati, Chiara, additional, Pinto, Valeria Maria, additional, Gianesin, Barbara, additional, Gamberini, Rita, additional, Fortini, Monica, additional, Barella, Susanna, additional, Denotti, Rita, additional, Perrotta, Silverio, additional, Casale, Maddalena, additional, Maggio, Aurelio, additional, Pitrolo, Lorella, additional, Tartaglia, Eleonora, additional, Mortari, Eva Piano, additional, Colavita, Francesca, additional, Puro, Vincenzo, additional, Francalancia, Massimo, additional, Marini, Valeria, additional, Caminati, Marco, additional, Mazzi, Filippo, additional, De Franceschi, Lucia, additional, Forni, Gian Luca, additional, and Locatelli, Franco, additional

Published
2022
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13. Multiple clinical forms of dehydrated hereditary stomatocytosis arise from mutations in PIEZO1

Author

Andolfo, Immacolata, Alper, Seth L., De Franceschi, Lucia, Auriemma, Carla, Russo, Roberta, De Falco, Luigia, Vallefuoco, Fara, Esposito, Maria Rosaria, Vandorpe, David H., Shmukler, Boris E., Narayan, Rupa, Montanaro, Donatella, D'Armiento, Maria, Vetro, Annalisa, Limongelli, Ivan, Zuffardi, Orsetta, Glader, Bertil E., Schrier, Stanley L., Brugnara, Carlo, Stewart, Gordon W., Delaunay, Jean, and Iolascon, Achille

Published
2013
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14. Resolvins Modulate Netosis and Autoimmunity in Sickle Cell Disease

Author

Alessandro Mattè, Antonio Recchiuti, Enrica Federti, Filippo Mazzi, Jacopo Ceolan, Annamaria Porreca, Marta Di Nicola, Sofia Menotti, Stefano Alivernini, Carlo Brugnara, and Lucia De Franceschi

Subjects
Immunology, Cell Biology, Hematology, Biochemistry
Published
2022

16. Identification of the Proteasome Subunits PSMB4 and PSMD4 As Novel Targets in Multiple Myeloma Patients Carrying 1q21 Amplification

Author

Jessica Burroughs Garcia, Paola Storti, Nicolas Thomas Iannozzi, Laura Notarfranchi, Denise Toscani, Valentina Marchica, Vincenzo Raimondi, Luca Agnelli, Valentina Franceschi, Giannalisa Todaro, Oxana Lungu, Matia Bernardi, Matteo Scita, Gabriella Sammarelli, Gaetano Donofrio, Anna Benedetta Dalla Palma, and Nicola Giuliani

Subjects
Immunology, Cell Biology, Hematology, Biochemistry
Published
2022

18. PSMB4 and PSMD4 Are Correlated with 1q21 Amplification in CD138 + Plasma Cells: New Potential Druggable Targets in Myeloma Patients

Author

Burroughs-Garcia, Jessica, primary, Storti, Paola, additional, Agnelli, Luca, additional, Toscani, Denise, additional, Marchica, Valentina, additional, Sammarelli, Gabriella, additional, Todaro, Giannalisa, additional, Raimondi, Vincenzo, additional, Franceschi, Valentina, additional, Soressi, Naomi, additional, Dalla Palma, Anna Benedetta, additional, Notarfranchi, Laura, additional, Donofrio, Gaetano, additional, and Giuliani, Nicola, additional

Published
2021
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20. Trial in Progress: The Randomized, Double-Blind, Placebo-Controlled Phase IIa CROSSWALK-c Trial Evaluating the Efficacy of Crovalimab As Adjunct Treatment in the Prevention of Vaso-Occlusive Episodes (VOEs) in Patients with Sickle Cell Disease (SCD)

Author

Callaghan, Michael, primary, Ataga, Kenneth I., additional, De Franceschi, Lucia, additional, Minniti, Caterina, additional, Balachandran, Nadiesh, additional, Imbs, Diane-Charlotte, additional, Perretti, Thomas, additional, Ramos, Julia, additional, Sostelly, Alexandre, additional, and Bartolucci, Pablo, additional

Published
2021
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21. Nrf2 Plays a Key Role in Iron-Overload Cardiomyopathy

Author

Federti, Enrica, primary, Vinchi, Francesca, additional, Iatcenko, Iana, additional, Ghigo, Alessandra, additional, Mattè, Alessandro, additional, Cedrick, Serge, additional, Siciliano, Angela, additional, Chiabrando, Deborah, additional, Tolosano, Emanuela, additional, Vance, S. Zebulon, additional, Riccardi, Veronica, additional, Andolfo, Immacolata, additional, Iolascon, Achille, additional, and de Franceschi, Lucia, additional

Published
2021
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22. Trial in Progress: The Randomized, Double-Blind, Placebo-Controlled Phase Ib CROSSWALK-a Trial Evaluating the Safety of Crovalimab for the Management of Acute Uncomplicated Vaso-Occlusive Episodes (VOEs) in Patients with Sickle Cell Disease (SCD)

Author

Bartolucci, Pablo, primary, Ataga, Kenneth I., additional, Callaghan, Michael U., additional, De Franceschi, Lucia, additional, Minniti, Caterina, additional, Alexandrou, Ari, additional, Imbs, Diane-Charlotte, additional, Fox, Richard, additional, Patel, Himika, additional, Sostelly, Alexandre, additional, and Schimmel, Jonathan, additional

Published
2021
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23. Hodgkin lymphoma in the Swiss HIV Cohort Study

Author

Clifford, Gary M., Rickenbach, Martin, Lise, Mauro, Dal Maso, Luigino, Battegay, Manuel, Bohlius, Julia, Boffi El Amari, Emmanuelle, Karrer, Urs, Jundt, Gernot, Bordoni, Andrea, Ess, Silvia, and Franceschi, Silvia

Published
2009
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24. PYGO2-MDR1 Axis in Multiple Myeloma Patients with 1q21 Amplification As Promising Target to Overcome Carfilzomib Resistance

Author

Iannozzi, Nicolas Thomas, Burroughs Garcia, Jessica, Marchica, Valentina, Franceschi, Valentina, Toscani, Denise, Vescovini, Rosanna, Raimondi, Vincenzo, Lungu, Oxana, Todaro, Giannalisa, Sammarelli, Gabriella, Scita, Matteo, Librale, Federica, Dalla Palma, Anna Benedetta, Donofrio, Gaetano, Storti, Paola, Agnelli, Luca, Pruneri, Giancarlo, and Giuliani, Nicola

Published
2023
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26. Trials in Progress: The Randomized, Double-Blind, Placebo-Controlled Phase 1b CROSSWALK-a and Phase 2a CROSSWALK-c Trials - Crovalimab for the Treatment and Prevention of Vaso-Occlusive Episodes in Sickle Cell Disease

Author

Salvino, Marco Aurelio, Antmen, Bulent, Chite Asirwa, Frederick, Chonat, Satheesh, De Franceschi, Lucia, Eleftheriou, Perla, Inati, Adlette, Mahlangu, Johnny, Nur, Erfan, Payán-Pernía, Salvador, Charania, Asad, Gradinaru, Diana, Hsia, Allison, Luder, Yves, Perretti, Thomas, Srekovic, Sasha, and Bartolucci, Pablo

Published
2023
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29. Luspatercept in the Treatment of Beta Thalassemia in Italy: Lights and Shadows in Clinical Practice

