bims-hemali Biomed News
on Hematologic malignancies
Issue of 2026–01–25
thirty papers selected by
Alexandros Alexandropoulos, Γενικό Νοσοκομείο Αθηνών Λαϊκό
  1. Introduction to a How I Treat series on chronic myeloid leukemia.
  2. Advances of next-generation STAMP inhibitors in chronic myeloid leukemia.
  3. Three-year follow-up of epcoritamab therapy in Japanese patients with relapsed/refractory follicular lymphoma in EPCORE NHL-3.
  4. Second attempt to discontinue TKI after molecular relapse in patients with chronic myeloid leukemia: A real-life Italian multicenter study.
  5. Ibrutinib in combination with rituximab, methotrexate, vincristine, and procarbazine (R-MVP/i) for newly diagnosed primary CNS lymphoma (PCNSL).
  6. Treatment-free remission after two nilotinib consolidation durations in chronic myeloid leukemia treated with imatinib: Phase 3 ENESTPath results.
  7. Drug resistance in chronic myeloid leukemia: the involvement of Galectin-1 and Galectin-3.
  8. Triplet regimens for frontline treatment of CLL-Great company or just a crowd?
  9. Novel targeted therapies in chronic myeloid leukemia.
  10. Efficacy and Safety of Selinexor Combined with VRD in Newly Diagnosed Multiple Myeloma with EMD: A Phase 2 Trial.
  11. Time to Revise Myeloma Diagnostic Criteria? A Decade of Accumulated Evidence on Serum Free Light Chain Ratio ≥100.
  12. Extended long-term follow-up and the survival of Stop Imatinib study.
  13. Immunomodulatory effect of dasatinib plus blinatumomab versus ponatinib plus blinatumomab in newly diagnosed Ph+ acute lymphoblastic leukemia.
  14. Faulty antibody editing permits antiplatelet B cells in ITP.
  15. One-year consolidation with Ponatinib 15 mg in chronic myeloid leukaemia on deep molecular response with Imatinib.
  16. Therapy by omission: observation as a strategy in JMML.
  17. Clinicopathological features and management of IgM multiple myeloma and Waldenstrom macroglobulinemia.
  18. Therapeutic Potential of Exportin 1 and Aurora Kinase A Inhibition in Multiple Myeloma Cells.
  19. Diagnosis, risk stratification and management of smouldering multiple myeloma.
  20. Menin and BCL2 inhibitors- shaken and stirred.
  21. Mediastinal Gray Zone Lymphomas: Diagnostic Challenges, Clinicopathologic Overlap, and Emerging Management Strategies.
  22. Glucose-6-phosphate dehydrogenase deficiency is associated with improved survival in patients with acute myeloid leukemia treated with venetoclax and azacitidine.
  23. TP53-mutated AML with salmon-colored globules, a single Auer rod, pseudo-Chédiak-Higashi granules, and micronuclei.
  24. The Role of Stem Cell Transplantation in Hodgkin Lymphoma.
  25. Bendamustine in combination with gemcitabine and vinorelbine as salvage regimen for relapsed or refractory peripheral T-cell lymphomas: A retrospective single-centre experience.
  26. Bruton's Tyrosine Kinase: Pathophysiological Roles and Inhibitor-Based Therapeutic Advances.
  27. Optimal management of elderly/old Ph+ acute lymphoblastic leukemia patients.
  28. A comprehensive analysis of pirtobrutinib in Chinese patients with chronic lymphocytic leukaemia/small lymphocytic lymphoma (CLL/SLL): Results from the phase 3 study BRUIN CLL-321.
  29. Safety and efficacy of a pre-phase with dexamethasone followed by fractionated R-CHOP in diffuse large B-cell lymphoma patients with gastrointestinal involvement at diagnosis.
  30. Synergistic apoptosis induction in myelodysplastic syndrome cells by azacitidine and PIM-2 inhibitors via nuclear factor-kappa B pathway inhibition.
  1. Blood. 2026 Jan 22. 147(4): 319-320
    Introduction to a How I Treat series on chronic myeloid leukemia.
    Jason Gotlib.
      
    DOI:  https://doi.org/10.1182/blood.2025031933
  2. Expert Opin Investig Drugs. 2026 Jan 23. 1-15
    Advances of next-generation STAMP inhibitors in chronic myeloid leukemia.
    Alessandro Costa, Massimo Breccia.
       INTRODUCTION: Specifically Targeting the ABL1 Myristoyl Pocket inhibitors (STAMPi) have reshaped the management of chronic myeloid leukemia (CML). Yet, major challenges remain, including resistance and compound mutations, cross-intolerance, and long-term toxicities. Asciminib has shown efficacy in heavily pretreated patients and in the first-line setting, but resistance and limited benefit after ponatinib highlight the need for new therapeutic options.
    COVERED AREAS: This review summarizes preclinical and early clinical evidence on next-generation STAMPi. TGRX-678 exhibits potent activity against wild-type and mutant ABL1, including T315I, synergism with orthosteric tyrosine kinase inhibitors (TKIs), central nervous system (CNS) penetration, and encouraging phase Ia/Ib clinical activity in heavily pretreated CML. Early but promising data are also emerging for TERN-701 from the CARDINAL trial.
    EXPERT OPINION: Next-generation STAMPi may extend therapeutic options beyond asciminib by addressing resistant mutations and enabling rational dual-site inhibition. TGRX-678 ability to achieve CNS exposure raises potential in blast phase CML and Ph+ acute lymphoblastic leukemia. Key questions regarding durability, long-term safety, and optimal integration with ATP-competitive TKIs remain open. Ongoing trials will define the clinical role of these STAMPi and their potential to advance cure-directed strategies, including treatment-free remission.
