Your search keyword '"Vannucchi P"' showing total 1,052 results

1. Proposals for revised International Working Group–European LeukemiaNet criteria for anemia response in myelofibrosis

Author

Tefferi, Ayalew, Barosi, Giovanni, Passamonti, Francesco, Hernandez-Boluda, Juan-Carlos, Bose, Prithviraj, Döhner, Konstanze, Ellis, Martin, Gangat, Naseema, Garcia, Jacqueline S., Gisslinger, Heinz, Gotlib, Jason, Guglielmelli, Paola, Gupta, Vikas, Harrison, Claire, Hexner, Elizabeth O., Hobbs, Gabriela S., Kiladjian, Jean-Jacques, Koschmieder, Steffen, Kroger, Nicolaus, Kuykendall, Andrew T., Loscocco, Giuseppe G., Mascarenhas, John, Masarova, Lucia, Mesa, Ruben, Mora, Barbara, Odenike, Olatoyosi, Oh, Stephen T., Pardanani, Animesh, Patel, Anand, Pemmaraju, Naveen, Rambaldi, Alessandro, Rampal, Raajit, Sirhan, Shireen, Szuber, Natasha, Talpaz, Moshe, Vachhani, Pankit J., Vannucchi, Alessandro M., and Barbui, Tiziano

Abstract

•An international panel of 38 experts and clinical trialists in MF participated in the preparation of the current document.•New definitions of transfusion status, gender-specific hemoglobin thresholds, and criteria for major and minor responses are submitted.

Published

2024

2. Efficacy and safety of fedratinib in patients with myelofibrosis previously treated with ruxolitinib (FREEDOM2): results from a multicentre, open-label, randomised, controlled, phase 3 trial

Author

Harrison, Claire N, Mesa, Ruben, Talpaz, Moshe, Al-Ali, Haifa Kathrin, Xicoy, Blanca, Passamonti, Francesco, Palandri, Francesca, Benevolo, Giulia, Vannucchi, Alessandro Maria, Mediavilla, Clemence, Iurlo, Alessandra, Kim, InHo, Rose, Shelonitda, Brown, Patrick, Hernandez, Christopher, Wang, Jia, and Kiladjian, Jean-Jacques

Abstract

Most patients with myelofibrosis develop ruxolitinib intolerance or disease that is relapsed or refractory, and survival rates after ruxolitinib discontinuation are poor. We aimed to evaluate the safety and efficacy of fedratinib versus best available therapy (BAT) in patients with myelofibrosis previously treated with ruxolitinib.

Published

2024

3. Safety and efficacy of luspatercept for the treatment of anemia in patients with myelofibrosis

Author

Gerds, Aaron T., Harrison, Claire, Kiladjian, Jean-Jacques, Mesa, Ruben, Vannucchi, Alessandro M., Komrokji, Rami, Bose, Prithviraj, Kremyanskaya, Marina, Mead, Adam J., Gotlib, Jason, Rose, Shelonitda, Sanabria, Fabian, Marsousi, Niloufar, Giuseppi, Ana Carolina, Jiang, Huijing, Palmer, Jeanne M., McCaul, Kelly, Ribrag, Vincent, and Passamonti, Francesco

Abstract

•Luspatercept improved anemia in patients with MF with/without transfusion dependence, particularly those receiving ruxolitinib.•After 3 years of minimal follow-up, luspatercept safety profile was consistent with previous studies; no new safety signals identified.

Published

2024

4. Tumor microenvironment of Burkitt lymphoma: different immune signatures with different clinical behavior

Author

Siciliano, Maria Chiara, Bertolazzi, Giorgio, Morello, Gaia, Tornambè, Salvatore, Del Corvo, Marcello, Granai, Massimo, Sapienza, Maria Rosaria, Leahy, Ciara I., Fennell, Eanna, Belmonte, Beatrice, Arcuri, Felice, Vannucchi, Margherita, Mancini, Virginia, Guazzo, Raffaella, Boccacci, Roberto, Onyango, Noel, Nyagol, Joshua, Santi, Raffaella, Di Stefano, Gioia, Ferrara, Domenico, Bellan, Cristiana, Marafioti, Teresa, Ott, German, Siebert, Reiner, Quintanilla-Fend, Leticia, Fend, Falko, Murray, Paul, Tripodo, Claudio, Pileri, Stefano, Lazzi, Stefano, and Leoncini, Lorenzo

Abstract

•BL with granulomatous reaction was characterized by an M1 signature and INFG in CD8+ cells, whereas BL with starry sky showed M2 genes.•Tumor-associated macrophages repolarization and epigenetic regulators may open new therapeutic options for the fight against BL lymphoma.

Published

2024

5. The bacterial community of the European spruce bark beetle in space and time

Author

Moussa, Abdelhameed, Nones, Stefano, Vannucchi, Patrizia Elena, Shahzad, Gul-i-Rayna, Dittmer, Jessica, Corretto, Erika, Schebeck, Martin, Faccoli, Massimo, Battisti, Andrea, Stauffer, Christian, and Schuler, Hannes

Abstract

The European spruce bark beetle Ips typographus is a pest causing severe damage in forests dominated by Norway spruce in Europe. Microorganisms play essential roles in bark beetles, including nutrition, fitness as well as in overcoming host defenses. Here, we performed high-throughput 16S rRNA metabarcoding of I. typographus across different populations in Europe, to assess its bacterial community. We investigated four postglacial refugial areas in Europe and focused specifically on a current bark beetle hot spot in the Dolomites where we compared populations with different epidemiological phases (outbreaking vs. non-outbreaking) and across different seasons (pre-overwintering vs. overwintering). Our results show that the bacterial community structure varied among populations from the refugial areas and between different regions within the Dolomites. We found a significant difference in the bacterial community between pre-overwintering and overwintering individuals, but we did not find differences between epidemic and endemic populations. The prevalence of the genera Erwinia (which was present in all individuals) and Pseudoxanthomonas (present in almost all individuals) across all populations suggests that these taxa form the core bacterial community of I. typographus. Furthermore, several additional bacterial taxa occurred in all populations, but with variable frequencies. This study highlights a complex interaction of I. typographus and various bacterial taxa across different regions and ecological phases and provides new insights into the role of microorganisms in the biology of this important pest species.

Published

2024

6. A safety evaluation of ruxolitinib for the treatment of polycythemia vera

Author

Boldrini, Valentina, Vannucchi, Alessandro M., and Guglielmelli, Paola

Abstract

ABSTRACTIntroductionPolycythemia Vera (PV) is a chronic myeloproliferative neoplasm hallmarked by deregulated proliferation of hematopoietic stem cells leading to prevalent expansion of red cell mass, increased rate of vascular events, splenomegaly, disease-associated symptoms, and risk of evolution to secondary myelofibrosis and blast phase. PV is pathogenetically associated with autonomously persistent activation of JAK2, which causes overproduction of blood cells and an inflammatory condition responsible for the clinical manifestations of the disease. Extensively supported by preclinical studies, targeting JAK2-dependent signaling represents a rational therapeutic approach to PV, finally leading to the approval of ruxolitinib, a JAK1/2 inhibitor.Areas covered (literature research)We analyzed reports of phase 2 and phase 3 trials with ruxolitinib in PV and relevant literature dealing with efficacy and safety aspects, including most recent real-world reports.Expert opinionRuxolitinib is the only JAK2 inhibitor approved for the treatment of PV with well-known efficacy for splenomegaly, symptoms, and potentially reduction of vascular events. The treatment regimen is notably manageable and safe, with the most prevalent side effects primarily encompassing myelosuppression, hyperlipidemia, non-melanoma skin cancer and infections, mainly reactivation of Herpes Zoster. These effects necessitate ongoing surveillance and proactive preventive measures.

Published

2024

7. Proteomic screening identifies PF4/Cxcl4 as a critical driver of myelofibrosis

Author

Capitanio, Daniele, Calledda, Francesca R., Abbonante, Vittorio, Cattaneo, Daniele, Moriggi, Manuela, Niccolò, Bartalucci, Bucelli, Cristina, Tosi, Delfina, Gianelli, Umberto, Vannucchi, Alessandro Maria, Iurlo, Alessandra, Gelfi, Cecilia, Balduini, Alessandra, and Malara, Alessandro

Abstract

Despite increased understanding of the genomic landscape of Myeloproliferative Neoplasms (MPNs), the pathological mechanisms underlying abnormal megakaryocyte (Mk)-stromal crosstalk and fibrotic progression in MPNs remain unclear. We conducted mass spectrometry-based proteomics on mice with Romiplostim-dependent myelofibrosis to reveal alterations in signaling pathways and protein changes in Mks, platelets, and bone marrow (BM) cells. The chemokine Platelet Factor 4 (PF4)/Cxcl4 was up-regulated in all proteomes and increased in plasma and BM fluids of fibrotic mice. High TPO concentrations sustained in vitro PF4 synthesis and secretion in cultured Mks, while Ruxolitinib restrains the abnormal PF4 expression in vivo. We discovered that PF4 is rapidly internalized by stromal cells through surface glycosaminoglycans (GAGs) to promote myofibroblast differentiation. Cxcl4gene silencing in Mks mitigated the profibrotic phenotype of stromal cells in TPO-saturated co-culture conditions. Consistently, extensive stromal PF4 uptake and altered GAGs deposition were detected in Romiplostim-treated, JAK2V617Fmice and BM biopsies of MPN patients. BM PF4 levels and Mk/platelet CXCL4expression were elevated in patients, exclusively in overt fibrosis. Finally, pharmacological inhibition of GAGs ameliorated in vivo fibrosis in Romiplostim-treated mice. Thus, our findings highlight the critical role of PF4 in the fibrosis progression of MPNs and substantiate the potential therapeutic strategy of neutralizing PF4-GAGs interaction.