Author

Gianesin, Barbara, Rosso, Rosamaria, Lisi, Roberto, Zappu, Antonietta, Motta, Irene, Longo, Filomena, Pinto, Valeria, Sanna, Paola Maria Grazia, De Franceschi, Lucia, Ruffo, Giovan Battista, DI Maggio, Rosario, Bulla, Anna, Di Giorgio, Mary Ann, Denotti, Anna Rita, Panzieri, Daniele Lello, Culcasi, Martina, Quintino, Sabrina, Marchisio, Andrea, Mazzi, Filippo, Miciotto, Francesca, Barone, Rita, Di Raimondo, Francesco, Ferraresi, Marta, Marchetti, Beatrice, and Origa, Raffaella

Published
2023
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30. Fyn Kinase Is Involved in EPO Receptor Signaling and Is Required to Harmonize the Response to Oxidation

Author

Mohandas Narla, Emanuela Tolosano, Lucia De Franceschi, Deborah Chiabrando, Elisabetta Beneduce, Alessandro Matte, Serge Cedrick, Angela Siciliano, Achille Iolascon, and Luigia De Falco

Subjects
Chemistry, Immunology, Autophagy, hemic and immune systems, Cell Biology, Hematology, environment and public health, Biochemistry, Cell biology, medicine.anatomical_structure, FYN, Reticulocyte, LYN, Erythropoietin, medicine, Erythropoiesis, Signal transduction, Proto-oncogene tyrosine-protein kinase Src, medicine.drug
Abstract

Erythropoiesis is a complex multistep process during which committed erythroid progenitors undergo terminal differentiation to produce circulating mature red cells. Erythroid differentiation is characterized by the production of reactive oxygen species (ROS) both in response to erythropoietin (EPO) and to the large amount of iron imported into the cells for heme biosynthesis. During erythropoiesis, ROS might function as second messenger by modulating intracellular signaling pathways. Fyn, an Src kinase, has been previously reported to participate in signaling pathways in response to ROS in various cell types. Here, we explore the potential contribution of Fyn to normal and stress erythropoiesis by studying 2-4 months-old Fyn knockout mouse strain (Fyn-/-) and C57B6/2J as wild-type controls. Fyn-/- mice showed a mild compensated microcytic anemia associated with signs of dyserythropoiesis. Increased ROS levels and Annexin-V+ cells were presented in all Fyn-/- erythroblast subpopulations compared to wild-type, suggesting a possible reduction in the efficiency of erythropoietin (EPO) signaling pathway in the absence of Fyn. Indeed, in Fyn-/- erythroblasts we observed a reduction in Tyr-phosphorylation state of EPO-R associated with a compensatory activation of Jak2 without major change in Lyn activity. A reduction in STAT5 activation resulting in down-regulation of Cish, a known direct STAT5 target gene, was noted in Fyn-/- erythroblasts. This was paralleled by a reduction in GATA1 and increased HSP70 nuclear translocation compared to wild type, supporting a higher cellular pro-oxidant environment in the absence of Fyn. Using the vitro cell forming colony unit assay, we found a lower in CFU-E and BFU-E cells production, which once again was associated with decreased activation of EPO mediated cascade in the absence of Fyn. To explore the possible role of Fyn in stress erythropoiesis, mice were treated with either phenylhydrazine (PHZ) or doxorubicin (Doxo). Fyn-/- mice showed prolonged anemia after either PHZ or Doxo treatment with a delayed hematologic recovery compared to wild-type animals. When we analyzed the expression of a battery of ARE-genes related to oxidative response such as catalase, Gpx, heme-oxygenase 1 and peroxiredoxin-2, we noted up-regulated expression of these genes in sorted Fyn-/- erythroblasts compared to wild-type cells. In agreement, we observed increased activation of the redox-sensitive transcriptional factor Nrf2 targeting ARE-genes, whose regulation has been previously linked to Fyn. In fact, Nrf2 is switched-off by Fyn, ubiquitylated and delivered to the autophagosome by the p62 cargo protein. In Fyn-/- sorted erythroblasts, we observed (i) accumulation of p62 in large clusters; and (ii) reduction of Nrf2-p62 complex compared to wild-type cells. To address the question whether the perturbation of Nrf2-p62 system results in impairment of autophagy in the absence of Fyn, we used Lysotrack to explore late phases of autophagy. Lysosomal progression was defective in Fyn-/- reticulocytes and it was associated with accumulation of p62 during in vitro reticulocyte maturation. These data indicate that the absence of Fyn blocks the Nrf2 post-induction response to oxidation, resulting in impaired autophagy. To validate our working hypothesis, we treated Fyn-/- mice with Rapamycin, an inducer of autophagy. In Fyn-/- mice, Rapamycin treatment resulted in decrease dyserythropoiesis, ROS levels and Annexin V+ cells, associated with reduction in accumulation of p62 in Fyn-/- erythroblasts. As a proof of concept, we treated both mouse strains with PHZ with or without Rapamycin. This latter worsened PHZ induced acute anemia in wild-type mice but not in Fyn-/- animals. Collectively, our data enabled us to document a novel role for Fyn in erythropoiesis, contributing to EPO-R activation and harmonizing the Nrf2-p62 adaptive cellular response against oxidation during normal and more importantly in stress erythropoiesis. Disclosures No relevant conflicts of interest to declare.

Published
2020

31. PSMB4 and PSMD4 Are Correlated with 1q21 Amplification in CD138 + Plasma Cells: New Potential Druggable Targets in Myeloma Patients

Author

Jessica Burroughs-Garcia, Paola Storti, Luca Agnelli, Denise Toscani, Valentina Marchica, Gabriella Sammarelli, Giannalisa Todaro, Vincenzo Raimondi, Valentina Franceschi, Naomi Soressi, Anna Benedetta Dalla Palma, Laura Notarfranchi, Gaetano Donofrio, and Nicola Giuliani