    Keywords:  Chronic myeloid leukemia; STAMP inhibitor; TERN-701; TGRX-678; asciminib; tyrosine kinase inhibitor
    DOI:  https://doi.org/10.1080/13543784.2026.2618980
  3. Int J Hematol. 2026 Jan 18.
    Three-year follow-up of epcoritamab therapy in Japanese patients with relapsed/refractory follicular lymphoma in EPCORE NHL-3.
    Koji Izutsu, Daigo Akahane, Tomomi Toubai, Toko Saito, Yuko Mishima, Tomoaki Fujisaki, Momoko Nishikori, Takahiro Kumode, Youko Suehiro, Kenji Ishitsuka, Poliana Patah, Ami Takahashi, Barbara D'Angelo Månsson, Elena Favaro, Noriko Fukuhara.
       BACKGROUND: The CD3xCD20 bispecific antibody epcoritamab demonstrated deep, durable responses with manageable safety in relapsed/refractory (R/R) follicular lymphoma (FL) in EPCORE NHL-3 (phase 1/2; NCT04542824). This analysis evaluated 3-year follow-up outcomes in Japanese patients.
    METHODS: Adults with CD20 + FL and ≥ 2 prior lines of therapy (LOTs) received subcutaneous epcoritamab (0.16/0.8-mg step-up doses; 48-mg full doses) until disease progression or death. The primary endpoint was overall response rate (ORR).
    RESULTS: Twenty-one patients received epcoritamab (median age: 65 years; median prior LOTs: 4; 57.1% double refractory; 57.1% progressed within 24 months of any first-line treatment). At a median follow-up of 35 months, the ORR was 95.2% and the complete response (CR) rate was 76.2%. Median duration of response, duration of CR, progression-free survival, and overall survival were not reached. At 3 years, 66.7% and 93.3% of complete responders remained progression-free and alive, respectively. Minimal residual disease negativity was achieved in 88.9% (16/18) of evaluable patients. Common treatment-emergent adverse events included cytokine release syndrome (90.5%) and injection-site reaction (71.4%), all predominantly grade 1-2 and occurring in early treatment cycles, and none fatal.
    CONCLUSIONS: Epcoritamab monotherapy provided durable long-term remission with favorable safety in Japanese patients with R/R FL over 3 years of follow-up.
    Keywords:  Bispecific antibodies; Clinical trial; Follicular lymphoma; Non-Hodgkin lymphoma
    DOI:  https://doi.org/10.1007/s12185-025-04139-1
  4. Cancer. 2026 Feb 01. 132(3): e70261
    Second attempt to discontinue TKI after molecular relapse in patients with chronic myeloid leukemia: A real-life Italian multicenter study.
    Alessandra Iurlo, Daniele Cattaneo, Carmen Fava, Fausto Castagnetti, Massimiliano Bonifacio, Mariella D'Adda, Maria Cristina Miggiano, Isabella Capodanno, Chiara Elena, Luciano Levato, Anna Rita Scortechini, Francesca Lunghi, Marianna Caramella, Nicola Orofino, Margherita Maffioli, Valentina Bellani, Valentina Bonuomo, Selene Grano, Giulia Cotilli, Emilia Scalzulli, Matteo Dalmazzo, Sabrina Leonetti Crescenzi, Luigiana Luciano, Bruno Martino, Tamara Intermesoli, Davide Rapezzi, Gianni Binotto, Mario Tiribelli, Dario Consonni, Fabrizio Pane, Giuseppe Saglio, Carlo Gambacorti-Passerini, Massimo Breccia, Gianantonio Rosti.
       BACKGROUND: Approximately half of patients with chronic myeloid leukemia (CML) who attempted tyrosine kinase inhibitor (TKI) discontinuation for the first time experienced molecular relapse and restarted TKIs. Although several studies have already investigated first treatment-free remission (TFR) attempts (TFR1), few previously published articles have focused on the plausibility and predictors of second TFR (TFR2).
    METHODS: To evaluate the feasibility and likelihood of TFR2 success in real-life, 90 patients with CML regularly followed in 23 Italian hematological centers were analyzed; these patients reattempted TKI discontinuation after a first failed attempt.
    RESULTS: Forty-five (50.0%) patients lost major molecular response after a median of 4.0 months off therapy, whereas 45 (50.0%) remained treatment-free for a median of 18.8 months. In univariate analysis, there was no association between TFR2 and the following variables: age, gender, Sokal risk score, BCR::ABL1 transcript type, prior interferon exposure, type and number of previous TKIs, resistance to any prior TKIs, and TKI switching after TFR1. In contrast, factors identified as associated with TFR2 success included a lower ELTS risk score, a longer time from TFR1 to molecular relapse (≥3 months), as well as a longer TKI treatment and deep molecular response (DMR) duration (≥4 years) before TFR2.
    CONCLUSIONS: While confirming the critical prognostic role of ELTS risk and TKI treatment and DMR duration even before TFR2, this real-life study provides further information to support the safety of a second effort to discontinue TKIs in patients with CML, as a failed first attempt does not appear to preclude a second successful one.
    Keywords:  chronic myeloid leukemia; second treatment‐free remission; tyrosine kinase inhibitors
    DOI:  https://doi.org/10.1002/cncr.70261
  5. Neuro Oncol. 2026 Jan 20. pii: noag011. [Epub ahead of print]
    Ibrutinib in combination with rituximab, methotrexate, vincristine, and procarbazine (R-MVP/i) for newly diagnosed primary CNS lymphoma (PCNSL).