Published

2024

8. Chromosome 9p trisomy increases stem cells clonogenic potential and fosters T-cell exhaustion in JAK2-mutant myeloproliferative neoplasms

Author

Carretta, Chiara, Parenti, Sandra, Bertesi, Matteo, Rontauroli, Sebastiano, Badii, Filippo, Tavernari, Lara, Genovese, Elena, Malerba, Marica, Papa, Elisa, Sperduti, Samantha, Enzo, Elena, Mirabile, Margherita, Pedrazzi, Francesca, Neroni, Anita, Tombari, Camilla, Mora, Barbara, Maffioli, Margherita, Mondini, Marco, Brociner, Marco, Maccaferri, Monica, Tenedini, Elena, Martinelli, Silvia, Bartalucci, Niccolò, Bianchi, Elisa, Casarini, Livio, Potenza, Leonardo, Luppi, Mario, Tagliafico, Enrico, Guglielmelli, Paola, Simoni, Manuela, Passamonti, Francesco, Norfo, Ruggiero, Vannucchi, Alessandro Maria, and Manfredini, Rossella

Abstract

JAK2V617F is the most recurrent genetic mutation in Philadelphia-negative chronic Myeloproliferative Neoplasms (MPNs). Since the JAK2locus is located on Chromosome 9, we hypothesized that Chromosome 9 copy number abnormalities may be a disease modifier in JAK2V617F-mutant MPN patients. In this study, we identified a subset of MPN patients with partial or complete Chromosome 9 trisomy (+9p patients), who differ from JAK2V617F-homozygous MPN patients as they carry three JAK2alleles as well as three copies of all neighboring gene loci, including CD274, encoding immunosuppressive Programmed death-ligand 1 (PD-L1) protein. Investigation of the clonal hierarchy revealed that the JAK2V617F occurs first, followed by +9p. Functionally, CD34+ cells from +9p MPN patients demonstrated increased clonogenicity, generating a greater number of primitive colonies, due to high OCT4and NANOGexpression, with knock-down of these genes leading to a genotype-specific decrease in colony numbers. Moreover, our analysis revealed increased PD-L1 surface expression in malignant monocytes from +9p patients, while analysis of the T cell compartment unveiled elevated levels of exhausted cytotoxic T cells. Overall, here we identify a distinct novel subgroup of MPN patients, who feature a synergistic interplay between +9p and JAK2V617F that shapes immune escape characteristics and increased stemness in CD34+ cells.

Published

2024

9. Indication and management of allogeneic haematopoietic stem-cell transplantation in myelofibrosis: updated recommendations by the EBMT/ELN International Working Group

Author

Kröger, Nicolaus, Bacigalupo, Andrea, Barbui, Tiziano, Ditschkowski, Markus, Gagelmann, Nico, Griesshammer, Martin, Gupta, Vikas, Hamad, Nada, Harrison, Claire, Hernandez-Boluda, Juan Carlos, Koschmieder, Steffen, Jain, Tania, Mascarenhas, John, Mesa, Ruben, Popat, Uday R, Passamonti, Francesco, Polverelli, Nicola, Rambaldi, Alessandro, Robin, Marie, Salit, Rachel B, Schroeder, Thomas, Scott, Bart L, Tamari, Roni, Tefferi, Ayalew, Vannucchi, Alessandro M, McLornan, Donal P, and Barosi, Giovanni

Abstract

New options for medical therapy and risk scoring systems containing molecular data are leading to increased complexity in the management of patients with myelofibrosis. To inform patients’ optimal care, we updated the 2015 guidelines on indications for and management of allogeneic haematopoietic stem-cell transplantation (HSCT) with the support of the European Society for Blood and Marrow Transplantation (EBMT) and European LeukemiaNet (ELN). New recommendations were produced using a consensus-building methodology after a comprehensive review of articles released from January, 2015 to December, 2022. Seven domains and 18 key questions were selected through a series of questionnaires using a Delphi process. Key recommendations in this update include: patients with primary myelofibrosis and an intermediate-2 or high-risk Dynamic International Prognostic Scoring System score, or a high-risk Mutation-Enhanced International Prognostic Score Systems (MIPSS70 or MIPSS70-plus) score, or a low-risk or intermediate-risk Myelofibrosis Transplant Scoring System score should be considered candidates for allogeneic HSCT. All patients who are candidates for allogeneic HSCT with splenomegaly greater than 5 cm below the left costal margin or splenomegaly-related symptoms should receive a spleen-directed treatment, ideally with a JAK-inhibitor; HLA-matched sibling donors remain the preferred donor source to date. Reduced intensity conditioning and myeloablative conditioning are both valid options for patients with myelofibrosis. Regular post-transplantation driver mutation monitoring is recommended to detect and treat early relapse with donor lymphocyte infusion. In a disease where evidence-based guidance is scarce, these recommendations might help clinicians and patients in shared decision making.

Published

2024

10. Addition of danicopan to ravulizumab or eculizumab in patients with paroxysmal nocturnal haemoglobinuria and clinically significant extravascular haemolysis (ALPHA): a double-blind, randomised, phase 3 trial

Author

Lee, Jong Wook, Griffin, Morag, Kim, Jin Seok, Lee Lee, Lily Wong, Piatek, Caroline, Nishimura, Jun-ichi, Carrillo Infante, Cynthia, Jain, Deepak, Liu, Peng, Filippov, Gleb, Sicre de Fontbrune, Flore, Risitano, Antonio, Kulasekararaj, Austin G, Barcellini, Wilma, Barraco, Fiorenza, Beneitez Pastor, David, Capra, Marcelo, Chew, Lee Ping, Chrysavgi, Lalayanni, De Castro, Carlos, de la Tour, Régis Peffault, De Oliveira, Michel Michels, Di Bona, Eros, Forcade, Edouard, Fu, Chieh-Lin, Furha, Cossor, Gaya Valls, Anna, Giannouli, Stavroula, Gonzalez-Fernandez, Ataulfo, Griffin, Morag, Gural, Alexander, Gutierrez, Emilio Ojeda, Hernández-Rodríguez, Inés, Ibrahim, Ibrahim, Iori, Anna Paola, Ishida, Tadao, Jang, Jun Ho, Kim, Jeong-A, Kim, Jin Seok, Kitano, Toshiyuki, Kosugi, Hiroshi, Kreiniz, Natalia, Kulasekararaj, Austin, Lee, Jong Wook, Lee Lee, Lily Wong, Mayer, Jiri, Mitchell, Lindsay, Mori, Yasuo, Nishiwaki, Kaichi, Notaro, Rosario, Nunez, Ramiro, Obara, Naoshi, Oliva, Esther Natalie, Patriquin, Christopher, Pessoa, Viviani, Piatek, Caroline, Piekarska, Agnieszka, Raza, Shahzad, Risitano, Antonio Maria, Rojnuckarin, Ponlapat, Samuel, Desmond, Shammo, Jamile, Tadmor, Tamar, Takami, Akiyoshi, Tamari, Roni, Terriou, Louis, Uchiyama, Hitoji, Vannucchi, Alessandro Maria, and Yamaguchi, Hiroki

Abstract

Symptoms of anaemia due to clinically significant extravascular haemolysis can affect patients with paroxysmal nocturnal haemoglobinuria (PNH) treated with C5 inhibitors (ravulizumab or eculizumab). The aim of this study was to assess the efficacy and safety of danicopan (ALXN2040), an investigational, first-in-class, oral complement factor D inhibitor, as add-on therapy to ravulizumab or eculizumab in patients with PNH and clinically significant extravascular haemolysis.

Published

2023

11. Matching-adjusted indirect comparison of the pelabresib-ruxolitinib combination vs JAKi monotherapy in myelofibrosis

Author

Gupta, Vikas, Mascarenhas, John, Kremyanskaya, Marina, Rampal, Raajit K., Talpaz, Moshe, Kiladjian, Jean-Jacques, Vannucchi, Alessandro M., Verstovsek, Srdan, Colak, Gozde, Dey, Debarshi, and Harrison, Claire

Abstract

•Pelabresib plus ruxolitinib combination has potential for higher clinical efficacy than JAKi monotherapy in patients with MF.•Greater SVR and durable TSS improvement was observed with pelabresib plus ruxolitinib vs JAKi monotherapy.

Published

2023

12. Momelotinib versus danazol in symptomatic patients with anaemia and myelofibrosis previously treated with a JAK inhibitor (MOMENTUM): an updated analysis of an international, double-blind, randomised phase 3 study

Author

Gerds, Aaron T, Verstovsek, Srdan, Vannucchi, Alessandro M, Al-Ali, Haifa Kathrin, Lavie, David, Kuykendall, Andrew T, Grosicki, Sebastian, Iurlo, Alessandra, Goh, Yeow Tee, Lazaroiu, Mihaela C, Egyed, Miklos, Fox, Maria Laura, McLornan, Donal, Perkins, Andrew, Yoon, Sung-Soo, Gupta, Vikas, Kiladjian, Jean-Jacques, Granacher, Nikki, Lee, Sung-Eun, Ocroteala, Luminita, Passamonti, Francesco, Harrison, Claire N, Oh, Stephen, Klencke, Barbara J, Yu, Jing, Donahue, Rafe, Kawashima, Jun, and Mesa, Ruben

Abstract

The MOMENTUM study met all key endpoints at week 24, demonstrating symptom, spleen, and anaemia benefits with momelotinib versus danazol in patients with myelofibrosis. In this updated analysis, we report duration of week 24 responses and new responses with momelotinib through week 48.