Subjects
Immunology, Cell Biology, Hematology, Biochemistry
Abstract

The amplification of the 1q21 (amp1q21) region is one of the most acquired cytogenetic abnormalities (CA) in multiple myeloma (MM) associated with a worse patient outcome and disease progression. Moreover, different studies have demonstrated that the number of copies (CN) 1q21 (gain1q21: three copies or amp1q21: ≥ four copies) have a different impact in the response to anti-MM therapies. Particularly, it has been proposed that in MM patients, additional copies of 1q21 may be associated with the resistance to proteasome inhibitor (PI) treatment as bortezomib. A recent study showed that newly diagnosed MM (MMD) patients carrying amp1q21 but not gain1q21 receiving carfilzomib-based treatment have an early disease progression with shorter overall survival. Previous studies underlined that the amplification of 1q21 can lead to the overexpression and/or dysregulation of several candidate genes associated with cell proliferation, apoptosis, and drug resistance. Here we aim to identify 1q21 target genes possibly correlated to the response to PI therapy. We evaluated a total cohort of 29 primary plasma cells (PCs) purified from bone marrow (BM) blood aspirates from 11 smoldering MM (SMM) and 18 MMD. The median age of our cohort was 70 years (range: 38-86). Fluorescence in situ hybridization (FISH) analysis was performed to access the presence or absence of copy number alteration (CNA) in the 1q21 region in all patients. 14 out of 29 patients carried 1q21 CNA (5 with gain1q21 and 9 with amp1q21). A score reflecting the number of 1q21 copies was calculated based on the hybridization pattern. The transcriptional profiles of the 29 BM PCs samples were generated on GeneChip ClariomD Arrays (Affymetrix Inc., Santa Clara, CA, USA). The samr package was used in R for call genes as differentially expressed between 1q21 CN-altered and wild-type samples. The correlation between the 1q21 copy number score and the gene expression levels was performed. Moreover, we have evaluated by FISH the 1q21 CNA in a panel of human myeloma cell lines (HMCLs): OCY-MY5, JJN3, RPMI-8226, NCI-H929, and OPM2. JJN3 were transfected with a control vector and PSMB4 and PSMD4 short hairpin RNA (shRNA) lentivectors. The gene and protein expression levels of PSMB4 and PSMD4 in MM cell lines were analyzed by qRT-PCR and Western Blot, respectively. Cell viability and proliferation were assessed using MTT assay and flow cytometry. Our bioinformatic analyses highlighted the overexpression of different genes (IL6R, ILF2, BCL9, MCL1, CSk1B, ADAR1, ARNT, ANP32E) in the 1q21 CNA samples with respect to the controls, as already reported in the literature. Our analysis showed a significantly higher expression of two proteasome subunits (PSMB4 and PSMD4) in patients with 1q21 CNA when compared with patients without (PSMB4 p=0.0006; PSMD4 p= We have evaluated PSMB4 and PSMD4 mRNA and protein expression levels in a 1q21 wild-type cell line (OCY-MY5) and in a panel of MM cell lines carrying different degrees of 1q21 CN (in order: JJN3, U266, RPMI-8226, OPM2, and NCI-H929). The mRNA expression level of PSMB4 and PSMD4 was higher in cell lines carrying 1q21 amp, following a 1q21 copy number fashion. Similar results were obtained when protein levels of MM cell lines were analyzed by Western Blot. To further determine the potential role of both proteasome subunits in the pathogenesis of amp1q21, we generated a PSMB4-shRNA and PSMD4-shRNA knockdown stable MM cell lines. Functional studies showed that blockade of PSMB4 and PSMD4 decreased MM cell viability. In conclusion, our study identified proteasome subunits PSMB4 and PSMD4 to be significantly upregulated in MM patients carrying amp1q21, correlated with 1q21 copy number but not with disease stage. In addition, knockdown of both, PSMB4 and PSMD4 decreased MM cell proliferation. Therefore, targeting PSMB4 and PSMD4 could be a strategy to treat MM patients with ampq21 Disclosures Giuliani: Celgene: Membership on an entity's Board of Directors or advisory committees, Other: congress, Research Funding; Bristol Mayers Squibb: Other: congress; GSK: Other: clinical studies; Takeda: Membership on an entity's Board of Directors or advisory committees; Janssen: Membership on an entity's Board of Directors or advisory committees, Other: Clinical studies, congress, Research Funding; Millenium Pharmaceutical: Other: clincial studies.

Published
2021

32. Mitapivat Improves Transfusion Burden and Reduces Iron Overload in Thalassemic Mice

Author

Alessandro Matte, Enrica Federti, Penelope A. Kosinski, Lucia De Franceschi, Carlo Brugnara, Angela Siciliano, Lenny Dang, and Iana Iatcenko

Subjects
Immunology, Cell Biology, Hematology, Biochemistry
Abstract

Mitapivat, an oral activator of pyruvate kinase (PK), was recently shown to improve b-thalassemic anemia with a reduction of ineffective erythropoiesis and an amelioration of b-thalassemic red cell features in a mouse model for b-thalassemia (Hbb 3th/+ mice).). These changes were also associated with a beneficial effect on iron homeostasis by modulation of duodenal DMT1 expression (Matte A et al JCI 2021). Two clinical studies have shown improvement of anemia and ineffective erythropoiesis with mitapivat treatment in patients with non-transfusion-dependent (NTD) thalassemia (Kuo et al. EHA 2021). Based on these results, Phase 3 studies in both NTD and TD thalassemia are currently on going. The objective of this preclinical study was to determine if treatment with mitapivat affects the length between transfusion of red blood cells (RBCs) and the liver iron concentration (LIC). Using a previously established murine model of RBCs transfusions (Park Y et al Blood 2020), in Hbb 3th/+ mice, we used Hb 10.5 g/dL as threshold for RBCs transfusion, with washed RBCs, at 40% Hct (400 uL total volume infused). The animals were divided into two groups: vehicle and mitapivat (50mg/Kg by gavage BID for up to 61 days).The length of the interval between transfusions increased in mitapivat treated compared to vehicle treated animals (transfusion interval: 13.8±1.0 days vs vehicle 10.5±1.0 days respectively n=4 and n=3). In both groups, the transfusion regimen induced a significant reduction in spleen weight/mouse weight ratio and in extramedullary erythropoiesis. We also found a significant reduction in liver iron content (LIC) in mitapivat treated compared to vehicle treated animals. We then evaluated the effects of mitapivat in combination with iron chelation using deferiprone (DFP,1.25 mg/mL, drinking water). Casu et al. have previously shown in the same mouse model for β-thal that DFP did not affect erythropoiesis. In the β-thal mice, we did not find negative effects on hematologic parameters when mitapivat (50 mg/Kg/d by gavage BID) was co-administrated with DFP for 28 days. LIC was reduced in mitapivat treated mice and in mitapivat +DFP treated β-thal mice was further decreased compared to vehicle treated animals. This allowed us to reduce DFP dosage from 1.25 to 0.8 mg/mL in mitapivat treated β-thal mice. These data show that in mouse model of transfused β-thalassemia, mitapivat increases the time interval between transfusions, reduces transfusion burden and allows a reduction of the dosing iron chelation with DFP. Thus, mitapivat might represent an interesting option in transfusion dependent β-thalassemic patients, being transfusion burden still an unmet need in this patient population. Disclosures Kosinski: Agios Pharmaceuticals: Current Employment, Current equity holder in publicly-traded company. Dang: Agios Pharmaceuticals, Inc.: Current Employment, Current holder of stock options in a privately-held company. De Franceschi: F. Hoffmann-La Roche Ltd: Consultancy.

Published
2021

33. Nrf2 Plays a Key Role in Iron-Overload Cardiomyopathy

Author

Veronica Riccardi, S. Zebulon Vance, Enrica Federti, Iana Iatcenko, Immacolata Andolfo, Achille Iolascon, Emanuela Tolosano, Alessandra Ghigo, Deborah Chiabrando, Alessandro Matte, Serge Cedrick, Lucia De Franceschi, Angela Siciliano, and Francesca Vinchi

Subjects
Iron overload cardiomyopathy, business.industry, Immunology, Key (cryptography), Medicine, Cell Biology, Hematology, respiratory system, Bioinformatics, business, environment and public health, Biochemistry
Abstract

Cardiomyopathy due to iron-overload is a severe complication of patients undergoing chronic transfusion regimen such as β-thalassemia and myelodysplastic syndromes. Previous studies have shown the key role of Nrf2, a redox-related transcriptional factor, in both β-thalassemia erythropoiesis and iron homeostasis (Matte A et al. ARS 2018, 2019; Lim PJ et al Nat Metab, 2019). Here, we compared Nrf2 knockout male mice (Nrf2 -/-) and C57BL-6J as wild-type (WT) controls, with a focus on cardiac function. Nrf2 -/- mice were characterized by a mild chronic hemolytic anemia associated with ineffective erythropoiesis, similar to what observed in murineβ-thalassemia (Toya SCM et al., Blood, 2019). Aging Nrf2 -/- mice developed systolic and diastolic dysfunction, associated with increased cardiac oxidative stress, degradation of the calcium-dependent SERCA2A transporter and activation of metalloproteinase MMP9, involved in both SERCA2A degradation and heart remodeling. In Nrf2 -/- mice, we observed increased plasma NTBI, heart iron deposition and elevated expression of cardiac ferroportin when compared to WT animals. Moreover, cardiac Hamp mRNA levels were down-regulated in aging Nrf2 -/- mice when compared to WT mice. This pattern was consistent with progressive cardiac iron overload in absence of Nrf2. Interestingly, activation of TGF-b receptor and PDGF-B-related pathway as well as increased collagen deposition were observed in hearts from 12 months old Nrf2 -/- mice. Taken together our data suggest an aging-associated development of iron-overload cardiomyopathy in mice genetically lacking Nrf2. To evaluate the role of Nrf2 in iron overload cardiomyopathy, Nrf2 -/- and WT mice were exposed to dietary iron supplementation (2.5% w/w carbonyl iron for 28 days). Nrf2 -/- mice developed cardiac hypertrophy which was accompanied by a worsening in collagen deposition and persistent activation of PDGF-B pathway. This was associated with inflammatory vasculopathy. The biologic importance of Nrf2 is supported by the cardiac activation of Nrf2, degradation of SERC2A and activation of TGF-b receptor and PDGF-B pathway in a mouse model of beta thalassemia intermedia, the Hbb3th/+ mice. Collectively our data support the crucial role of Nrf2 in the protection of cardiomyocytes against iron cytotoxicity which significantly develops in aging as well as in β-thalassemia. Disclosures Vinchi: Silence Therapeutics: Membership on an entity's Board of Directors or advisory committees, Research Funding; Vifor Pharma: Research Funding; PharmaNutra: Research Funding; Novartis: Research Funding. Ghigo: Kither Biotech: Other: Board member and Co-Founder. Iolascon: Bluebird Bio: Other: Advisory Board; Celgene: Other: Advisory Board.