    Lauren R Schaff, Elena Pentsova, Rachna Malani, Jacqueline Stone, Igor T Gavrilovic, Thomas J Kaley, Laleh Emadi-Paramkouhi, Kerina Yang, Ashley Gonzalez, Lilian Quinn, Alyssa Rodriguez, Josey Tobin, Maya Kaluski, Anne S Reiner, Katherine S Panageas, Lisa M DeAngelis, Jasmine H Francis, Robert J Young, Ingo K Mellinghoff, Christian Grommes.
       BACKGROUND: High-dose methotrexate (MTX)-based chemotherapy is the mainstay of treatment of primary central nervous system lymphoma (PCNSL). Only ∼60% of patients achieve a complete response to first line therapy with frequent relapses. The Bruton's tyrosine kinase (BTK) inhibitor ibrutinib has shown promising antitumor activity in recurrent/refractory PCNSL. Methods: The goal of the current single-center phase 2 trial was to explore whether the addition of ibrutinib to the combination of rituximab, methotrexate, procarbazine, and vincristine ((R-MVP/i) increases complete response rate (CCR).
    RESULTS: Thirty newly diagnosed PCNSLs were enrolled; median age 69 (range 41-79), median ECOG = 1. 29 patients completed R-MVP/i, 1 withdrew consent after 2 cycles.A CR/CRu was achieved in 29 patients and a partial response in 1 for a CRR of 29/30 (97%, 95% CI : 83.3%, 99.8%)). Treatment was well tolerated with no grade 5 toxicity was observed. Eight patients experienced 13 grade 4 toxicities (lymphopenia (n = 3), neutropenia (n = 4), thrombocytopenia (n = 3) white cell count decrease (n = 3)). The most common toxicities were thrombocytopenia, anemia, lymphopenia and liver enzyme elevations. No Aspergillus or Pneumocystis infections occurred. No refractory disease was observed. For the 29 patients completing the trial, 19 received consolidation with cytarabine (Ara-C), 8 autologous stem cell transplant, 1 rituximab maintenance and 1 was observed without maintenance or consolidation. At a median follow up of 25.1 months (range 3.3-49.2), the median progression-free (PFS) and overall survival (OS) was not reached with a 2-year PFS of 84.2% (95% CI: 62.7%-93.9%).
    CONCLUSIONS: R-MVP/i was well tolerated and associated with excellent disease control and survival.
    Keywords:  R-MVP; clinical trial; first line; ibrutinib; primary central nervous system lymphoma
    DOI:  https://doi.org/10.1093/neuonc/noag011
  6. Leukemia. 2026 Jan 19.
    Treatment-free remission after two nilotinib consolidation durations in chronic myeloid leukemia treated with imatinib: Phase 3 ENESTPath results.
    Delphine Rea, Slawomira Kyrcz-Krzemien, Paolo Sportoletti, Jiří Mayer, Arpad Illes, Anna Angona Figueras, Alexander Kiani, Aude Charbonnier, Theodoros Marinakis, Leif Stenke, Juan Luis Steegmann, Giuseppe Saglio, Andrzej Hellmann, Dietger Niederwieser, Peter Schuld, Gianantonio Rosti.
      The phase 3 ENESTPath study investigated treatment-free remission (TFR) rates in patients with chronic Philadelphia chromosome-positive (Ph+) and/or BCR::ABL1+ chronic myeloid leukemia who had not achieved deep molecular response (DMR) after >2 years of imatinib treatment and were switched to nilotinib 300 mg twice daily (BID). After 24 months of treatment, patients with a stable DMR were randomized to either enter the TFR phase (Arm 1) or continue nilotinib consolidation for an additional 12 months and then enter the TFR phase if in stable DMR (Arm 2). The primary endpoint was the proportion of patients who remained in TFR (≥MR4.0 [BCR::ABL1IS ≤ 0.01%]) without molecular relapse at the end of 12 months. Of the 620 patients enrolled, 239 (38.5%) achieved stable MR4.0 and were randomized to Arm 1 (n = 120) or Arm 2 (n = 119). In the TFR phase, MR4.0 rates at 12 months (Arm 1: 31.9%, Arm 2: 37.5%; p = 0.383) and 24 months (Arm 1: 29.4%, Arm 2: 30.8%) revealed no differences in TFR success between 2 and 3 years of nilotinib. Irrespective of the consolidation duration, switching to nilotinib 300 mg BID provided the opportunity to achieve TFR if patients were unable to reach stable DMR with first-line imatinib.
    DOI:  https://doi.org/10.1038/s41375-025-02847-5
  7. Mol Biol Rep. 2026 Jan 20. 53(1): 305
    Drug resistance in chronic myeloid leukemia: the involvement of Galectin-1 and Galectin-3.
    Cansu Yıldırım.
      Tyrosine kinase inhibitors (TKIs) have proven effective in treating chronic myeloid leukemia (CML), but some patients do not benefit from these drugs because TKI-resistant CML cells persist. Galectin-1 (Gal-1) and Galectin-3 (Gal-3) have emerged as critical modulators of CML cell drug resistance. High intracellular Gal-1 levels promote multidrug resistance in vitro by inducing MDR1 expression through p38 MAPK and NF-κB activation, enhancing drug efflux and diminishing anticancer drug efficacy. The effects of Gal-1 have so far been investigated only in in vitro systems; data from in vivo mouse and human studies are not available. Activation of GSK-3β induces Gal-3, which stabilizes anti-apoptotic proteins belonging to the Bcl-2 family and confers resistance to apoptosis-inducing agents in vitro. However, this pathway has not yet been evaluated in CML mouse models or in patients, particularly in the context of TKI resistance mechanisms. Gal-3 is induced by the bone marrow microenvironment (BMME) and promotes AKT and ERK activation to support CML cell proliferation, multidrug resistance (MDR), chemotaxis, and BM lodgment. However, it has not yet been elucidated how Gal-3 is induced by BM stromal cells in CML cells. Furthermore, Gal-3 suppresses the formation of the SERPINA1-albumin complex in vitro, abolishing its growth-inhibitory effects and enhancing paracrine proliferation of CML cells. Although preclinical evidence shows that elevated intracellular Gal-3 protein levels promote drug resistance in CML, these findings have not yet been confirmed at the clinical level. This review underscores that both galectins are critical regulators of CML pathophysiology and highlight their potential as therapeutic targets to overcome TKI resistance.