Published

2023

13. The risk of stroke recurrence in patients with atrial fibrillation and reduced ejection fraction

Author

Paciaroni, Maurizio, Agnelli, Giancarlo, Caso, Valeria, Becattini, Cecilia, Mosconi, Maria Giulia, Giustozzi, Michela, Tsivgoulis, Georgios, Seiffge, David Julian, Engelter, Stefan T., Lyrer, Philippe, Polymeris, Alexandros A., Dittrich, Tolga, Zietz, Annaelle, Putaala, Jukka, Strbian, Daniel, Tomppo, Liisa, Michel, Patrik, Strambo, Davide, Salerno, Alexander, Remillard, Suzette, Buehrer, Manuela, Bavaud, Odessa, Vanacker, Peter, Zuurbier, Susanna M., Yperzeele, Laetitia, Loos, Caroline M.J., Cappellari, Manuel, Emiliani, Andrea, Zedde, Marialuisa, Abdul-Rahim, Azmil H., Dawson, Jesse, Cronshaw, Robert, Schirinzi, Erika, Del Sette, Massimo, Stretz, Christoph, Kala, Narendra, Reznik, Michael, Schomer, Ashley, Mac Grory, Brian, Jayaraman, Mahesh, Yaghi, Shadi, Furie, Karen L., Masotti, Luca, Grifoni, Elisa, Toni, Danilo, Risitano, Angela, Falcou, Anne, Petraglia, Luca, Lotti, Enrico Maria, Padroni, Marina, Pavolucci, Lucia, Lochner, Piergiorgio, Silvestrelli, Giorgio, Ciccone, Alfonso, Alberti, Andrea, Venti, Michele, De Magistris, Ilaria Leone, Cancelloni, Virginia, Kargiotis, Odysseas, Rocco, Alessandro, Diomedi, Marina, Marcheselli, Simona, Caliandro, Pietro, Zauli, Aurelia, Reale, Giuseppe, Moci, Marco, Antonenko, Kateryna, Rota, Eugenia, Tassinari, Tiziana, Saia, Valentina, Palmerini, Francesco, Aridon, Paolo, Arnao, Valentina, Monaco, Serena, Cottone, Salvatore, Baldi, Antonio, D’Amore, Cataldo, Ageno, Walter, Pegoraro, Samuela, Ntaios, George, Sagris, Dimitrios, Giannopoulos, Sotirios, Kosmidou, Maria, Ntais, Evangelos, Romoli, Michele, Pantoni, Leonardo, Rosa, Silvia, Bertora, Pierluigi, Chiti, Alberto, Canavero, Isabella, Saggese, Carlo Emanuele, Plocco, Maurizio, Giorli, Elisa, Palaiodimou, Lina, Bakola, Eleni, Bandini, Fabio, Gasparro, Antonio, Terruso, Valeria, Mannino, Marina, Pezzini, Alessandro, Morotti, Andrea, Magoni, Mauro, Ornello, Raffaele, Sacco, Simona, Popovic, Nemanja, Scoditti, Umberto, Genovese, Antonio, Denti, Licia, Flomin, Yuriy, Mancuso, Michelangelo, Ferrari, Elena, Caselli, Maria Chiara, Ulivi, Leonardo, Giannini, Nicola, Vadikolias, Kostantinos, Liantinioti, Chrysoula, Chondrogianni, Maria, Carletti, Monica, Karagkiozi, Efstathia, Athanasakis, George, Makaritsis, Kostantinos, Lanari, Alessia, Tatlisumak, Turgut, Acciarresi, Monica, Vannucchi, Vieri, Lorenzini, Gianni, Tassi, Rossana, Guideri, Francesca, Acampa, Maurizio, Martini, Giuseppe, Sohn, Sung-Il, Mumoli, Nicola, Tadi, Prasanna, Letteri, Federica, Maccarrone, Miriam, Galati, Franco, Tiseo, Cindy, Gourbali, Vanessa, Halvatsiotis, Panagiotis, Orlandi, Giovanni, Giuntini, Martina, Corea, Francesco, Bellesini, Marta, Baronello, Mario Maimone, Karapanayiotides, Theodore, Rueckert, Christina, Csiba, Laszló, Szabó, Lilla, Rigatelli, Alberto, Imberti, Davide, Zabzuni, Dorjan, Pieroni, Alessio, Barlinn, Kristian, Pallesen, Lars-Peder, Barlinn, Jessica, Doronin, Boris, Volodina, Vera, Deleu, Dirk, Bonetti, Bruno, Porta, Cesare, Gentile, Luana, Eskandari, Ashraf, and De Marchis, Gian Marco

Abstract

Background: Atrial fibrillation (AF) and congestive heart failure often coexist due to their shared risk factors leading to potential worse outcome, particularly cerebrovascular events. The aims of this study were to calculate the rates of ischemic and severe bleeding events in ischemic stroke patients having both AF and reduced ejection fraction (rEF) (⩽40%), compared to ischemic stroke patients with AF but without rEF.Methods: We performed a retrospective analysis that drew data from prospective studies. The primary outcome was the composite of either ischemic (stroke or systemic embolism), or hemorrhagic events (symptomatic intracranial bleeding and severe extracranial bleeding).Results: The cohort for this analysis comprised 3477 patients with ischemic stroke and AF, of which, 643 (18.3%) had also rEF. After a mean follow-up of 7.5 ± 9.1 months, 375 (10.8%) patients had 382 recorded outcome events, for an annual rate of 18.0%. While the number of primary outcome events in patients with rEF was 86 (13.4%), compared to 289 (10.2%) for the patients without rEF; on multivariable analysis rEF was not associated with the primary outcome (OR 1.25; 95% CI 0.84–1.88). At the end of follow-up, 321 (49.9%) patients with rEF were deceased or disabled (mRS ⩾3), compared with 1145 (40.4%) of those without rEF; on multivariable analysis, rEF was correlated with mortality or disability (OR 1.35; 95% CI 1.03–1.77).Conclusions: In patients with ischemic stroke and AF, the presence of rEF was not associated with the composite outcome of ischemic or hemorrhagic events over short-term follow-up but was associated with increased mortality or disability.

Published

2023

14. Risk of recurrent stroke in patients with atrial fibrillation treated with oral anticoagulants alone or in combination with anti-platelet therapy

Author

Caliandro, Pietro, Cancelloni, Virginia, Marco, Moci, Reale, Giuseppe, Zauli, Aurelia, Agnelli, Giancarlo, Caso, Valeria, Becattini, Cecilia, Calabresi, Paolo, Giulia Mosconi, Maria, Giustozzi, Michela, Tsivgoulis, Georgios, Julian Seiffge, David, Engelter, Stefan T., Lyrer, Philippe, Polymeris, Alexandros A., Dittrich, Tolga, Zietz, Annaelle, Marco De Marchis, Gian, Putaala, Jukka, Strbian, Daniel, Tomppo, Liisa, Michel, Patrik, Strambo, Davide, Salerno, Alexander, Remillard, Suzette, Buehrer, Manuela, Bavaud, Odessa, Vanacker, Peter, Zuurbier, Susanna, Yperzeele, Laetitia, Loos, Caroline M.J., Cappellari, Manuel, Emiliani, Andrea, Zedde, Marialuisa, Abdul-Rahim, Azmil, Dawson, Jesse, Cronshaw, Robert, Schirinzi, Erika, Del Sette, Massimo, Stretz, Christoph, Kala, Narendra, Reznik, Michael, Schomer, Ashley, Mac Grory, Brian, Jayaraman, Mahesh, McTaggart, Ryan, Yaghi, Shadi, Furie, Karen L., Masotti, Luca, Grifoni, Elisa, Toni, Danilo, Risitano, Angela, Falcou, Anne, Petraglia, Luca, Maria Lotti, Enrico, Padroni, Marina, Pavolucci, Lucia, Lochner, Piergiorgio, Silvestrelli, Giorgio, Ciccone, Alfonso, Alberti, Andrea, Venti, Michele, Leone De Magistris, Ilaria, Kargiotis, Odysseas, Rocco, Alessandro, Diomedi, Marina, Marcheselli, Simona, Antonenko, Kateryna, Rota, Eugenia, Tassinari, Tiziana, Saia, Valentina, Palmerini, Francesco, Aridon, Paolo, Arnao, Valentina, Monaco, Serena, Cottone, Salvatore, Baldi, Antonio, D’Amore, Cataldo, Ageno, Walter, Pegoraro, Samuela, Ntaios, George, Sagris, Dimitrios, Giannopoulos, Sotirios, Kosmidou, Maria, Ntais, Evangelos, Romoli, Michele, Pantoni, Leonardo, Rosa, Silvia, Bertora, Pierluigi, Chiti, Alberto, Canavero, Isabella, Emanuele Saggese, Carlo, Plocco, Maurizio, Giorli, Elisa, Palaiodimou, Lina, Bakola, Eleni, Bandini, Fabio, Gasparro, Antonio, Terruso, Valeria, Mannino, Marina, Pezzini, Alessandro, Ornello, Raffaele, Sacco, Simona, Popovic, Nemanja, Scoditti, Umberto, Genovese, Antonio, Denti, Licia, Flomin, Yuriy, Mancuso, Michelangelo, Ferrari, Elena, Chiara Caselli, Maria, Ulivi, Leonardo, Giannini, Nicola, Vadikolias, Kostantinos, Liantinioti, Chrysoula, Chondrogianni, Maria, Halvatsiotis, Panagiotis, Carletti, Monica, Karagkiozi, Efstathia, Athanasakis, George, Makaritsis, Kostantinos, Lanari, Alessia, Tatlisumak, Turgut, Acciarresi, Monica, Vannucchi, Vieri, Lorenzini, Gianni, Tassi, Rossana, Guideri, Francesca, Acampa, Maurizio, Martini, Giuseppe, Sohn, Sung-Il, Mumoli, Nicola, Tadi, Prasanna, Letteri, Federica, Maccarrone, Miriam, Poli, Loris, Magoni, Mauro, Galati, Franco, Tiseo, Cindy, Gourbali, Vanessa, Orlandi, Giovanni, Giuntini, Martina, Corea, Francesco, Bellesini, Marta, Girardi, Laura, Maimone Baronello, Mario, Karapanayiotides, Theodore, Rueckert, Christina, Csiba, Laszló, Szabó, Lilla, Rigatelli, Alberto, Imberti, Davide, Zabzuni, Dorjan, Pieroni, Alessio, Barlinn, Kristian, Pallesen, Lars-Peder, Barlinn, Jessica, Doronin, Boris, Volodina, Vera, Deleu, Dirk, Bonetti, Bruno, Porta, Cesare, Gentile, Luana, Eskandari, Ashraf, and Paciaroni, Maurizio