Published
2021

34. Trial in Progress: The Randomized, Double-Blind, Placebo-Controlled Phase IIa CROSSWALK-c Trial Evaluating the Efficacy of Crovalimab As Adjunct Treatment in the Prevention of Vaso-Occlusive Episodes (VOEs) in Patients with Sickle Cell Disease (SCD)

Author

Caterina P. Minniti, Pablo Bartolucci, Julia Ramos, Diane-Charlotte Imbs, Lucia De Franceschi, Nadiesh Balachandran, Thomas Perretti, Alexandre Sostelly, Michael U. Callaghan, and Kenneth I. Ataga

Subjects
medicine.medical_specialty, business.industry, Immunology, Cell Biology, Hematology, Disease, Placebo, Biochemistry, Adjunct, Double blind, Internal medicine, medicine, In patient, business
Abstract

Background SCD is a group of autosomal recessive red blood cell (RBC) disorders caused by a single point mutation in the β- globin gene, with either homozygous inheritance, or heterozygous co-inheritance with other pathogenic variants of the β-globin gene. This point mutation results in the production of hemoglobin S, which polymerizes within RBCs under certain conditions, leading to the distortion of the RBC membrane and generation of dense and sickle RBCs. These pathologic RBCs contribute to microvascular occlusions in patients with SCD, which present as acute painful episodes called VOEs. In addition to VOEs, patients with SCD may experience severe chronic anemia, chronic pain, immune dysfunction, and progressive multi-organ damage. The current treatment strategy for patients with SCD includes hydroxyurea, along with newer treatments such as L-glutamine, crizanlizumab, and voxelotor. However, despite the availability of these treatments, considerable morbidity and mortality among patients with SCD represents a significant unmet medical need. Activation of the complement pathway has been described in patients with SCD at baseline, in acute pain crisis, and in delayed hemolytic transfusion reaction. Accumulating nonclinical data suggest the potential multimodal role for complement dysregulation in the pathophysiology of SCD, including vaso-occlusion, hemolysis, inflammation, thrombogenicity, endothelial activation, and end-organ damage (Roumenina et al. Am J Hematol 2020). Crovalimab is a novel anti-C5 monoclonal antibody that allows for small-volume subcutaneous (SC) self-injection. Crovalimab demonstrated rapid and sustained complement inhibition with promising efficacy and safety in a Phase I/II study (Röth et al. Blood 2020), in patients with paroxysmal nocturnal hemoglobinuria, a complement-mediated disorder. Study Design and Methods CROSSWALK-c (NCT number pending) is a placebo-controlled, randomized, double-blind, Phase IIa study evaluating the efficacy and safety of crovalimab as adjunct therapy in preventing VOEs in patients with SCD. Patients aged ≥ 12 years to ≤ 55 years, weighing ≥ 40 kg, with a confirmed diagnosis of SCD, homozygous hemoglobin S (HbSS) or sickle cell β 0 thalassemia (HbSβ 0), and presenting with ≥ 2 to ≤ 10 VOEs are eligible for this study. Patients on concurrent SCD-directed therapies are also eligible. Vaccination against Neisseria meningitidis, Haemophilus influenzae type B, and Streptococcus pneumonia are required for enrollment. Patients with a history of hematopoietic stem cell transplant are excluded from the study. Eligible patients will be randomized 1:1 to the crovalimab or placebo treatment arms (Figure). An initial intravenous loading dose of crovalimab or placebo will be administered on Day 1 Week 1, followed by four weekly SC doses on Day 2 Week 1, and then on Weeks 2-4. Maintenance dosing will be administered from Week 5, followed by once every 4 weeks thereafter, for 48 weeks. All patients will receive study treatment according to a weight-based tiered dosing schedule. The primary objective is to evaluate the efficacy of crovalimab compared with placebo, based on the annualized rate of medical facility VOEs. Secondary efficacy objectives include the annualized rate of acute chest syndrome, the annualized rate of home VOE, and change in urinary albumin-creatinine ratio, tricuspid regurgitant jet velocity, and Patient-Reported Outcomes Measurement Information System (PROMIS)-Fatigue score in adults, from baseline to Week 49. Safety, pharmacokinetics, immunogenicity, and exploratory biomarker objectives will also be evaluated. Figure 1 Figure 1. Disclosures Callaghan: Agios Pharmaceuticals: Current Employment; Roche/Genentech: Consultancy, Speakers Bureau; Global Blood Therapeutics: Consultancy, Speakers Bureau; Forma: Consultancy; Hema Biologics: Consultancy; Takeda: Consultancy, Speakers Bureau; Sanofi: Consultancy; BioMarin: Consultancy; Spark: Consultancy; uniQure: Consultancy; Chiesi: Consultancy; Kedrion: Consultancy; Pfizer: Consultancy. Ataga: Novartis: Membership on an entity's Board of Directors or advisory committees; Agios Pharmaceuticals: Consultancy; Forma Therapeutics: Membership on an entity's Board of Directors or advisory committees; Global Blood Therapeutics: Membership on an entity's Board of Directors or advisory committees; F. Hoffmann-La Roche Ltd: Consultancy; Novo Nordisk: Membership on an entity's Board of Directors or advisory committees. De Franceschi: F. Hoffmann-La Roche Ltd: Consultancy. Minniti: CSL Behring: Other: Endpoint adjudicator ; Forma: Consultancy; Novo Nordisk: Consultancy; Chiesi: Consultancy; Bluebird Bio: Other: Endpoint adjudicator ; Novartis: Consultancy; GBT: Consultancy; F. Hoffmann-La Roche Ltd: Consultancy. Balachandran: F. Hoffmann-La Roche Ltd: Current Employment. Imbs: F. Hoffmann-La Roche Ltd: Consultancy; Certara Inc.: Current Employment. Perretti: F. Hoffmann-La Roche Ltd: Current Employment. Ramos: Genentech, Inc.: Current Employment. Sostelly: F. Hoffmann-La Roche Ltd: Current Employment. Bartolucci: Bluebird: Consultancy, Research Funding; Novartis: Consultancy, Membership on an entity's Board of Directors or advisory committees, Other: Lecture fees, Steering committee, Research Funding; Fabre Foundation: Research Funding; Jazz Pharma: Other: Lecture fees; AGIOS: Consultancy; INNOVHEM: Other: Co-founder; Emmaus: Consultancy; Addmedica: Consultancy, Other: Lecture fees, Research Funding; Hemanext: Consultancy; F. Hoffmann-La Roche Ltd: Consultancy; GBT: Consultancy.