    Keywords:  Chronic myeloid leukemia; Drug resistance; Galectin-1; Galectin-3; Tyrosine kinase inhibitor
    DOI:  https://doi.org/10.1007/s11033-026-11473-y
  8. Hemasphere. 2026 Jan;10(1): e70303
    Triplet regimens for frontline treatment of CLL-Great company or just a crowd?
    Sean McKeague, John F Seymour.
      Standard frontline treatment of chronic lymphocytic leukemia (CLL) is with fixed-duration venetoclax-based doublets or indefinite covalent Bruton tyrosine kinase inhibitor (BTKI). Although these approaches achieve excellent results, venetoclax doublets have diminished efficacy in high-risk biological subgroups, and indefinite covalent Bruton tyrosine kinase inhibitor (cBTKI) is associated with cumulative cardiovascular and infectious toxicity. Triplet regimens for treatment of CLL involve simultaneous use of cBTKI, venetoclax, and anti-CD20 monoclonal antibody. Three major frontline Phase 3 trials (CLL-13/GAIA, AMPLIFY, and A041702) have demonstrated higher rates of undetectable minimal residual disease (uMRD) and longer remissions with triplets than doublets, particularly in patients with IGHV-unmutated (IGHV-U) disease. However, this comes at the cost of increased infectious toxicity, particularly with COVID-19, and thus has translated into a variable impact on progression-free survival (PFS) and, to-date, no overall survival (OS) benefit. Although there are promising Phase 2 data for triplets in patients with TP53 aberrant or relapsed disease, the heterogeneity of treatment duration/MRD definition, lack of control arm, and potential increased toxicity make it premature to use triplets in these groups. We recommend considering triplets in treatment naïve CLL patients with IGHV-U, TP53 wild type, anticipated low incidence/good tolerance of Gr ≥ 3 infection (<70 years old, no major comorbidity and fully immunized) who are well informed and prioritize maximal time off therapy at the expense of increased short-term logistical complexity. Future triplet research should focus on randomized trials in specific genomic subgroups, incorporating novel agents (e.g., non-covalent BTKI, BTK degrader, and next-generation BCL2 inhibitors) and new ways of adapting treatment duration to maximize efficacy and minimize toxicity.
    DOI:  https://doi.org/10.1002/hem3.70303
  9. Pharm Sci Adv. 2024 Dec;2 100052
    Novel targeted therapies in chronic myeloid leukemia.
    Muhammad Sameer Ashaq, Qian Zhou, Zhuoran Li, Baobing Zhao.
      Chronic myeloid leukemia (CML) is the chronic proliferation of myeloid-lineage cells in hematopoietic stem cells driven by the BCR-ABL1 fusion oncoprotein. The development of tyrosine kinase inhibitors (TKIs) has revolutionized CML treatment; however, resistance and intolerance to these drugs remain key challenges. CML stem cells (CMLSCs) are the root cause of CML relapse and resistance to TKIs. This review discusses novel targeted therapeutic options targeting CMLSCs to address the abovementioned challenges. Numerous novel TKIs, such as flumatinib, vodobatinib, and olverembatinib, have shown remarkable potential against BCR-ABL1, but few, including AT9283, MK0457, and DCC-2036, are still undergoing clinical trials. Targeting CMLSCs is a fundamental therapeutic approach for the treatment of CML progression, relapse, and TKI resistance. In this review, novel agents targeting core signaling pathways and novel molecular targets in CMLSCs are highlighted. Currently, multiple approaches, such as targeting epigenetic modifications or microRNAs and altering metabolism in leukemic cells, have shown desirable effects in treating CML. Immunotherapy, autophagy inhibitors, and protein synthesis inhibitors are novel and effective therapies for the treatment of CML. Although various therapeutic strategies have provided exceptional results in the treatment of CML, the challenges of TKI resistance and CML remission or relapse remain. Therefore, current therapeutic approaches and targeted therapies have practical and clinical implications for achieving desirable outcomes.
    Keywords:  BCR-ABL1; Chronic myeloid leukemia; Stem cells; Targeted therapy; Tyrosine kinase inhibitors
    DOI:  https://doi.org/10.1016/j.pscia.2024.100052
  10. Blood Adv. 2026 Jan 21. pii: bloodadvances.2025018945. [Epub ahead of print]
    Efficacy and Safety of Selinexor Combined with VRD in Newly Diagnosed Multiple Myeloma with EMD: A Phase 2 Trial.
    Yuanyuan Jin, Xin Cheng, Xuezhong Zhang, Qinglin Shi, Yu Zhu, Jianyong Li, Lei Fan, Lijuan Chen.