Abstract

Introduction: Ischaemic stroke patients with atrial fibrillation (AF) are at high risk of stroke recurrence despite oral anticoagulation therapy. Patients with cardiovascular comorbidities may take both antiplatelet and oral anticoagulation therapy (OAC/AP). Our study aims to evaluate the safety and efficacy of OAC/AP therapy as secondary prevention in people with AF and ischaemic stroke.Patients and methods: We performed a post-hoc analysis of pooled individual data from multicenter prospective cohort studies and compared outcomes in the OAC/AP cohort and patients on DOAC/VKA anticoagulation alone (OAC cohort). Primary outcome was a composite of ischaemic stroke, systemic embolism, intracranial bleeding, and major extracranial bleeding, while secondary outcomes were ischaemic and haemorrhagic events considered separately. A multivariable logistic regression analysis was performed to identify independent predictors for outcome events. To compare the risk of outcome events between the two cohorts, the relation between the survival function and the set of explanatory variables were calculated by Cox proportional hazard models and the results were reported as adjusted hazard ratios (HR). Finally another analysis was performed to compare the overall risk of outcome events in both OAC/AP and OAC cohorts after propensity score matching (PSM).Results: During a mean follow-up time of 7.5 ± 9.1 months (median follow-up time 3.5 months, interquartile range ±3), 2284 stroke patients were on oral anticoagulants and 215 were on combined therapy. The multivariable model demonstrated that the composite outcome is associated with age (OR: 1.03, 95% CI: 1.01–1.04 for each year increase) and concomitant antiplatelet therapy (OR: 2.2, 95% CI: 1.48–3.27), the ischaemic outcome with congestive heart failure (OR: 1.55, 95% CI: 1.02–2.36) and concomitant antiplatelet therapy (OR: 1.93, 95% CI: 1.19–3.13) and the haemorrhagic outcome with age (OR: 1.03, 95% CI: 1.01–1.06 for each year increase), alcoholism (OR: 2.15, 95% CI: 1.06–4.39) and concomitant antiplatelet therapy (OR: 2.22, 95% CI: 1.23–4.02). Cox regression demonstrated a higher rate of the composite outcome (hazard ratio of 1.93 [95% CI, 1.35–2.76]), ischaemic events (HR: 2.05 [95% CI: 1.45–2.87]) and bleeding outcomes (HR: 1.90 [95% CI, 1.06–3.40]) in OAC/AP cohort. After PSM analysis, the composite outcome remained more frequent in people treated with OAC + AP (RR: 1.70 [95% CI, 1.05–2.74]).Discussion: Secondary prevention with combination of oral anticoagulant and antiplatelet therapy after ischaemic stroke was associated with worse outcomes in our cohort.Conclusion: Further research is needed to improve secondary prevention by investigating the mechanisms of recurrent ischaemic stroke in patients with atrial fibrillation.

Published

2023

15. Momelotinib versus danazol in symptomatic patients with anaemia and myelofibrosis (MOMENTUM): results from an international, double-blind, randomised, controlled, phase 3 study

Author

Verstovsek, Srdan, Gerds, Aaron T, Vannucchi, Alessandro M, Al-Ali, Haifa Kathrin, Lavie, David, Kuykendall, Andrew T, Grosicki, Sebastian, Iurlo, Alessandra, Goh, Yeow Tee, Lazaroiu, Mihaela C, Egyed, Miklos, Fox, Maria Laura, McLornan, Donal, Perkins, Andrew, Yoon, Sung-Soo, Gupta, Vikas, Kiladjian, Jean-Jacques, Granacher, Nikki, Lee, Sung-Eun, Ocroteala, Luminita, Passamonti, Francesco, Harrison, Claire N, Klencke, Barbara J, Ro, Sunhee, Donahue, Rafe, Kawashima, Jun, Mesa, Ruben, Abulafia, Adi Shacham, Al-Ali, Haifa Kathrin, Andreasson, Bjorn, Angona, Anna, Ayala, Rosa, Bang, Soo-Mee, Bank, Bruce, Barraco, Fiorenza, Beggiato, Eloise, Benghiat, Fleur Samantha, Bonifacio, MassimiliaNo, Bories, Claire, Borsaru, Gabriela, Brabrand, Mette, Braester, Andrei, Broliden, Andes, Buxhofer-Ausch, Veronika, Cambier, Nathalie, Caramella, Marianna, Carpentier, Benjamin, Cascavilla, Nicola, Castellano, Maria Giraldo, Chang, Hung, Chen, Chih-Cheng, Cheong, June-Won, Choi, Yunsuk, Choi, Philip, Corsetti, Maria Teresa, Cuadrado, Isabel Montero, Cunningham, Julia, Damaj, Gandhi Laurent, De Stefano, Valerio, Delage, Robert, Delgado, Regina Garcĺa, Diaz, Jose Miguel Torregrosa, Dombi, Péter, Dubruille, Viviane, Egyed, Miklós, El Fassi, Daniel, Elinder-Camburn, Anna, Elli, Elena Maria, Ellis, Martin, Fava, Carmen, Fazal, Salman, Fleischman, Angela, Foltz, Lynda, Fox, Laura, Gabrail, Nashat, Garcĺa-Gutiérrez, Jose Valentĺn, Gerds, Aaron, Girault, Stephane, Gisslinger, Heinz, Gluvacov, Alexandru, Goh, Yeow Tee, Göthert, Joachim, Granacher, Nikki, Grosicki, Sebastian, Gupta, Vikas, Hadjiev (Hadzhiev), Evgeni (Evgueniy), Hafraoui, Kaoutar, Hamed, Aryan, Harrison, Claire, Hasselbalch, Hans, Hauser, Hanns, Heaney, Mark, Hebart, Holger, Hernandez Rivas, Jesus Maria, Higuero Saavedra, Victor, Hillis, Christopher, Hou, Hsin-An, How, Jonathan, Huang, Daniel, Hus, Marek, Illés, Arpad, Isidori, Alessandro, Iurlo, Alessandra, Ivanov, Vadim, Johansson, Peter, Jung, Chul Won, Kiladjian, Jean-Jacques, Kirgner, Ilya, Koren-Michowitz, Maya, Koschmieder, Steffen, Kosztolanyi, Szabolcs Ors, Kreiniz, Natalia, Kuykendall, Andrew, Lambert, Jonathan, Laribi, Kamel, Lascaux, Axelle, Lavie, Noa, Lavie, David, Lazaroiu, Mihaela, Leahy, Michael, Lech-Maranda, Ewa, Lee, Sung-Eun, Lee, Won Sik, Legrand, Ollivier, Lemoli, Roberto, Liang, James, Lim, Sung-Nam, Loschi, Michael, Lucchesi, Alessandro, Macarie, Ioan, Marolleau, Jean-Pierre, Martelli, Maurizio, Mayer, Jiri, McCloskey, James, McDermott, Christopher, McLornan, Donal, McMahon, Brandon, Mehta, Priyanka, Mesa, Ruben, Mikala, Gábor, Milojkovic, Dragana, Mineur, Philippe, Mishchenko, Elena, Moon, Joon Ho, Nagy, Zsolt, Narayanan, Srinivasan, O'Connell, Casey, Ocroteala, Luminita, Oh, Stephen, Ojeda-Uribe, Mario, Ong, Kiat Hoe, Otegbeye, Folashade, Palmer, Jeanne, Pane, Fabrizio, Passamonti, Francesco, Patriarca, Andrea, Perkins, Andrew, Pietrantuono, Giuseppe, Plander, Mark, Platzbecker, Uwe, Prasad, Ritam, Prejzner, Witold, Rachow, Tobias, Radinoff, Atanas, Rejtő, László, Rinaldi, Ciro, Robak, Tadeusz, Rodriguez, Maria Angeles Fernandez, Ronson, Aaron, Ross, David, Sacha, Tomasz, Sadjadian, Parvis, Salar, Antonio, Santillana, Guillermo Sanz, Scheid, Christof, Schmidt, Aline, Severinsen, Marianne Tang, Stoeva, Vera, Szwedyk, Paweł, Tiribelli, Mario, Trautmann-Grill, Karolin, Trottier, Amy, Tzvetkov, Nikolay, van Droogenbroeck, Janusz, Vannucchi, Alessandro, Verstovsek, Srdan, Vianelli, Nicola, von Bubnoff, Nikolas, Wolf, Dominik, Woszczyk, Dariusz, Woźny, Tomasz, Wróbel, Tomasz, Xicoy, Blanca, Yeh, Su-Peng, and Yoon, Sung-Soo

Abstract

Janus kinase (JAK) inhibitors approved for myelofibrosis provide spleen and symptom improvements but do not meaningfully improve anaemia. Momelotinib, a first-in-class inhibitor of activin A receptor type 1 as well as JAK1 and JAK2, has shown symptom, spleen, and anaemia benefits in myelofibrosis. We aimed to confirm the differentiated clinical benefits of momelotinib versus the active comparator danazol in JAK-inhibitor-exposed, symptomatic patients with anaemia and intermediate-risk or high-risk myelofibrosis.

Published

2023

16. CALRmutations possess unique prognostic relevance in myelofibrosis—before and after transplant

Author

Tefferi, Ayalew and Vannucchi, Alessandro M.

Published

2024

17. Momelotinib long-term safety and survival in myelofibrosis: integrated analysis of phase 3 randomized controlled trials

Author

Verstovsek, Srdan, Mesa, Ruben, Gupta, Vikas, Lavie, David, Dubruille, Viviane, Cambier, Nathalie, Platzbecker, Uwe, Hus, Marek, Xicoy, Blanca, Oh, Stephen T., Kiladjian, Jean-Jacques, Vannucchi, Alessandro M., Gerds, Aaron, Egyed, Miklos, Mayer, Jiří, Sacha, Tomasz, Kawashima, Jun, Morris, Marc, Huang, Mei, and Harrison, Claire

Abstract

•AEs with momelotinib were mostly grade 1/2, noncumulative, and associated with low rates of discontinuation.•In this large, heterogeneous MF data set evaluating a JAK inhibitor, 12% of patients received momelotinib for ≥5 years.

Published

2023

18. Comprehensive response criteria for myeloid/lymphoid neoplasms with eosinophilia and tyrosine kinase gene fusions: a proposal from the MLN International Working Group

Author

Shomali, William, Colucci, Philomena, George, Tracy I., Kiladjian, Jean-Jacques, Langford, Cheryl, Patel, Jay L., Reiter, Andreas, Vannucchi, Alessandro M., and Gotlib, Jason

Published

2023

19. Biological drivers of clinical phenotype in myelofibrosis

Author

Mascarenhas, John, Gleitz, Hélène F. E., Chifotides, Helen T., Harrison, Claire N., Verstovsek, Srdan, Vannucchi, Alessandro Maria, Rampal, Raajit K., Kiladjian, Jean-Jacques, Vainchenker, William, Hoffman, Ronald, Schneider, Rebekka K., and List, Alan F.

Abstract

Myelofibrosis (MF) is a myeloproliferative disorder that exhibits considerable biological and clinical heterogeneity. At the two ends of the disease spectrum are the myelodepletive or cytopenic phenotype and the myeloproliferative phenotype. The cytopenic phenotype has a high prevalence in primary MF (PMF) and is characterized by low blood counts. The myeloproliferative phenotype is typically associated with secondary MF (SMF), mild anemia, minimal need for transfusion support, and normal to mild thrombocytopenia. Differences in somatic driver mutations and allelic burden, as well as the acquisition of non-driver mutations further influences these phenotypic differences, prognosis, and response to therapies such as JAK2 inhibitors. The outcome of patients with the cytopenic phenotype are comparatively worse and frequently pose a challenge to treat given the inherent exacerbation of cytopenias. Recent data indicate that an innate immune deregulated state that hinges on the myddosome-IRAK-NFκB axis favors the cytopenic myelofibrosis phenotype and offers opportunity for novel treatment approaches. We will review the biological and clinical features of the MF disease spectrum and associated treatment considerations.