Published
2021

35. The Increased Burden of Sickle Cell Disease in Italy: Findings from the Greatalys (Generating Real world Evidence Across ITALy In SCD) Study

Author

Gian Luca Forni, Luca Degli Esposti, Eleonora Premoli, Valentina Perrone, Carina Fiocchi, Claudia Condorelli, Diletta Valsecchi, Chiara Castiglioni, and Lucia De Franceschi

Subjects
business.industry, Environmental health, Immunology, Medicine, Cell Biology, Hematology, Disease, Real world evidence, business, Biochemistry
Abstract

Introduction. Sickle Cell Disease (SCD) is an evolving public health issue with a significant impact on patient survival, quality of life and costs for health systems also in Italy, a multiethnic country where epidemiology has deeply changed. We present final results from the GREATalyS study that aimed to better understand the SCD burden in Italy in terms of prevalence, clinical features, treatments and resource consumption in the clinical practice setting. Methods. Retrospective observational analysis of administrative databases for health resources consumption from a representative sample of Region/Local Health Units in Italy, covering approximately 15.3 million inhabitants. All patients with ≥1hospitalization (outside Emergency Room, ER) with main or secondary discharge diagnosis of SCD (with/without crisis) identified by ICD-9-CM codes were included between January-2010 to December-2017 (up to December 2018 for epidemiologic analysis). Prevalence of SCD in 2018 was projected to the Italian population. Patients were followed-up from the first diagnosis identified within the inclusion period (index date) to death or end of data availability. Treatments and healthcare resource consumption were evaluated on patients with at least 1 year of data availability before and after index date. SCD treatments were classified as SCD-specific, SCD-related, SCD-complication-related. Both day hospitals and ordinary hospitalizations were evaluated. Vaso-occlusive crisis (VOCs) (identified by hospitalization discharge diagnosis for SCD with crisis) and main SCD organ complications were assessed during follow-up. Mean annual healthcare resource costs were analyzed during follow-up according to the NHS perspective in terms of overall treatments, all-cause hospitalizations and out-patients services. Results. SCD prevalence in 2018 was 13 cases per 100,000 inhabitants. Prevalence projected to Italian population estimated in total 7,977 SCD patients in Italy in 2018 (of whom 1,690 and 6,287 were Conclusions. This Italian real-world study may have revealed a SCD sub-population probably not noticed yet to SCD centers of reference, and still probably underestimated since ER flows were not present. Similarly, also VOC could be underestimated as only most severe episodes requiring hospitalization were captured. Proportion of patients with antithrombotic agents might be an indicator of the underlying multiorgan complications. The present data describe an SCD population with high resource utilization and heavy economic burden and warrants further efforts to increase an earlier patient identification that could lead to a timely and comprehensive treatment with less SCD-related complications. Figure 1 Figure 1. Disclosures Forni: Bluebirdbio: Membership on an entity's Board of Directors or advisory committees; Celgene: Membership on an entity's Board of Directors or advisory committees; Novartis: Membership on an entity's Board of Directors or advisory committees. Castiglioni: Novartis Farma SpA: Current Employment. Condorelli: Novartis Farma SpA: Current Employment. Valsecchi: Novartis Farma SpA: Current Employment. Premoli: Novartis Farma SpA: Current Employment. Fiocchi: Novaris Farma SpA: Current Employment.

Published
2021

36. Trial in Progress: The Randomized, Double-Blind, Placebo-Controlled Phase Ib CROSSWALK-a Trial Evaluating the Safety of Crovalimab for the Management of Acute Uncomplicated Vaso-Occlusive Episodes (VOEs) in Patients with Sickle Cell Disease (SCD)

Author

Caterina P. Minniti, Pablo Bartolucci, Lucia De Franceschi, Kenneth I. Ataga, A. Alexandrou, Himika Patel, Michael U. Callaghan, Jonathan Schimmel, Richard Fox, Alexandre Sostelly, and Diane-Charlotte Imbs

Subjects
medicine.medical_specialty, business.industry, Immunology, Occlusive, Cell Biology, Hematology, Disease, Placebo, Biochemistry, Double blind, Internal medicine, Medicine, In patient, business
Abstract

Background SCD is a group of autosomal recessive red blood cell (RBC) disorders caused by a single point mutation in the β-globin gene, resulting in the production of hemoglobin S. Hemoglobin S polymerizes within RBCs under certain conditions, leading to the distortion of the RBC membrane and generation of dense and sickle RBCs. These pathologic RBCs contribute to microvascular occlusions in patients with SCD, which present as acute painful episodes called VOEs. Despite the majority of VOEs being managed at home, they remain the most common reason for emergency department (ED) visits and hospitalization among patients with SCD, with > 70% of ED visits and > 90% of hospital admissions for SCD being related to VOEs (Ballas et al. Am J Hematol 2005; Lanzkron et al. Am J Hematol 2010). One of the most severe complications of VOEs is acute chest syndrome, which is a leading cause of mortality among patients with VOEs (Vichinsky et al. N Engl J Med 2000; Bartolucci et al. eBioMedicine 2016). In the absence of targeted therapies for the management of VOEs in patients with SCD, treatment is currently limited to pain management, blood exchange transfusion (with the risk of complications), and other supportive care, representing a significant unmet medical need. Activation of the complement pathway has been described in patients with SCD at baseline, in acute pain crises, and in patients with delayed hemolytic transfusion reaction. Accumulating nonclinical data have suggested a multimodal role for complement dysregulation in the pathophysiology of SCD including vaso-occlusion, hemolysis, inflammation, thrombogenicity, endothelial activation, and end-organ damage (Roumenina et al. Am J Hematol 2020). Crovalimab is a novel, engineered, anti-complement C5 monoclonal antibody. In a Phase I/II study (Röth et al. Blood 2020) in patients with paroxysmal nocturnal hemoglobinuria, a complement-mediated disorder, crovalimab demonstrated rapid and sustained complement inhibition with promising efficacy and safety. Study Design and Methods CROSSWALK-a (NCT04912869) is a randomized, double-blind, placebo-controlled, Phase Ib study evaluating the safety of crovalimab for the management of acute uncomplicated VOEs in patients with SCD. Patients aged ≥ 12 years to ≤ 55 years, weighing ≥ 40 kg, and with a confirmed diagnosis of SCD homozygous hemoglobin S (HbSS) or sickle cell β 0 thalassemia (HbSβ 0) are eligible for the study (Figure). Patients must present with an acute uncomplicated VOE, requiring hospitalization and treatment with parenteral opioid analgesics. Vaccinations against Neisseria meningitidis, Hemophilus influenzae type B, and Streptococcus pneumoniae must be up to date. Eligible patients will be randomized 2:1 to receive either a single intravenous weight-based tiered dose of crovalimab or placebo. Patients in both study arms will continue to undergo pain management and receive other supportive care for their VOE and may also continue to receive ongoing concurrent SCD-directed therapies. Patients will be followed during the hospitalization until discharge and will continue to be followed post-discharge during an observational period. The maximum total study duration for an individual patient will be 12 weeks, which includes the hospitalization and observational periods. The primary objective is to evaluate the incidence and severity of adverse events according to National Cancer Institute Common Terminology Criteria for Adverse Events, Version 5.0, incidence and severity of infusion-related reactions and hypersensitivity, and change from baseline in targeted vital signs and clinical laboratory test results. Efficacy, pharmacokinetics, pharmacodynamics, immunogenicity, and exploratory biomarker endpoints will also be evaluated. Figure 1 Figure 1. Disclosures Bartolucci: F. Hoffmann-La Roche Ltd: Consultancy; Bluebird: Consultancy, Research Funding; Emmaus: Consultancy; Hemanext: Consultancy; Jazz Pharma: Other: Lecture fees; AGIOS: Consultancy; GBT: Consultancy; Novartis: Consultancy, Membership on an entity's Board of Directors or advisory committees, Other: Lecture fees, Steering committee, Research Funding; INNOVHEM: Other: Co-founder; Fabre Foundation: Research Funding; Addmedica: Consultancy, Other: Lecture fees, Research Funding. Ataga: Forma Therapeutics: Membership on an entity's Board of Directors or advisory committees; Novo Nordisk: Membership on an entity's Board of Directors or advisory committees; F. Hoffmann-La Roche Ltd: Consultancy; Novartis: Membership on an entity's Board of Directors or advisory committees; Agios Pharmaceuticals: Consultancy; Global Blood Therapeutics: Membership on an entity's Board of Directors or advisory committees. Callaghan: Alnylum: Current equity holder in publicly-traded company; Roche/Genentech: Consultancy, Speakers Bureau; Takeda: Consultancy, Speakers Bureau; Sanofi: Consultancy; Pfizer: Consultancy; Global Blood Therapeutics: Consultancy, Speakers Bureau; uniQure: Consultancy; Spark: Consultancy; Biomarin: Consultancy; Kedrion: Consultancy; Hema Biologics: Consultancy; Forma: Consultancy; Chesei: Consultancy; Agios Pharmaceuticals: Current Employment. De Franceschi: F. Hoffmann-La Roche Ltd: Consultancy. Minniti: F. Hoffmann-La Roche: Consultancy; Bluebird Bio: Other: Endpoint adjudicator; Forma: Consultancy; GBT: Consultancy; Novo Nordisk: Consultancy; CSL Behring: Other: Endpoint adjudicator; Novartis: Consultancy; Chiesi: Consultancy. Alexandrou: F. Hoffmann-La Roche Ltd: Consultancy, Current equity holder in publicly-traded company; Pfizer: Current equity holder in publicly-traded company. Imbs: F. Hoffmann-La Roche Ltd: Consultancy; Certara Inc.: Current Employment. Fox: Parexel International: Current Employment; Genentech, Inc.: Current Employment. Patel: Genentech, Inc.: Current Employment. Sostelly: F. Hoffmann-La Roche Ltd: Current Employment.