      Extramedullary disease (EMD) at diagnosis confers a poor prognosis in newly diagnosed multiple myeloma (NDMM). This multicenter, open-label, single-arm phase II investigator-initiated trial evaluated selinexor combined with bortezomib, lenalidomide, and dexamethasone (SVRD) in NDMM with EMD. Between October 17, 2022 and November 27, 2025, 30 patients were enrolled; 29 treated patients formed the modified intention-to-treat (mITT) and safety populations (median age 60 years). Induction comprised four 28-day SVRD cycles with protocol-specified consolidation/maintenance and optional ASCT. The primary endpoint was best overall response rate (ORR) during induction per IMWG; patients without a post-baseline assessment were imputed non-responders. In the mITT cohort, ORR was 89.7% (sCR 58.6%, CR 3.4%, VGPR 10.3%, PR 17.2%). Imaging documented EMD regression in 89.7% (complete resolution 79.3%, partial 10.3%); 12-month PFS and OS rates were 87.9% and 96.3%, respectively (medians not reached; median follow-up 18 months). High-risk cytogenetics were present in 31.0%, and 27.6% met ultra-high-risk ("double-hit") criteria. Grade ≥3 treatment-emergent adverse events occurred in 37.3% patients, most commonly thrombocytopenia (24.1%), neutropenia (6.9%), and pneumonia (10.3%); no treatment-related deaths occurred. SVRD produced deep hematologic responses and high EMD clearance with manageable toxicity, enabling ASCT in 51.7%. These findings support SVRD as a rational frontline option for EMD-positive NDMM and justify randomized studies to confirm durability and benchmark against contemporary quadruplets and cellular therapies. NCT# NCT05900882.
    DOI:  https://doi.org/10.1182/bloodadvances.2025018945
  11. Blood. 2026 Jan 20. pii: blood.2025031907. [Epub ahead of print]
    Time to Revise Myeloma Diagnostic Criteria? A Decade of Accumulated Evidence on Serum Free Light Chain Ratio ≥100.
    Rajshekhar Chakraborty, Ghulam Rehman Mohyuddin.
      In 2014, the International Myeloma Working Group (IMWG) expanded multiple myeloma diagnostic criteria to include serum free light chain (sFLC) ratio ≥100 as a standalone myeloma-defining biomarker based on studies suggesting approximately 80% risk of progression to overt myeloma at 2 years. However, subsequent studies demonstrate a substantially lower risk of progression, with a population-based registry data showing 2-year risk as low as 30.4% in this group. Importantly, subsequent data showed that over 70% of patients with sFLC ratio ≥100 have 24-hour monoclonal proteinuria <200 mg-a subgroup with particularly low progression risk (13.5% at 2 years) and minimal risk of irreversible renal failure. Furthermore, with the IMWG diagnostic amendment, sFLC ratio ≥100 is currently included within the composite endpoint of progression-free survival in early intervention clinical trials of high-risk smoldering multiple myeloma, which poses a risk of misclassifying biochemical changes as clinically meaningful events. We propose immediate revision of the diagnostic criteria to remove sFLC ratio ≥100 as standalone myeloma-defining event and exclusion of patients with sFLC ratio ≥100 from trials of newly diagnosed myeloma. These patients should be included in prospective studies on therapeutic interventions in high-risk smoldering myeloma as well as active surveillance with modern imaging to define their natural history in the contemporary era.
    DOI:  https://doi.org/10.1182/blood.2025031907
  12. Blood Neoplasia. 2026 Feb;3(1): 100177
    Extended long-term follow-up and the survival of Stop Imatinib study.
    François-Xavier Mahon, Stéphanie Dulucq, Delphine Réa, Franck-Emmanuel Nicolini, Françoise Rigal-Huguet, Katerina Machova Polakova, Viviane Dubruille, Marie-Pierre Noel, Jean-Christophe Ianotto, Bruno Villemagne, Émilie Cayssials, Sophie Park, Philippe Rousselot, Gabriel Etienne.
      The French Stop Imatinib study (STIM1) was one of the first trials to explore the possibility of discontinuing imatinib in patients with chronic myeloid leukemia (CML) who had achieved a sustained molecular response (at least a 4.5-log reduction). The stringent criteria for molecular recurrence (MRec) were defined as BCR::ABL1 transcript positivity confirmed by a second test showing either a 1-log increase or loss of major molecular response across consecutive assessments. This comprehensive update presents long-term follow-up data from the STIM1 study, with a median molecular follow-up of 12.8 years (range, 0.8-15). Results showed a molecular recurrence-free survival rate of 37% (95% confidence interval [CI], 28-48) at 120 months, and 35% (95% CI, 26-46) at 156 months after imatinib discontinuation. Importantly, no patients experienced CML progression during the follow-up. Overall survival rates were 97% (95% CI, 94-100) at 10 years and 88% (95% CI, 81-96) at 20 years. A case of late MRec, confirmed through DNA BCR::ABL1 breakpoint analysis and comparison at diagnosis and recurrence, indicated the persistence of the original disease rather than the onset of new CML. This study offers valuable insights into the safety and feasibility of imatinib discontinuation for patients with CML, supporting long-term remission while maintaining survival. This study was registered at ClinicalTrials.gov as #NCT00478985.
    DOI:  https://doi.org/10.1016/j.bneo.2025.100177
  13. Leukemia. 2026 Jan 22.
    Immunomodulatory effect of dasatinib plus blinatumomab versus ponatinib plus blinatumomab in newly diagnosed Ph+ acute lymphoblastic leukemia.
    Michela Ansuinelli, Nadia Peragine, Maria Stefania De Propris, Maria Cristina Puzzolo, Mariangela Di Trani, Loredana Elia, Cristina Skert, Roberto Cairoli, Simona Sica, Alessandro Rambaldi, Alessandra Tucci, Marco Cerrano, Daniele Vallisa, Valeria Cardinali, Antonino Mulè, Sabina Chiaretti, Anna Guarini, Robin Foà.