Published

2023

20. Splenomegaly in patients with primary or secondary myelofibrosis who are candidates for allogeneic hematopoietic cell transplantation: a Position Paper on behalf of the Chronic Malignancies Working Party of the EBMT

Author

Polverelli, Nicola, Hernández-Boluda, Juan Carlos, Czerw, Tomasz, Barbui, Tiziano, D'Adda, Mariella, Deeg, Hans Joachim, Ditschkowski, Markus, Harrison, Claire, Kröger, Nicolaus Martin, Mesa, Ruben, Passamonti, Francesco, Palandri, Francesca, Pemmaraju, Naveen, Popat, Uday, Rondelli, Damiano, Vannucchi, Alessandro Maria, Verstovsek, Srdan, Robin, Marie, Colecchia, Antonio, Grazioli, Luigi, Damiani, Enrico, Russo, Domenico, Brady, Jessica, Patch, David, Blamek, Slawomir, Damaj, Gandhi Laurent, Hayden, Patrick, McLornan, Donal P, and Yakoub-Agha, Ibrahim

Abstract

Splenomegaly is a hallmark of myelofibrosis, a debilitating haematological malignancy for which the only curative option is allogeneic haematopoietic cell transplantation (HCT). Considerable splenic enlargement might be associated with a higher risk of delayed engraftment and graft failure, increased non-relapse mortality, and worse overall survival after HCT as compared with patients without significantly enlarged splenomegaly. Currently, there are no standardised guidelines to assist transplantation physicians in deciding optimal management of splenomegaly before HCT. Therefore, the aim of this Position Paper is to offer a shared position statement on this issue. An international group of haematologists, transplantation physicians, gastroenterologists, surgeons, radiotherapists, and radiologists with experience in the treatment of myelofibrosis contributed to this Position Paper. The key issues addressed by this group included the assessment, prevalence, and clinical significance of splenomegaly, and the need for a therapeutic intervention before HCT for the control of splenomegaly. Specific scenarios, including splanchnic vein thrombosis and COVID-19, are also discussed. All patients with myelofibrosis must have their spleen size assessed before allogeneic HCT. Myelofibrosis patients with splenomegaly measuring 5 cm and larger, particularly when exceeding 15 cm below the left costal margin, or with splenomegaly-related symptoms, could benefit from treatment with the aim of reducing the spleen size before HCT. In the absence of, or loss of, response, patients with increasing spleen size should be evaluated for second-line options, depending on availability, patient fitness, and centre experience. Splanchnic vein thrombosis is not an absolute contraindication for HCT, but a multidisciplinary approach is warranted. Finally, prevention and treatment of COVID-19 should adhere to standard recommendations for immunocompromised patients.

Published

2023

21. Inhibition of ERK1/2 signaling prevents bone marrow fibrosis by reducing osteopontin plasma levels in a myelofibrosis mouse model

Author

Bianchi, Elisa, Rontauroli, Sebastiano, Tavernari, Lara, Mirabile, Margherita, Pedrazzi, Francesca, Genovese, Elena, Sartini, Stefano, Dall’Ora, Massimiliano, Grisendi, Giulia, Fabbiani, Luca, Maccaferri, Monica, Carretta, Chiara, Parenti, Sandra, Fantini, Sebastian, Bartalucci, Niccolò, Calabresi, Laura, Balliu, Manjola, Guglielmelli, Paola, Potenza, Leonardo, Tagliafico, Enrico, Losi, Lorena, Dominici, Massimo, Luppi, Mario, Vannucchi, Alessandro Maria, and Manfredini, Rossella

Abstract

Clonal myeloproliferation and development of bone marrow (BM) fibrosis are the major pathogenetic events in myelofibrosis (MF). The identification of novel antifibrotic strategies is of utmost importance since the effectiveness of current therapies in reverting BM fibrosis is debated. We previously demonstrated that osteopontin (OPN) has a profibrotic role in MF by promoting mesenchymal stromal cells proliferation and collagen production. Moreover, increased plasma OPN correlated with higher BM fibrosis grade and inferior overall survival in MF patients. To understand whether OPN is a druggable target in MF, we assessed putative inhibitors of OPN expression in vitro and identified ERK1/2 as a major regulator of OPN production. Increased OPN plasma levels were associated with BM fibrosis development in the Romiplostim-induced MF mouse model. Moreover, ERK1/2 inhibition led to a remarkable reduction of OPN production and BM fibrosis in Romiplostim-treated mice. Strikingly, the antifibrotic effect of ERK1/2 inhibition can be mainly ascribed to the reduced OPN production since it could be recapitulated through the administration of anti-OPN neutralizing antibody. Our results demonstrate that OPN is a novel druggable target in MF and pave the way to antifibrotic therapies based on the inhibition of ERK1/2-driven OPN production or the neutralization of OPN activity.

Published

2023

22. Molecular prognostication in Ph-negative MPNs in 2022

Author

Vannucchi, Alessandro Maria and Guglielmelli, Paola

Abstract

The application of genomic techniques, including cytogenetics and DNA sequencing, to decipher the molecular landscape of patients with myeloproliferative neoplasms (MPNs) has radically modified diagnostic approach and management through improved risk stratification. Three driver mutated genes (JAK2, MPL, CALR) are variably harbored by >80% of patients and associated with clinical characteristics, as well as major disease-related complications and different survival outcomes. Therefore, JAK2 V617F mutation is included in the revised International Prognosis Score of Thrombosis for Essential Thrombocythemia score for prediction of thrombosis in patients with essential thrombocythemia and prefibrotic primary myelofibrosis, while a CALR type 1 mutated genotype constitutes a favorable variable for survival in patients with myelofibrosis (MF). Novel, integrated clinical and cytogenetic/mutation scores (Mutation-Enhanced International Prognostic Score System for Transplantation-Age Patients with Primary Myelofibrosis [MIPSS70/v2], genetically inspired prognostic scoring system [GIPSS], Myelofibrosis Secondary to PV and ET- Prognostic Model [MYSEC-PM]) have been devised that guide selection of stem cell transplantation candidates with MF or help predict the risk associated with the transplant procedure (Myelofibrosis Transplant Scoring System), with greater performance compared with conventional scores based on hematologic and clinical variables only. On the other hand, several clinical needs remain unmet despite the great amount of molecular information available nowadays. These include the prediction of evolution to acute leukemia in a clinically actionable time frame, the identification of patients most likely to derive durable benefits from target agents, in primis JAK inhibitors, and, conversely, the significance of molecular responses that develop in patients receiving interferon or some novel agents. Here, we discuss briefly the significance and the role of genomic analysis for prognostication in patients with MPNs from a clinician's point of view, with the intent to provide how-to-use hints.

Published

2022

23. Genomic profiling for clinical decision making in myeloid neoplasms and acute leukemia

Author

Duncavage, Eric J., Bagg, Adam, Hasserjian, Robert P., DiNardo, Courtney D., Godley, Lucy A., Iacobucci, Ilaria, Jaiswal, Siddhartha, Malcovati, Luca, Vannucchi, Alessandro M., Patel, Keyur P., Arber, Daniel A., Arcila, Maria E., Bejar, Rafael, Berliner, Nancy, Borowitz, Michael J., Branford, Susan, Brown, Anna L., Cargo, Catherine A., Döhner, Hartmut, Falini, Brunangelo, Garcia-Manero, Guillermo, Haferlach, Torsten, Hellström-Lindberg, Eva, Kim, Annette S., Klco, Jeffery M., Komrokji, Rami, Lee-Cheun Loh, Mignon, Loghavi, Sanam, Mullighan, Charles G., Ogawa, Seishi, Orazi, Attilio, Papaemmanuil, Elli, Reiter, Andreas, Ross, David M., Savona, Michael, Shimamura, Akiko, Skoda, Radek C., Solé, Francesc, Stone, Richard M., Tefferi, Ayalew, Walter, Matthew J., Wu, David, Ebert, Benjamin L., and Cazzola, Mario

Abstract

Myeloid neoplasms and acute leukemias derive from the clonal expansion of hematopoietic cells driven by somatic gene mutations. Although assessment of morphology plays a crucial role in the diagnostic evaluation of patients with these malignancies, genomic characterization has become increasingly important for accurate diagnosis, risk assessment, and therapeutic decision making. Conventional cytogenetics, a comprehensive and unbiased method for assessing chromosomal abnormalities, has been the mainstay of genomic testing over the past several decades and remains relevant today. However, more recent advances in sequencing technology have increased our ability to detect somatic mutations through the use of targeted gene panels, whole-exome sequencing, whole-genome sequencing, and whole-transcriptome sequencing or RNA sequencing. In patients with myeloid neoplasms, whole-genome sequencing represents a potential replacement for both conventional cytogenetic and sequencing approaches, providing rapid and accurate comprehensive genomic profiling. DNA sequencing methods are used not only for detecting somatically acquired gene mutations but also for identifying germline gene mutations associated with inherited predisposition to hematologic neoplasms. The 2022 International Consensus Classification of myeloid neoplasms and acute leukemias makes extensive use of genomic data. The aim of this report is to help physicians and laboratorians implement genomic testing for diagnosis, risk stratification, and clinical decision making and illustrates the potential of genomic profiling for enabling personalized medicine in patients with hematologic neoplasms.