Published
2021

37. Real World Efficacy Evaluation of Branded and Copy Imatinib in Chronic Myeloid Leukemia: A Retrospective Multicentric Study from Argentina

Author

Varela, Ana Ines, primary, Bendek, Georgina, additional, Pavlovsky, Carolina, additional, Freitas, Maria Josefina, additional, Ventriglia, Veronica, additional, Enrico, Alicia, additional, Riva, Maria Elisa, additional, Perez, Mariel Ana, additional, Mariano, Romina, additional, Beligoy, Luis, additional, Pagani, Maria, additional, Tannuri, Ricardo Khalil, additional, Larripa, Irene, additional, Bengio, Raquel, additional, Rojas, Francisca, additional, Riveros, Dardo, additional, Debus, Mariana Raquel, additional, Franceschi, Erica, additional, Osycka, Maria Victoria, additional, Pavlovsky, Miguel A., additional, and Moiraghi, Beatriz, additional

Published
2020
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38. COVID 19 and Hemoglobinopathies: Update of the Italian Experience

Author

Motta, Irene, primary, Pinto, Valeria Maria, additional, Longo, Filomena, additional, Bonetti, Federico, additional, De Michele, Elisa, additional, Piperno, Alberto, additional, Pitrolo, Lorella, additional, Quaresima, Micol, additional, Ribersani, Michela, additional, Migone De Amicis, Margherita, additional, Balocco, Manuela, additional, Gianesin, Barbara, additional, Graziadei, Giovanna, additional, Cappellini, Maria Domenica, additional, De Franceschi, Lucia, additional, Piga, Antonio, additional, and Forni, Gian Luca, additional

Published
2020
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39. The Pyruvate Kinase Activator Mitapivat Ameliorates Anemia and Prevents Iron Overload in a Mouse Model of Hereditary Spherocytosis

Author

Mattè, Alessandro, primary, Anand, Wilson, additional, Federti, Enrica, additional, Kung, Charles, additional, Kosinski, Penelope A., additional, Riccardi, Veronica, additional, Iatcenko, Iana, additional, Dang, Lenny, additional, Leboeuf, Christophe, additional, Janin, Anne, additional, Brugnara, Carlo, additional, Narla, Mohandas, additional, and De Franceschi, Lucia, additional

Published
2020
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40. Pathologic angiogenesis in the bone marrow of humanized sickle cell mice is reversed by blood transfusion

Author

Park, Shin-Young, primary, Matte, Alessandro, primary, Jung, Yookyung, primary, Ryu, Jina, primary, Anand, Wilson Babu, primary, Han, Eun-Young, primary, Liu, Min, primary, Carbone, Carmine, primary, Melisi, Davide, primary, Nagasawa, Takashi, primary, Locascio, Joseph J., primary, Lin, Charles P., primary, Silberstein, Leslie E., primary, and De Franceschi, Lucia, primary

Published
2020
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41. Resolution of sickle cell disease-associated inflammation and tissue damage with 17

Author

Olga K. Weinberg, Valentine Brousse, Pierre-Louis Tharaux, Paul C. Norris, Antonio Recchiuti, Angela Siciliano, Ian R. Riley, Achille Iolascon, Alessia Lamolinara, Lucia De Franceschi, Alessandro Matte, Carlo Brugnara, Thomas Mintz, Enrica Federti, Bérengère Koehl, Charles N. Serhan, Wassim El Nemer, Immacolata Andolfo, Matte, Alessandro, Recchiuti, Antonio, Federti, Enrica, Koehl, Bérengère, Mintz, Thoma, Nemer, Wassim El, Tharaux, Pierre-Loui, Brousse, Valentine, Andolfo, Immacolata, Lamolinara, Alessia, Weinberg, Olga, Siciliano, Angela, Norris, Paul C., Riley, Ian R., Iolascon, Achille, Serhan, Charles N., Brugnara, Carlo, and De Franceschi, Lucia

Subjects
0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Docosahexaenoic Acids, Neutrophils, Immunology, Pain, Inflammation, Anemia, Sickle Cell, Defective proresolving response to acute vaso-occlusive events characterizes murine SCD, Biochemistry, Proinflammatory cytokine, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Red Cells, Iron, and Erythropoiesis, In vivo, hemic and lymphatic diseases, medicine, Animals, Humans, Efferocytosis, business.industry, Anti-Inflammatory Agents, Non-Steroidal, Lipid signaling, Hematology, Cell Biology, Pneumonia, Hypoxia (medical), Treatment with 17R-RvD1 reduces inflammation and vascular dysfunction in SCD mice, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, Cytokines, Kidney Diseases, medicine.symptom, business, Resolvin, BLOOD Commentary, Ex vivo
Abstract

Resolvins (Rvs), endogenous lipid mediators, play a key role in the resolution of inflammation. Sickle cell disease (SCD), a genetic disorder of hemoglobin, is characterized by inflammatory and vaso-occlusive pathologies. We document altered proresolving events following hypoxia/reperfusion in humanized SCD mice. We demonstrate novel protective actions of 17R-resolvin D1 (17R-RvD1; 7S, 8R, 17R-trihydroxy-4Z, 9E, 11E, 13Z, 15E, 19Z-docosahexaenoic acid) in reducing ex vivo human SCD blood leukocyte recruitment by microvascular endothelial cells and in vivo neutrophil adhesion and transmigration. In SCD mice exposed to hypoxia/reoxygenation, oral administration of 17R-RvD1 reduces systemic/local inflammation and vascular dysfunction in lung and kidney. The mechanism of action of 17R-RvD1 involves (1) enhancement of SCD erythrocytes and polymorphonuclear leukocyte efferocytosis, (2) blunting of NF-κB activation, and (3) a reduction in inflammatory cytokines, vascular activation markers, and E-selectin expression. Thus, 17R-RvD1 might represent a new therapeutic strategy for the inflammatory vasculopathy of SCD.