      In Ph+ acute lymphoblastic leukemia, frontline dasatinib plus blinatumomab (dasa+blina) is associated with long-term survival rates of 75-80%. The phase III GIMEMA ALL2820 trial has explored ponatinib with blinatumomab (pona+blina). In the present study, the immune modulation induced by dasa+blina and pona+blina was investigated. Immune cells were analyzed at the end of induction (T0) and after 2, 4 and 5 blinatumomab cycles (T2, T4, T5). Among 153 patients (43 dasa+blina, 110 pona+blina), the dasa+blina combination induced a significantly greater lymphocyte increase at T4 and T5 compared to pona+blina. The Treg counts decreased only in the dasa+blina treated patients. NK and NK-T cells increased significantly in the dasa+blina group, at all timepoints. Complete molecular responders (CMR) after dasatinib induction had significantly higher lymphocytes, T and NK cells compared to non-CMR patients. Bone marrow analyses showed higher activation (CD25, CD69) and lower exhaustion (PD1, TIM3) markers on NK and NK-T cells in dasa+blina treated patients. Dasa+blina patients exhibited a significantly enhanced NK cell capacity compared to ponatinib treated patients. Patients remaining on dasatinib maintained elevated NK cells with a more mature phenotype, suggesting a durable effect. These results highlight the greater dasa+blina immune activation, supporting a potential synergistic effect of the drug combination.
    DOI:  https://doi.org/10.1038/s41375-025-02855-5
  14. Blood. 2026 Jan 22. 147(4): 323-325
    Faulty antibody editing permits antiplatelet B cells in ITP.
    Jeffrey J Bednarski.
      
    DOI:  https://doi.org/10.1182/blood.2025031605
  15. Ann Hematol. 2026 Jan 20. 105(2): 40
    One-year consolidation with Ponatinib 15 mg in chronic myeloid leukaemia on deep molecular response with Imatinib.
    Lucía Pérez-Lamas, Mario Manzanares, Juan Carlos Hernández Boluda, Luis Felipe Casado Montero, María Teresa Gómez Casares, Rosa Ayala, Blanca Xicoy, Francisca Ferrer Marin, Guillermo Ortí, Raquel De Paz Arias, Santiago Osorio Prendes, Raul Perez Lopez, Elvira Mora, Concepción Ruiz Nuño, Antonio Jimenez Velasco, Concepción Boqué, Magdalena Sierra Pacho, Joaquin Martinez Lopez, Gonzalo Carreño-Tarragona, Mayte Coiras, Valentin Garcia-Gutierrez.
      Tyrosine kinase inhibitors (TKIs) discontinuation is the standard option for patients with chronic myeloid leukaemia (CML) in deep molecular response (MR) with imatinib. This study aimed to evaluate the efficacy and safety of one year consolidation with ponatinib on treatment-free remission (TFR) rate. This was a multicenter open-label, single-arm, phase II, exploratory clinical trial including patients with CML treated ≥4 years with imatinib therapy, and MR4.0 ≥12 months. Patients entered the TFR phase after receiving ponatinib at 15 mg/day for one year. Twenty three patients received ponatinib and 19 completed consolidation. Among the patients with detectable BCR::ABL1, 70% deepened response. The 48-weeks MR4.0 rate was 68.4% (95%CI: 43.4-87.4). The 48-week TFR rate as classically defined was 73.7% (95% CI: 8 56.3-96.4). Five restarted TKIs and all regained MR. The most frequent adverse events (AEs) were constipation (34.8%), asthenia (30.4%) and myalgia (21.7%). Patients who remained relapse-free one year after ponatinib discontinuation exhibited higher levels of NK and NKT-like cells with degranulation capacity. Consolidation with ponatinib showed a high TFR rate and adequate safety, granting further research.
    Keywords:  Chronic myeloid leukaemia; Consolidation treatment; Ponatinib; Treatment-Free remission
    DOI:  https://doi.org/10.1007/s00277-026-06806-7
  16. Blood. 2026 Jan 22. 147(4): 321-322
    Therapy by omission: observation as a strategy in JMML.
    Elliot Stieglitz.
      
    DOI:  https://doi.org/10.1182/blood.2025031279
  17. Leuk Lymphoma. 2026 Jan 21. 1-8
    Clinicopathological features and management of IgM multiple myeloma and Waldenstrom macroglobulinemia.
    Shayna Sarosiek, Jorge J Castillo, Zachary R Hunter, Andrew R Branagan, Steven P Treon.
      Waldenström macroglobulinemia (WM) is the most common malignancy associated with an IgM paraprotein, but in rare cases, a clonal IgM may be the result of IgM multiple myeloma (IgM-MM). Although there are some overlapping features associated with these two entities, there are specific characteristics that can help differentiate IgM-MM from WM. In each patient a thorough clinical, pathologic, and genomic evaluation is required to distinguish these conditions and allow for accurate diagnosis and appropriate treatment.
    Keywords:  IgM multiple myeloma; Waldenström macroglobulinemia; lymphoplasmacytic lymphoma; plasma cell disorder
    DOI:  https://doi.org/10.1080/10428194.2026.2616331
  18. Hematol Rep. 2026 Jan 09. pii: 10. [Epub ahead of print]18(1):
    Therapeutic Potential of Exportin 1 and Aurora Kinase A Inhibition in Multiple Myeloma Cells.
    Seiichi Okabe, Yuko Tanaka, Shunsuke Otsuki, Mitsuru Moriyama, Seiichiro Yoshizawa, Akihiko Gotoh, Daigo Akahane.