Published

2022

24. Genomic profiling for clinical decision making in myeloid neoplasms and acute leukemia

Author

Duncavage, Eric J., Bagg, Adam, Hasserjian, Robert P., DiNardo, Courtney D., Godley, Lucy A., Iacobucci, Ilaria, Jaiswal, Siddhartha, Malcovati, Luca, Vannucchi, Alessandro M., Patel, Keyur P., Arber, Daniel A., Arcila, Maria E., Bejar, Rafael, Berliner, Nancy, Borowitz, Michael J., Branford, Susan, Brown, Anna L., Cargo, Catherine A., Döhner, Hartmut, Falini, Brunangelo, Garcia-Manero, Guillermo, Haferlach, Torsten, Hellström-Lindberg, Eva, Kim, Annette S., Klco, Jeffery M., Komrokji, Rami, Lee-Cheun Loh, Mignon, Loghavi, Sanam, Mullighan, Charles G., Ogawa, Seishi, Orazi, Attilio, Papaemmanuil, Elli, Reiter, Andreas, Ross, David M., Savona, Michael, Shimamura, Akiko, Skoda, Radek C., Solé, Francesc, Stone, Richard M., Tefferi, Ayalew, Walter, Matthew J., Wu, David, Ebert, Benjamin L., and Cazzola, Mario

Abstract

Myeloid neoplasms and acute leukemias derive from the clonal expansion of hematopoietic cells driven by somatic gene mutations. Although assessment of morphology plays a crucial role in the diagnostic evaluation of patients with these malignancies, genomic characterization has become increasingly important for accurate diagnosis, risk assessment, and therapeutic decision making. Conventional cytogenetics, a comprehensive and unbiased method for assessing chromosomal abnormalities, has been the mainstay of genomic testing over the past several decades and remains relevant today. However, more recent advances in sequencing technology have increased our ability to detect somatic mutations through the use of targeted gene panels, whole-exome sequencing, whole-genome sequencing, and whole-transcriptome sequencing or RNA sequencing. In patients with myeloid neoplasms, whole-genome sequencing represents a potential replacement for both conventional cytogenetic and sequencing approaches, providing rapid and accurate comprehensive genomic profiling. DNA sequencing methods are used not only for detecting somatically acquired gene mutations but also for identifying germline gene mutations associated with inherited predisposition to hematologic neoplasms. The 2022 International Consensus Classification of myeloid neoplasms and acute leukemias makes extensive use of genomic data. The aim of this report is to help physicians and laboratorians implement genomic testing for diagnosis, risk stratification, and clinical decision making and illustrates the potential of genomic profiling for enabling personalized medicine in patients with hematologic neoplasms.

Published

2022

25. Protection Against Breakthrough Delta/Omicron Variants in Vaccinated Patients with Myeloproliferative Neoplasms (MPN)

Author

Barbui, Tiziano, Carobbio, Alessandra, Ghirardi, Arianna, Iurlo, Alessandra, De Stefano, Valerio, Sobas, Marta Anna, Rumi, Elisa, Elli, Elena Maria, Lunghi, Francesca, Gasior Kabat, Mercedes, Cuevas, Beatriz, Guglielmelli, Paola, Bonifacio, Massimiliano, Marchetti, Monia, Alvarez-Larran, Alberto, Fox, Laura Maria, Bellini, Marta, Daffini, Rosa, Benevolo, Giulia, Carreño, Gonzalo, Patriarca, Andrea, Al-Ali, Haifa Kathrin, Andrade, Marcio, Palandri, Francesca, Harrison, Claire, Foncillas, Maria Angeles, Osorio, Santiago, Koschmieder, Steffen, Magro, Elena, Kiladjian, Jean-Jacques, Bolaños, Estefanía, Heidel, Florian H., Quiroz, Keina, Griesshammer, Martin, García Gutiérrez, Valentín, Marin Sanchez, Alberto, Hernandez Boluda, Juan Carlos, Lopez Abadia, Emma, Carli, Giuseppe, Sagüés, Miguel, Kusec, Rajko, Xicoy, Blanca, Guenova, Margarita, Navas, Begoña, Angona, Anna, Cichocka, Edyta, Masternak, Anna, Cattaneo, Daniele, Bucelli, Cristina, Betti, Silvia, Borsani, Oscar, Cavalca, Fabrizio, Carbonell, Sara, Curto-Garcia, Natalia, Benajiba, Lina, Rambaldi, Alessandro, and Vannucchi, Alessandro M.

Published

2022

26. MYF3001: A Randomized Open Label, Phase 3 Study to Evaluate Imetelstat Versus Best Available Therapy in Patients with Intermediate-2 or High-Risk Myelofibrosis Relapsed/Refractory to Janus Kinase Inhibitor

Author

Mascarenhas, John, Harrison, Claire, Kiladjian, Jean-Jacques, Komrokji, Rami S., Koschmieder, Steffen, Vannucchi, Alessandro M., Berry, Tymara, Redding, Denise, Sherman, Laurie, Dougherty, Souria, Peng, Lixian, Sun, Libo, Huang, Fei, Wan, Ying, Feller, Faye, and Verstovsek, Srdan

Published

2022

27. A Phase 2 Study of the LSD1 Inhibitor Bomedemstat (IMG-7289) for the Treatment of Essential Thrombocythemia (ET)

Author

Gill, Harinder, Palandri, Francesca, Ross, David M, Cochrane, Tara, Tate, Courtney, Lane, Steven W, Larsen, Stephen R, Gerds, Aaron T., Halpern, Anna B., Shortt, Jake, Rossetti, James M., Pettit, Kristen M., Liang, James, Mead, Adam J, Marchetti, Monia, Vannucchi, Alessandro M., Wilson, Andrew J, Göthert, Joachim R, Hanna, Merit, Passamonti, Francesco, Stevenson, William S, Harrison, Claire, Talpaz, Moshe, Vianelli, Nicola, and Rienhoff, Hugh Young

Published

2022

28. Pelabresib (CPI-0610) As Add-on to Ruxolitinib in Myelofibrosis: Durability of Response and Safety Beyond Week 24 in the Phase 2 MANIFEST Study

Author

Harrison, Claire, Kremyanskaya, Marina, Bose, Prithviraj, Gupta, Vikas, Rampal, Raajit K, Lambert, Jonathan, Talpaz, Moshe, Vannucchi, Alessandro, Kuykendall, Andrew, Kiladjian, Jean-Jacques, Verstovsek, Srdan, Mesa, Ruben, Colak, Gozde, Klein, Sandra, Dutta, Soumik, and Mascarenhas, John

Published

2022

29. Pelabresib (CPI-0610) As Add-on to Ruxolitinib in Myelofibrosis: Durability of Response and Safety Beyond Week 24 in the Phase 2 MANIFEST Study

Author

Harrison, Claire, Kremyanskaya, Marina, Bose, Prithviraj, Gupta, Vikas, Rampal, Raajit K, Lambert, Jonathan, Talpaz, Moshe, Vannucchi, Alessandro, Kuykendall, Andrew, Kiladjian, Jean-Jacques, Verstovsek, Srdan, Mesa, Ruben, Colak, Gozde, Klein, Sandra, Dutta, Soumik, and Mascarenhas, John

Published

2022

30. Updated Results from the Momentum Phase 3 Study of Momelotinib (MMB) Versus Danazol (DAN) in Symptomatic and Anemic Myelofibrosis (MF) Patients Previously Treated with a JAK Inhibitor

Author

Gerds, Aaron T., Mesa, Ruben, Vannucchi, Alessandro M, Al-Ali, Haifa Kathrin, Lavie, David, Kuykendall, Andrew, Grosicki, Sebastian, Iurlo, Alessandra, Goh, Yeow Tee, Lazaroiu, Mihaela, Egyed, Miklos, Fox, Maria Laura, McLornan, Donal P., Perkins, Andrew Charles, Yoon, Sung-Soo, Gupta, Vikas, Kiladjian, Jean-Jacques, Donahue, Rafe, Kawashima, Jun, and Verstovsek, Srdan

Published

2022

31. Protection Against Breakthrough Delta/Omicron Variants in Vaccinated Patients with Myeloproliferative Neoplasms (MPN)

Author

Barbui, Tiziano, Carobbio, Alessandra, Ghirardi, Arianna, Iurlo, Alessandra, De Stefano, Valerio, Sobas, Marta Anna, Rumi, Elisa, Elli, Elena Maria, Lunghi, Francesca, Gasior Kabat, Mercedes, Cuevas, Beatriz, Guglielmelli, Paola, Bonifacio, Massimiliano, Marchetti, Monia, Alvarez-Larran, Alberto, Fox, Laura Maria, Bellini, Marta, Daffini, Rosa, Benevolo, Giulia, Carreño, Gonzalo, Patriarca, Andrea, Al-Ali, Haifa Kathrin, Andrade, Marcio, Palandri, Francesca, Harrison, Claire, Foncillas, Maria Angeles, Osorio, Santiago, Koschmieder, Steffen, Magro, Elena, Kiladjian, Jean-Jacques, Bolaños, Estefanía, Heidel, Florian H., Quiroz, Keina, Griesshammer, Martin, García Gutiérrez, Valentín, Marin Sanchez, Alberto, Hernandez Boluda, Juan Carlos, Lopez Abadia, Emma, Carli, Giuseppe, Sagüés, Miguel, Kusec, Rajko, Xicoy, Blanca, Guenova, Margarita, Navas, Begoña, Angona, Anna, Cichocka, Edyta, Masternak, Anna, Cattaneo, Daniele, Bucelli, Cristina, Betti, Silvia, Borsani, Oscar, Cavalca, Fabrizio, Carbonell, Sara, Curto-Garcia, Natalia, Benajiba, Lina, Rambaldi, Alessandro, and Vannucchi, Alessandro M.