Published
2018

42. The N-terminal 11 amino acids of human erythrocyte band 3 are critical for aldolase binding and protein phosphorylation: implications for band 3 function

Author

Perrotta, Silverio, Borriello, Adriana, Scaloni, Andrea, De Franceschi, Lucia, Brunati, Anna Maria, Turrini, Francesco, Nigro, Vincenzo, Miraglia del Giudice, Emanuele, Nobili, Bruno, Conte, Maria Luisa, Rossi, Francesca, Iolascon, Achille, Donella-Deana, Arianna, Zappia, Vincenzo, Poggi, Vincenzo, Anong, William, Low, Philip, Mohandas, Narla, and Della Ragione, Fulvio

Published
2005
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44. COVID 19 and Hemoglobinopathies: Update of the Italian Experience

Author

Giovanna Graziadei, Michela Ribersani, Irene Motta, Lorella Pitrolo, L De Franceschi, G. L. Forni, M. M. De Amicis, Manuela Balocco, Alberto Piperno, Barbara Gianesin, E. De Michele, Micol Quaresima, Valeria Pinto, M.D. Cappellini, Federico Bonetti, A. Piga, and Filomena Longo

Subjects
medicine.medical_specialty, History, Coronavirus disease 2019 (COVID-19), Family medicine, Immunology, medicine, Cell Biology, Hematology, Biochemistry, 112.Thalassemia and Globin Gene Regulation
Abstract

Background. Patients with pre-existent chronic morbidities are likely to be more severely affected by SARS-Cov2 infection. In Italy, the "Società Italiana Talassemie ed Emoglobinopatie" (SITE) has recently estimated the number of patients (Pts) with Hemoglobinopathies followed by Italian Specialized Centers (SITE Network). Five thousand Transfusion-dependent beta-thalassemia (TDT), 1900 Non-Transfusion-dependent beta-thalassemia (NTDT) and 2000 Sickle Cell Disease (SCD) were registered [1]. To verify the impact of SARS-CoV-2 infection on Pts with Hemoglobinopathies, we performed a specific survey by electronic Case Report Form (eCRF). Inclusion criteria included positive swab or serology in a patient with hemoglobinopathy and at least 15 days of follow-up from either the onset of symptoms or SARS-CoV2 positivity. The survey was approved by the Ethics Committee, and eCRF was shared with the Centers of Italian Hemoglobinopathies Network. Preliminary data updated to April 10, 2020, were published [2]. Results. As of July 31, 2020, 27 cases have been reported: 18 TDT, 4 NTDT, 5 SCD. 89% of the cases were in Northern Italy, where the rate of infection was much higher than the rest of the country, reflecting the national epidemiology. The mean age of thalassemia patients (TDT and NTDT) was 43±11 years, and 55% were male; the mean age of SCD patients was 33±15 years, and 40% was male. The likely source of infection has been detected in 63% (17/27) of cases: 11 had occupational exposure, 6 had a positive relative. Five patients were asymptomatic: for them, the SARS-CoV-2 infection was identified by positive swab for 1 patient and by positive level of IgG for 4. Twenty patients had associated comorbidities, 14 were splenectomized, and 3 had functional asplenia. Eleven patients were hospitalized, only one in high-intensity care unit. Three patients required more intensive ventilation support with continuous positive airway pressure (CPAP), one of these has a history of diffuse large B-cell lymphoma treated with chemotherapy in the previous year. Three other patients required support by oxygen. No Pts required intubation. Two Pts increased blood requirement. Only five received supposedly specific treatment for COVID-19: two hydroxychloroquine (HCQ), one HCQ plus ritonavir/darunavir, and one HCQ plus anakinra, one HCQ plus Tocilizumab plus Lopinavir/Ritonavir. The clinical course of hospitalized patients was 18±7 days. All patients recovered. Conclusions. The prevalence of COVID-19 infection in Italian patients with Hemoglobinopathies result 0,3% while in general population the prevalence in Italy is 0,4% [3]. Considering that the thalassemia population is more strictly observed, we could postulate that the precautions suggested or self-applied by the Pts were effective. No death nor severe SARS with intubation, nor signs of cytokines storm, only one thromboembolic event was observed although most individuals had pre-existing complications. A single case with pulmonary hypertension has been described in detail [4]. In most individuals the infection has been pauci or asymptomatic and all recovered. This experience differs from what has been observed in Iran on a similar series with different severity and mortality and ask for a more in-depth comparison [5]. In conclusion, our data do not indicate increased severity of COVID-19 in Pts with Hemoglobinopathies followed in Specialized Centers. Acknowledgment. We would like to thank ALT (Associazione per la Lotta alla Talassemia R.Vullo - Ferrara).. References 1. http://www.site-italia.org/2020/covid-19.php. SITE communication. Accessed April 1, 2020 2. Motta I, Migone De Amicis M, Pinto VM, et al. SARS-CoV-2 infection in beta thalassemia: Preliminary data from the Italian experience. Am J Hematol. 2020;95(8): E198-E199. 3. https://www.epicentro.iss.it/coronavirus/sars-cov-2-dashboard, Accessed July 31, 2020 4. Pinto VM, Derchi GE, Bacigalupo L, Pontali E, Forni GL. COVID-19 in a Patient with β-Thalassemia Major and Severe Pulmonary Arterial Hypertension. Hemoglobin. 2020;44(3):218-220. 5. Karimi M, Haghpanah S, Azarkeivan A, et al. Prevalence and mortality in β-thalassaemias due to outbreak of novel coronavirus disease (COVID-19): the nationwide Iranian experience. Br J Haematol. 2020;190(3):e137-e140. Disclosures Motta: Sanofi Genzyme: Honoraria. Cappellini:BMS: Honoraria; Genzyme/Sanofi: Honoraria, Membership on an entity's Board of Directors or advisory committees; CRISPR Therapeutics, Novartis, Vifor Pharma: Membership on an entity's Board of Directors or advisory committees. Piga:BMS: Research Funding; Novartis: Research Funding. Forni:Novartis: Membership on an entity's Board of Directors or advisory committees.