      Background/Objectives: Aurora kinases (AURKs) are key regulators of mitosis, and their dysregulation contributes to plasma cell disorders, including multiple myeloma (MM) and plasma cell leukemia (PCL). Methods: The expression and prognostic relevance of AURK family members were examined, and the therapeutic potential of AURKA inhibition was evaluated. Results: Gene expression analysis demonstrated significant upregulation of AURKA in PCL. Treatment of MM cells with the selective AURKA inhibitor LY3295668 induced dose-dependent cytotoxicity, caspase-3/7 activation, and cellular senescence. Similarly, selinexor, a selective exportin-1 inhibitor, elicited dose-dependent cytotoxicity and apoptosis. Combined treatment with LY3295668 and selinexor significantly improved apoptosis compared with either agent alone, and AURKA knockdown further sensitized MM cells to selinexor, thereby increasing apoptosis. In bortezomib-resistant MM cells and primary PCL samples, the combination therapy induced cytotoxicity and caspase-3/7 activation. Conclusions: These findings underscore AURKA expression as a prognostic marker in plasma cell disorders and support the therapeutic potential of combining AURKA inhibition with selinexor for bortezomib-resistant MM and PCL. To explore biomarker-driven strategies for optimizing therapeutic outcomes, future studies are warranted.
    Keywords:  XPO1 inhibitor; aurora kinase inhibitor; multiple myeloma; plasma cell leukemia
    DOI:  https://doi.org/10.3390/hematolrep18010010
  19. Nat Rev Clin Oncol. 2026 Jan 22.
    Diagnosis, risk stratification and management of smouldering multiple myeloma.
    Saurabh Zanwar, Shaji Kumar, S Vincent Rajkumar.
      New therapies have markedly improved survival outcomes for patients with multiple myeloma (MM). However, the onset of active disease, as defined by the 2014 International Myeloma Working Group SLiM-CRAB criteria, is often linked to substantial and irreversible morbidity. MM always develops from an asymptomatic precursor state called smouldering multiple myeloma (SMM). The clinical trajectory of SMM varies considerably; low-risk SMM often has an indolent course, similar to monoclonal gammopathy of undetermined significance, whereas nearly half of the subset of patients with high-risk SMM have progression to symptomatic MM within 2 years. Highly active treatments for MM, which remains an incurable disease, are being investigated for the management of SMM, with the aim of delaying or even preventing such progression. Both early therapeutic intervention and active surveillance are reasonable management options for patients with high-risk SMM, with decisions individualized through a detailed risk-benefit discussion with the patient. In this Review, we discuss current approaches for diagnostic evaluation, risk stratification and management of SMM, as well as future challenges and emerging opportunities in the field.
    DOI:  https://doi.org/10.1038/s41571-026-01119-0
  20. Haematologica. 2026 Jan 22.
    Menin and BCL2 inhibitors- shaken and stirred.
    Alex Bataller, Ghayas C Issa.
      Not available.
    DOI:  https://doi.org/10.3324/haematol.2025.300285
  21. Hematol Rep. 2025 Dec 31. pii: 5. [Epub ahead of print]18(1):
    Mediastinal Gray Zone Lymphomas: Diagnostic Challenges, Clinicopathologic Overlap, and Emerging Management Strategies.
    Tugba Zorlu, Mert Seyhan, Nigar Abdullayeva, Turgay Ulas, Mehmet Sinan Dal.
      Background: Mediastinal gray zone lymphoma (MGZL) is a rare B-cell lymphoma characterized by overlapping clinicopathologic and molecular features of primary mediastinal B-cell lymphoma (PMBL) and classical Hodgkin lymphoma (CHL). Under current WHO-HEMA5 and International Consensus Classification (ICC) frameworks, MGZL is restricted to EBV-negative lymphomas arising in the mediastinum. Methods: This review summarizes current evidence on epidemiology, clinical presentation, pathology, molecular characteristics, diagnostic challenges, and therapeutic approaches to MGZL, with data derived from retrospective series, limited prospective cohorts, and recent molecular studies. Results: MGZL predominantly affects young adults and commonly presents with bulky mediastinal disease. Diagnosis is challenging due to transitional morphology, pleomorphic Reed-Sternberg-like cells, and variable expression of B-cell and activation markers. Molecular studies demonstrate shared alterations with PMBL and CHL, including 9p24.1 (JAK2/PD-L1/PD-L2) gains, while additional reported features such as HOXA5 hypomethylation and MYC copy number gains support its biological distinctiveness, although evidence remains limited. Frontline treatment commonly involves intensive chemoimmunotherapy regimens such as DA-EPOCH-R; however, outcomes remain inferior to PMBL and CHL, with 5-year overall survival rates of approximately 40-60%. Relapsed or refractory disease frequently requires salvage chemotherapy and autologous stem cell transplantation. Immune-based therapies, including brentuximab vedotin and PD-1 inhibitors, have shown promising activity, particularly in combination. Conclusions: MGZL remains a diagnostically challenging and therapeutically complex lymphoma with inferior outcomes compared with related mediastinal lymphomas. Advances in molecular profiling and immunotherapy offer promising avenues toward more personalized treatment; however, prospective clinical trials and international collaboration are urgently needed to establish evidence-based management strategies for this rare entity.
    Keywords:  PD-1 inhibitors; brentuximab vedotin; immunophenotype; molecular features; prognosis; treatment
    DOI:  https://doi.org/10.3390/hematolrep18010005
  22. Cancer. 2026 Feb 01. 132(3): e70265
    Glucose-6-phosphate dehydrogenase deficiency is associated with improved survival in patients with acute myeloid leukemia treated with venetoclax and azacitidine.
    Shira Buchrits, Alon Rozental, Noa Korngold, Ofer Algor, Shirly Partouche, Galit Granot, Pia Raanani, Ofir Wolach.