Published

2022

32. Improvement in Individual Symptoms and Total Symptom Score (TSS) and Matching-Adjusted Indirect Comparison (MAIC) Analysis to Compare TSS As a Continuous Endpoint in Patients with Myelofibrosis Treated with Pelabresib in Combination with Ruxolitinib Versus Janus Kinase Inhibitor Monotherapy

Author

Mesa, Ruben, Kremyanskaya, Marina, Patriarca, Andrea, Gupta, Vikas, Palandri, Francesca, Devos, Timothy, Harrison, Claire, Rampal, Raajit K., Talpaz, Moshe, Vannucchi, Alessandro, Kuykendall, Andrew, Kiladjian, Jean-Jacques, Verstovsek, Srdan, Colak, Gozde, Dey, Debarshi, and Mascarenhas, John

Published

2022

33. A Phase 2 Study of the LSD1 Inhibitor Bomedemstat (IMG-7289) for the Treatment of Advanced Myelofibrosis (MF): Updated Results and Genomic Analyses

Author

Pettit, Kristen M., Gill, Harinder, Yacoub, Abdulraheem, Bradley, Terrence, Gerds, Aaron T., Tatarczuch, Maciej, Shortt, Jake, Curtin, Natasha Joan, Rossetti, James M., Burbury, Kate, Mead, Adam J, Göthert, Joachim R, Koschmieder, Steffen, Reyer, Matt, Siranosian, Benjamin, Natsoulis, Georges, Stevenson, William S, Ewing, Joanne, Chacko, Joseph M., Rumi, Elisa, Halpern, Anna B., Palandri, Francesca, Vianelli, Nicola, Passamonti, Francesco, Mesa, Ruben, Marchetti, Monia, Harrison, Claire, Vannucchi, Alessandro M., Watts, Justin, Ross, David M, Talpaz, Moshe, and Rienhoff, Hugh Young

Published

2022

34. Pelabresib (CPI-0610) Combined with Ruxolitinib for JAK Inhibitor Treatment-Naïve Patients with Myelofibrosis: Durability of Response and Safety Beyond Week 24

Author

Mascarenhas, John, Kremyanskaya, Marina, Patriarca, Andrea, Gupta, Vikas, Palandri, Francesca, Devos, Timothy, Rampal, Raajit K, Talpaz, Moshe, Vannucchi, Alessandro, Kuykendall, Andrew, Kiladjian, Jean-Jacques, Verstovsek, Srdan, Mesa, Ruben, Colak, Gozde, Li, Qing, Klein, Sandra, and Harrison, Claire

Published

2022

35. Pelabresib (CPI-0610) Combined with Ruxolitinib for JAK Inhibitor Treatment-Naïve Patients with Myelofibrosis: Durability of Response and Safety Beyond Week 24

Author

Mascarenhas, John, Kremyanskaya, Marina, Patriarca, Andrea, Gupta, Vikas, Palandri, Francesca, Devos, Timothy, Rampal, Raajit K, Talpaz, Moshe, Vannucchi, Alessandro, Kuykendall, Andrew, Kiladjian, Jean-Jacques, Verstovsek, Srdan, Mesa, Ruben, Colak, Gozde, Li, Qing, Klein, Sandra, and Harrison, Claire

Published

2022

36. Siremadlin, a Human Double Minute-2 (HDM2) Inhibitor, Added to Ruxolitinib after Suboptimal Response to Ruxolitinib Alone in Patients with Myelofibrosis: Results from Part 1 of the Phase 1/2 Adore Study

Author

Heidel, Florian H, Perkins, Andrew Charles, Reiter, Andreas, Crodel, Carl C., Riley, Caroline Hasselbalch, Gómez-Casares, María Teresa, Takacs, Istvan, Becker, Heiko, Lehmann, Thomas, Vinogradova, Olga, Burbury, Kate, Vannucchi, Alessandro M., Gupta, Vikas, Harrison, Claire, Wondergem, Marielle, Kiladjian, Jean-Jacques, Cleary, Grace, Zhang, Angela, Mahuzier, Bruyère, Kota, Jagannath, Prahallad, Anirudh, and Ross, David M

Published

2022

37. Improvement in Individual Symptoms and Total Symptom Score (TSS) and Matching-Adjusted Indirect Comparison (MAIC) Analysis to Compare TSS As a Continuous Endpoint in Patients with Myelofibrosis Treated with Pelabresib in Combination with Ruxolitinib Versus Janus Kinase Inhibitor Monotherapy

Author

Mesa, Ruben, Kremyanskaya, Marina, Patriarca, Andrea, Gupta, Vikas, Palandri, Francesca, Devos, Timothy, Harrison, Claire, Rampal, Raajit K., Talpaz, Moshe, Vannucchi, Alessandro, Kuykendall, Andrew, Kiladjian, Jean-Jacques, Verstovsek, Srdan, Colak, Gozde, Dey, Debarshi, and Mascarenhas, John

Published

2022

38. A Phase 2 Study of the LSD1 Inhibitor Bomedemstat (IMG-7289) for the Treatment of Advanced Myelofibrosis (MF): Updated Results and Genomic Analyses

Author

Pettit, Kristen M., Gill, Harinder, Yacoub, Abdulraheem, Bradley, Terrence, Gerds, Aaron T., Tatarczuch, Maciej, Shortt, Jake, Curtin, Natasha Joan, Rossetti, James M., Burbury, Kate, Mead, Adam J, Göthert, Joachim R, Koschmieder, Steffen, Reyer, Matt, Siranosian, Benjamin, Natsoulis, Georges, Stevenson, William S, Ewing, Joanne, Chacko, Joseph M., Rumi, Elisa, Halpern, Anna B., Palandri, Francesca, Vianelli, Nicola, Passamonti, Francesco, Mesa, Ruben, Marchetti, Monia, Harrison, Claire, Vannucchi, Alessandro M., Watts, Justin, Ross, David M, Talpaz, Moshe, and Rienhoff, Hugh Young

Published

2022

39. A Phase 2 Study of the LSD1 Inhibitor Bomedemstat (IMG-7289) for the Treatment of Essential Thrombocythemia (ET)

Author

Gill, Harinder, Palandri, Francesca, Ross, David M, Cochrane, Tara, Tate, Courtney, Lane, Steven W, Larsen, Stephen R, Gerds, Aaron T., Halpern, Anna B., Shortt, Jake, Rossetti, James M., Pettit, Kristen M., Liang, James, Mead, Adam J, Marchetti, Monia, Vannucchi, Alessandro M., Wilson, Andrew J, Göthert, Joachim R, Hanna, Merit, Passamonti, Francesco, Stevenson, William S, Harrison, Claire, Talpaz, Moshe, Vianelli, Nicola, and Rienhoff, Hugh Young

Published

2022

40. Updated Results from the Momentum Phase 3 Study of Momelotinib (MMB) Versus Danazol (DAN) in Symptomatic and Anemic Myelofibrosis (MF) Patients Previously Treated with a JAK Inhibitor

Author

Gerds, Aaron T., Mesa, Ruben, Vannucchi, Alessandro M, Al-Ali, Haifa Kathrin, Lavie, David, Kuykendall, Andrew, Grosicki, Sebastian, Iurlo, Alessandra, Goh, Yeow Tee, Lazaroiu, Mihaela, Egyed, Miklos, Fox, Maria Laura, McLornan, Donal P., Perkins, Andrew Charles, Yoon, Sung-Soo, Gupta, Vikas, Kiladjian, Jean-Jacques, Donahue, Rafe, Kawashima, Jun, and Verstovsek, Srdan

Published

2022

41. Siremadlin, a Human Double Minute-2 (HDM2) Inhibitor, Added to Ruxolitinib after Suboptimal Response to Ruxolitinib Alone in Patients with Myelofibrosis: Results from Part 1 of the Phase 1/2 Adore Study

Author

Heidel, Florian H, Perkins, Andrew Charles, Reiter, Andreas, Crodel, Carl C., Riley, Caroline Hasselbalch, Gómez-Casares, María Teresa, Takacs, Istvan, Becker, Heiko, Lehmann, Thomas, Vinogradova, Olga, Burbury, Kate, Vannucchi, Alessandro M., Gupta, Vikas, Harrison, Claire, Wondergem, Marielle, Kiladjian, Jean-Jacques, Cleary, Grace, Zhang, Angela, Mahuzier, Bruyère, Kota, Jagannath, Prahallad, Anirudh, and Ross, David M

Published

2022

42. MYF3001: A Randomized Open Label, Phase 3 Study to Evaluate Imetelstat Versus Best Available Therapy in Patients with Intermediate-2 or High-Risk Myelofibrosis Relapsed/Refractory to Janus Kinase Inhibitor

Author

Mascarenhas, John, Harrison, Claire, Kiladjian, Jean-Jacques, Komrokji, Rami S., Koschmieder, Steffen, Vannucchi, Alessandro M., Berry, Tymara, Redding, Denise, Sherman, Laurie, Dougherty, Souria, Peng, Lixian, Sun, Libo, Huang, Fei, Wan, Ying, Feller, Faye, and Verstovsek, Srdan

Published

2022

43. Efficacy and safety of avapritinib in previously treated patients with advanced systemic mastocytosis

Author

Reiter, Andreas, Schwaab, Juliana, DeAngelo, Daniel J., Gotlib, Jason, Deininger, Michael W., Pettit, Kristen M., Alvarez-Twose, Iván, Vannucchi, Alessandro M., Panse, Jens, Platzbecker, Uwe, Hermine, Olivier, Dybedal, Ingunn, Lin, Hui-Min, Rylova, Svetlana N., Ehlert, Katrin, Dimitrijević, Saša, and Radia, Deepti H.

Abstract

Advanced systemic mastocytosis (AdvSM) is a rare myeloid neoplasm, driven by the KIT D816V mutation in >90% of patients. Avapritinib, a potent, highly selective D816V-mutant KIT inhibitor, is approved for treatment of adults with AdvSM by the US Food and Drug Administration, regardless of prior therapy, and the European Medicines Agency for patients with prior systemic therapy, based on EXPLORER (#NCT02561988; clinicaltrials.gov) and PATHFINDER (#NCT03580655; clinicaltrials.gov) clinical studies. We present latest pooled efficacy and safety analyses from patients who received ≥1 systemic therapy prior to avapritinib in EXPLORER/PATHFINDER. Overall response rate in response-evaluable patients (n = 31) was 71% (95% confidence interval: 52% to 86%; 22/31), including 19% (6/31) with complete remission (CR)/CR with partial recovery of peripheral blood counts (CRh). Median time to response was 2.3 months, median time to CR/CRh was 7.4 months, and median duration of response (DOR) was not reached. Reductions ≥50% in bone marrow mast cell infiltration (89%), KIT D816V variant allele fraction (66%), serum tryptase (89%), and reductions ≥35% in spleen size (70%) occurred in most patients. Median OS was not reached (median follow-up 17.7 months). Avapritinib was effective in all AdvSM subtypes, regardless of number/type of prior therapies or poor prognostic somatic mutations. Treatment-related adverse events (TRAEs) were observed in 94% of patients, most commonly grade 1/2; 57% had TRAEs of at least grade 3; 81% remained on treatment at 6 months. Avapritinib in adults with AdvSM who received prior systemic therapy was generally well tolerated, with high response rates regardless of prior systemic therapy.