Published
2020

45. Real World Efficacy Evaluation of Branded and Copy Imatinib in Chronic Myeloid Leukemia: A Retrospective Multicentric Study from Argentina

Author

Maria Pagani, Alicia Enrico, Maria Josefina Freitas, Maria Elisa Riva, Miguel A. Pavlovsky, Luis Beligoy, Mariana Debus, Beatriz Moiraghi, Romina Mariano, Ricardo Khalil Tannuri, Dardo Riveros, Carolina Pavlovsky, Raquel Bengió, Mariel Ana Perez, Veronica Ventriglia, Georgina Bendek, Irene Larripa, Ana Ines Varela, Erica Franceschi, Francisca Rojas, and Maria Victoria Osycka

Subjects
Response rate (survey), medicine.medical_specialty, business.industry, Immunology, Myeloid leukemia, Imatinib, Cell Biology, Hematology, Biochemistry, Imatinib mesylate, Median follow-up, Internal medicine, Cohort, Medicine, Progression-free survival, Sokal Score, business, medicine.drug
Abstract

Background: Data on the safety and efficacy of copy drugs is usually unavailable. Imatinib mesylate is used to treat chronic myeloid leukemia (CML) patients in Argentina since 2002. During the last decade more than ten different imatinib copies are marketed by the different health-care systems in the country, usually for cost issues. In spite of the undoubted benefit of this tyrosine-kinase inhibitor indication in CML, there is no solid evidence that supports copy drug equivalent outcomes for this patient population. Aim: To compare the clinical presentation, treatment response and outcome of a chronic phase (CP) CML patient cohort treated with branded and copy imatinib in the real-life setting. Methods: Multicentric, retrospective trial based on data obtained from medical charts of adult CP CML patients treated with imatinib in 9 centers in Argentina from 2002 to 2020.We analyzed demographic characteristics and clinical characteristics described for branded and copy imatinib treated cohorts. Frequency of complete cytogenetic response (CCyR) at 12 months, Major molecular response or better(≥MMR) at 12, 18 and 24 months and overall MR4.0, MR4.5 and deep molecular response (MR4.0 +MR4.5 IS) were analyzed. Event was defined as failure, progression or CML related death. Kaplan Meier comparison of event free, progression free and overall survival. Statistics: IBM SPSS version 1. Results: A total of 568 CP CML adult patients (pt) treated with imatinib were included. Mean age at diagnosis: 45.7 years (range 18 - 85). Male 55.6% (316/568). Sokal Score was recorded in 471 pt: 57% (269/471) low, 26% (122/471) intermediate and 17% (80/471) high-risk. Median follow-up 107 months (RIQ: 36-149). Branded imatinib treatment 330 (58%) and imatinib copies 238 (42%). For branded and copy imatinib cohorts mean age 46,1 (18-85) and 45.3(18-80), male 53% (175/330) and 59% (141/238), median follow up 102 (RIQ 101-130) and 61 (RIQ 62-146) respectively. Sokal score low 58% (164/284) and 56% (105/187), intermediate 27% (77/284) and 24% (45/187) and high 15% (43/284) and19% (37/187). Frequency of CCyR at 12 months 71% (67/94) and 69% (41/59), ≥MMR at 12 months 57% (79/138) and 43% (39/89), ≥MMR 18m 66 % (61/92) and 71% (43/60), ≥MMR 24m 65% (96/147) and 79% (58/73). Overall MR4, MR 4.5 and Deep MR with branded imatinib 62.4% (186/298), 42% (118/276) and 63% (189/300), compared to 45(97/214), 24% (50/207) and 46% (99/215) with copies. Difference in evaluation throughout the treatment periods with loss of data did not allow response rate statistical comparison in predetermined timepoints. Kaplan Meier Event free survival median 229 months vs 75 months p 0.001, Progression free survival mean 318 months vs 208 pt 0.034 and Overall Survival mean 275 months vs 206 months for branded and copy imatinib respectively. Discussion: Several case reports have shown poor outcomes in patients treated with imatinib copy drugs, including loss of responses previously attained with branded imatinib. This study reports data from a large cohort of CP CML patients treated in daily practice during a long period of time. Treatment results at determined timepoints is comparable. Although management and treatment decisions were performed in different time periods, results show different outcomes in EFS and PFS between patients treated with branded vs copy imatinib. Overall survival in both cohorts is comparable. As studies assesing the safety and efficacy of the copy drugs compared with branded imatinib will hardly be performed this evidence calls for careful attention and strict follow up measures when managing CML patients with copy imatinib. Figure Disclosures Varela: Novartis: Consultancy, Speakers Bureau. Pavlovsky:Pint Pharma: Speakers Bureau; Pfizer: Speakers Bureau; BMS: Speakers Bureau; Novartis: Membership on an entity's Board of Directors or advisory committees, Speakers Bureau. Freitas:Pfizer: Consultancy, Other: Advisory Board. Pavlovsky:Varifarma: Speakers Bureau; Astra Zeneca: Membership on an entity's Board of Directors or advisory committees, Speakers Bureau; Janssen: Membership on an entity's Board of Directors or advisory committees, Other: travel grants, Speakers Bureau; Abbvie: Membership on an entity's Board of Directors or advisory committees, Other: Travel grants, Speakers Bureau. Moiraghi:Novartis: Speakers Bureau; BMS: Speakers Bureau.

Published
2020

49. The Pyruvate Kinase Activator Mitapivat Ameliorates Anemia and Prevents Iron Overload in a Mouse Model of Hereditary Spherocytosis

Author

Lucia De Franceschi, Christophe Leboeuf, Alessandro Matte, Veronica Riccardi, Lenny Dang, Mohandas Narla, Enrica Federti, Penelope A. Kosinski, Iana Iatcenko, Charles Kung, Carlo Brugnara, Anne Janin, and Wilson Anand

Subjects
chemistry.chemical_classification, Hemolytic anemia, medicine.medical_specialty, Red Cell, biology, Anemia, business.industry, Immunology, Erythrocyte fragility, Cell Biology, Hematology, medicine.disease, Biochemistry, Hereditary spherocytosis, Endocrinology, chemistry, Internal medicine, medicine, biology.protein, Ankyrin, business, Band 3, Pyruvate kinase
Abstract

Hereditary spherocytosis (HS) is the most common cause of inherited red cell membranopathy, due to mutations in genes encoding for membrane or cytoskeletal proteins, including band 3, ankyrin, spectrin, band 4.1 or band 4.2. Membrane instability results in membrane surface area loss and generation of spherocytic red cells with elevated MCHC, decreased cellular deformability and reduced red cell survival, due to splenic sequestration. Clinical management of the hemolytic anemia due to HS depends on the age of the patient and the severity of anemia. Splenectomy is indicated in children with symptomatic anemia. A classic diagnostic test for HS is the incubated osmotic fragility: this test highlights the crucial role that ATP content plays in maintenance of normal RBC function including membrane stability: it is generally believed that the increased fragility of HS is the result of abnormal ATP depletion over the 24hr incubation. We explored the hypothesis that pyruvate kinase activator, mitapivat, by modulating ATP content could have potential beneficial effects for HS RBCs in band 4.2-/- mice, a well-established model of HS (Peters LL et al JCI 103: 1527, 1999). 4.2-/- mice exhibit moderate anemia which recapitulates most of the features of typical human HS without showing the profound anemization seen in other mouse models. Oral AG-348 administration to band 4.2-/- mice at dosages of 200 mg/kg/day over 6 months resulted in (i) improvement of anemia with reduced reticulocyte count (Hb 11.6±0.035 g/dL, n=17 vs 13.104±0.09 g/dL, n=9; P Disclosures Kung: Agios Pharmaceuticals: Current Employment, Current equity holder in publicly-traded company. Kosinski:Agios Pharmaceuticals Inc: Current Employment, Current equity holder in publicly-traded company. Dang:Agios Pharmaceuticals Inc.: Current Employment, Current equity holder in publicly-traded company. Brugnara:Sysmex America Inc.: Consultancy; American Journal of Hematology: Other.

Published
2020

50. The Vasculopathy in the Bone Marrow Microenvironment of Humanized Sickle Cell Mice Is Reversible By Blood Transfusion

Author

Park, Shin-Young, primary, Mattè, Alessandro, additional, Jung, Yookyung, additional, Ryu, Jina, additional, Anand, Wilson, additional, Han, Eun Young Anna, additional, Liu, Min, additional, Carbone, Carmine, additional, Melisi, Davide, additional, Nagasawa, Takashi, additional, Lin, Charles, additional, Silberstein, Leslie E., additional, and De Franceschi, Lucia, additional

Published
2019
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