Published

2022

44. Site‐specific venous thrombosis in essential thrombocythemia: Impact on subsequent vascular events and survival

Author

Gangat, Naseema, Singh, Amritpal, Szuber, Natasha, Begna, Kebede, Elliott, Michelle, Wolanskyj‐Spinner, Alexandra, Hanson, Curtis A., Pardanani, Animesh, De Stefano, Valerio, Barbui, Tiziano, Vannucchi, Alessandro M., and Tefferi, Ayalew

Published

2022

45. Site‐specific venous thrombosis in essential thrombocythemia: Impact on subsequent vascular events and survival

Author

Gangat, Naseema, Singh, Amritpal, Szuber, Natasha, Begna, Kebede, Elliott, Michelle, Wolanskyj‐Spinner, Alexandra, Hanson, Curtis A., Pardanani, Animesh, De Stefano, Valerio, Barbui, Tiziano, Vannucchi, Alessandro M., and Tefferi, Ayalew

Published

2022

46. International Consensus Classification of Myeloid Neoplasms and Acute Leukemias: integrating morphologic, clinical, and genomic data

Author

Arber, Daniel A., Orazi, Attilio, Hasserjian, Robert P., Borowitz, Michael J., Calvo, Katherine R., Kvasnicka, Hans-Michael, Wang, Sa A., Bagg, Adam, Barbui, Tiziano, Branford, Susan, Bueso-Ramos, Carlos E., Cortes, Jorge E., Dal Cin, Paola, DiNardo, Courtney D., Dombret, Hervé, Duncavage, Eric J., Ebert, Benjamin L., Estey, Elihu H., Facchetti, Fabio, Foucar, Kathryn, Gangat, Naseema, Gianelli, Umberto, Godley, Lucy A., Gökbuget, Nicola, Gotlib, Jason, Hellström-Lindberg, Eva, Hobbs, Gabriela S., Hoffman, Ronald, Jabbour, Elias J., Kiladjian, Jean-Jacques, Larson, Richard A., Le Beau, Michelle M., Loh, Mignon L.-C., Löwenberg, Bob, Macintyre, Elizabeth, Malcovati, Luca, Mullighan, Charles G., Niemeyer, Charlotte, Odenike, Olatoyosi M., Ogawa, Seishi, Orfao, Alberto, Papaemmanuil, Elli, Passamonti, Francesco, Porkka, Kimmo, Pui, Ching-Hon, Radich, Jerald P., Reiter, Andreas, Rozman, Maria, Rudelius, Martina, Savona, Michael R., Schiffer, Charles A., Schmitt-Graeff, Annette, Shimamura, Akiko, Sierra, Jorge, Stock, Wendy A., Stone, Richard M., Tallman, Martin S., Thiele, Jürgen, Tien, Hwei-Fang, Tzankov, Alexandar, Vannucchi, Alessandro M., Vyas, Paresh, Wei, Andrew H., Weinberg, Olga K., Wierzbowska, Agnieszka, Cazzola, Mario, Döhner, Hartmut, and Tefferi, Ayalew

Abstract

The classification of myeloid neoplasms and acute leukemias was last updated in 2016 within a collaboration between the World Health Organization (WHO), the Society for Hematopathology, and the European Association for Haematopathology. This collaboration was primarily based on input from a clinical advisory committees (CACs) composed of pathologists, hematologists, oncologists, geneticists, and bioinformaticians from around the world. The recent advances in our understanding of the biology of hematologic malignancies, the experience with the use of the 2016 WHO classification in clinical practice, and the results of clinical trials have indicated the need for further revising and updating the classification. As a continuation of this CAC-based process, the authors, a group with expertise in the clinical, pathologic, and genetic aspects of these disorders, developed the International Consensus Classification (ICC) of myeloid neoplasms and acute leukemias. Using a multiparameter approach, the main objective of the consensus process was the definition of real disease entities, including the introduction of new entities and refined criteria for existing diagnostic categories, based on accumulated data. The ICC is aimed at facilitating diagnosis and prognostication of these neoplasms, improving treatment of affected patients, and allowing the design of innovative clinical trials.

Published

2022

47. Overall survival in the SIMPLIFY-1 and SIMPLIFY-2 phase 3 trials of momelotinib in patients with myelofibrosis

Author

Mesa, Ruben, Harrison, Claire, Oh, Stephen T., Gerds, Aaron T., Gupta, Vikas, Catalano, John, Cervantes, Francisco, Devos, Timothy, Hus, Marek, Kiladjian, Jean-Jacques, Lech-Maranda, Ewa, McLornan, Donal, Vannucchi, Alessandro M., Platzbecker, Uwe, Huang, Mei, Strouse, Bryan, Klencke, Barbara, and Verstovsek, Srdan

Abstract

Janus kinase inhibitors (JAKi) approved for myelofibrosis provide spleen and symptom improvements but do not address anemia, a negative prognostic factor. Momelotinib, an inhibitor of ACVR1/ALK2, JAK1 and JAK2, demonstrated activity against anemia, symptoms, and splenomegaly in the phase 3 SIMPLIFY trials. Here, we report mature overall survival (OS) and leukemia-free survival (LFS) from both studies, and retrospective analyses of baseline characteristics and efficacy endpoints for OS associations. Survival distributions were similar between JAKi-naïve patients randomized to momelotinib, or ruxolitinib then momelotinib, in SIMPLIFY-1 (OS HR = 1.02 [0.73, 1.43]; LFS HR = 1.08 [0.78, 1.50]). Two-year OS and LFS were 81.6% and 80.7% with momelotinib and 80.6% and 79.3% with ruxolitinib then momelotinib. In ruxolitinib-exposed patients in SIMPLIFY-2, two-year OS and LFS were 65.8% and 64.2% with momelotinib and 61.2% and 59.7% with best available therapy then momelotinib (OS HR = 0.98 [0.59, 1.62]; LFS HR = 0.97 [0.59, 1.60]). Baseline transfusion independence (TI) was associated with improved survival in both studies (SIMPLIFY-1 HR = 0.474, p= 0.0001; SIMPLIFY-2 HR = 0.226, p= 0.0005). Week 24 TI response in JAKi-naïve, momelotinib-randomized patients was associated with improved OS in univariate (HR = 0.323; p< 0.0001) and multivariate (HR = 0.311; p< 0.0001) analyses. These findings underscore the importance of achieving or maintaining TI in myelofibrosis, supporting the clinical relevance of momelotinib’s pro-erythropoietic mechanism of action, and potentially informing treatment decision-making.

Published

2022

48. 1.5 million platelet count limit at essential thrombocythemia diagnosis: correlations and relevance to vascular events

Author

Gangat, Naseema, Szuber, Natasha, Jadoon, Yamna, Farrukh, Faiqa, Begna, Kebede, Elliott, Michelle A., Wolanskyj-Spinner, Alexandra P., Hanson, Curtis A., Pardanani, Animesh D., De Stefano, Valerio, Barbui, Tiziano, Vannucchi, Alessandro Maria, and Tefferi, Ayalew

Published

2022

49. 1.5 million platelet count limit at essential thrombocythemia diagnosis: correlations and relevance to vascular events

Author

Gangat, Naseema, Szuber, Natasha, Jadoon, Yamna, Farrukh, Faiqa, Begna, Kebede, Elliott, Michelle A., Wolanskyj-Spinner, Alexandra P., Hanson, Curtis A., Pardanani, Animesh D., De Stefano, Valerio, Barbui, Tiziano, Vannucchi, Alessandro Maria, and Tefferi, Ayalew

Published

2022

50. The Tectonic Structure and Evolution of the Potiguar‐Ceará Rifted Margin of Brazil

Author

Fonseca, Julia C., Ranero, Cesar R., Vannucchi, Paola, Iacopini, David, and Vital, Helenice

Abstract

The Brazilian Equatorial Margin (BEM) is interpreted as a transform margin, where the last segment opened during Gondwana rifting. However, margin evolution, and break‐up age remain unconstrained. We interpret >10k km of crustal‐scale seismic images extending along ∼600 km of the margin calibrated with drillholes. We determine the style and timing of tectonics across the rift system. We link changes in crustal‐scale structure and age of sediment deposits to interpret variations with the style of extension and intensity of thinning across the BEM. Observations support a rift evolution where deformation is initially distributed forming a shallow basin, subsequently focusses, and later migrates basin‐ward forming the deep‐water domain. We interpret that tectonic activity started ∼140–136 Ma and stopped earlier in the shallow basin causing minor thinning, than in the deep‐water domain with a ∼60 km wide area with 4–8 km thick crust extended in Late Aptian to Early Albian (116–110 Ma). Constraints from seismic and drilling help define an abrupt continent to ocean transition (COT) where continental crust may be abutted by oceanic crust, and breakup occurred at early Albian time. Basin sedimentation from the onset to the Late Aptian is continental, indicating an isolated environment disconnected from Atlantic oceans. During late‐most Aptian to Early Albian basin sedimentation changes and indicates a comparatively rapid marine water infill. Rifting of the BEM is not dominated by transcurrent deformation as previously inferred, with strike‐slip faulting limited to comparatively small sectors, whereas most of the margin extended by normal faulting deformation. Rifting occurs when stretching of continental lithosphere causes its extension and thinning. When extension continues, it leads to break‐up and the generation of a new spreading center. The basin is then split into two conjugate margins that diverge from each other as oceanic spreading creates new seafloor. Rifted margins attract studies as they host resources and may play a role in the impending energy transition. However, the vast majority of rifted margins are insufficiently studied. We have investigated the Brazil Equatorial Margin (BEM), the last region linking Africa and South America during Gondwana breakup, using a large seismic and drillholes data set released by industry. We investigated the tectonic structure and the sediment deposits, and how their joint analysis provides the information to unravel the history of deformation and the processes shaping rifting. Our interpretation supports that the opening of the margin was dominated by normal faulting kinematics rather than the transform‐type deformation previously inferred. Lithospheric deformation initiated with widespread distributed extension and was followed by localization of deformation causing focused thinning. Faulting later migrated basin‐ward creating <10 km thick crust forming a 50–70 km wide region. Break up and the first oceanic crust are possibly Earliest Albian time. Newly available seismic and drillhole information provide a novel view into the development of the Brazil Equatorial MarginWe provide a new conceptual model for rifting and ages for the different processes involved, including breakup and Continental Ocean Transition formation and ageWe propose a rift model in which deformation starts distributed, later localizes, and finally faulting evolves sequentially to break up Newly available seismic and drillhole information provide a novel view into the development of the Brazil Equatorial Margin We provide a new conceptual model for rifting and ages for the different processes involved, including breakup and Continental Ocean Transition formation and age We propose a rift model in which deformation starts distributed, later localizes, and finally faulting evolves sequentially to break up

Published

2024