       BACKGROUND: Glucose-6-phosphate dehydrogenase (G6PD) deficiency impairs cellular redox balance through reduced NADPH production and is the most common enzymatic disorder-causing anemia. Venetoclax combined with azacitidine (Ven-Aza) targets leukemic stem cells by disrupting oxidative phosphorylation and inducing mitochondrial stress. This study hypothesized that G6PD deficiency may enhance the efficacy of Ven-Aza in acute myeloid leukemia (AML) by reducing leukemic cell metabolic resilience.
    METHODS: The authors studied 73 consecutive patients with newly diagnosed (ND) AML treated with Ven-Aza. G6PD activity was systematically assessed at diagnosis in all patients and categorized as normal (n = 47), borderline (n = 11), or deficient (n = 15).
    RESULTS: Composite complete remission rates were 93% in the G6PD deficient group versus 69% in the normal/borderline group (p = .03). Patients with G6PD deficiency had a significantly longer median overall survival (23.8 months; 95% confidence interval [CI], 8.9-38.7), as compared to 8.96 months (95% CI, 2.9-15.0) in the normal/borderline group (p = .034). In multivariate analysis, G6PD-deficiency was associated with improved survival as compared to patients with normal G6PD activity (hazard ratio, 0.417; 95% CI, 0.181-0.965, p = .043). No significant differences were observed across groups in rates of febrile neutropenia, pneumonia, sepsis, or grade 3-4 cytopenia.
    CONCLUSION: G6PD deficiency is associated with higher response rates and improved survival in patients with ND-AML treated with Ven-Aza. These findings support G6PD deficiency as a potential biomarker of therapeutic sensitivity to Ven-AZA and may uncover metabolic vulnerabilities in AML with potential therapeutic implications.
    Keywords:  acute myeloid leukemia; azacitidine; biomarkers; glucose‐6‐phosphate dehydrogenase deficiency; survival analysis; venetoclax
    DOI:  https://doi.org/10.1002/cncr.70265
  23. Blood. 2026 Jan 22. 147(4): 471
    TP53-mutated AML with salmon-colored globules, a single Auer rod, pseudo-Chédiak-Higashi granules, and micronuclei.
    Zhaodong Xu, Nadia Medvedev.
      
    DOI:  https://doi.org/10.1182/blood.2025031282
  24. Hematol Oncol Clin North Am. 2026 Jan 17. pii: S0889-8588(25)00144-3. [Epub ahead of print]
    The Role of Stem Cell Transplantation in Hodgkin Lymphoma.
    Hanan Alharthy, Sairah Ahmed.
      Stem cell transplantation remains a cornerstone in managing relapsed/refractory classic Hodgkin lymphoma, though its role is evolving with the integration of targeted therapies. Autologous stem cell transplantation achieves cure rates of 50% to 60%, enhanced significantly with the introduction of novel agents including brentuximab vedotin and checkpoint inhibitor-based salvage and consolidation regimens. Allogeneic transplantation with reduced-intensity conditioning offers curative potential for patients with disease that relapses after autologous stem cell transplantation. This article reviews the evidence for autologous and allogeneic stem cell transplantation, their integration with novel agents, and the emerging transplant-sparing strategies.
    Keywords:  Allogeneic stem cell transplant; Autologous stem cell transplant; Brentuximab vedotin; Checkpoint inhibition; Hodgkin lymphoma; Novel therapy Hodgkin lymphoma; Stem cell transplantation
    DOI:  https://doi.org/10.1016/j.hoc.2025.12.003
  25. Br J Haematol. 2026 Jan 21.
    Bendamustine in combination with gemcitabine and vinorelbine as salvage regimen for relapsed or refractory peripheral T-cell lymphomas: A retrospective single-centre experience.
    Filippo Bagnoli, Jacopo Calabrese De Feo, Francesca Ricci, Francesco Corrado, Daniele Mannina, Daoud Rahal, Arturo Bonometti, Marcello Rodari, Laura Giordano, Stefania Bramanti, Carmelo Carlo-Stella, Armando Santoro.
      The prognosis of peripheral T-cell non-Hodgkin lymphomas (PTCL) is dismal, particularly in the relapsed/refractory (r/r) setting, where 3-year overall survival (OS) is 20%-30%. No superior second-line therapy for PTCL has been universally established, and durable remissions rely on consolidation with allogeneic haematopoietic stem cell transplantation (alloHSCT). Enhancing response rates to salvage therapy is, therefore, crucial to increase transplant eligibility. We retrospectively evaluated the efficacy of bendamustine, gemcitabine and vinorelbine combination (BeGeV) in 24 consecutive patients with r/r PTCL treated at our centre since 2017. BeGeV achieved an overall response rate (ORR) of 66% and a complete remission rate (CRR) of 41%. After a median follow-up of 41.8 months, 1-year progression-free survival (PFS) and OS were 37.5% and 58.3% respectively. Outcomes differed by histology: PTCL not otherwise specified (PTCL-NOS) showed inferior responses (ORR 41%, CRR 16%) compared with T-follicular helper lymphomas (PTCL-TFH; ORR 100%, CRR 75%) and systemic anaplastic large cell lymphoma (sALCL; ORR 75%, CRR 50%). Survival analyses confirmed substantial differences across subtypes, with 12-month PFS and OS rates of 8.3% and 41.7% for PTCL-NOS, 50% and 75% for sALCL and 75% and 75% for PTCL-TFH respectively. Despite the limitations of small sample size and retrospective design, this study provides preliminary evidence supporting BeGeV as a potential bridge to alloHSCT in r/r PTCL-TFH and sALCL.
    Keywords:  bendamustine; gemcitabine; peripheral T‐cell lymphoma
    DOI:  https://doi.org/10.1111/bjh.70292
  26. Cell Biochem Funct. 2026 Jan;44(1): e70174
    Bruton's Tyrosine Kinase: Pathophysiological Roles and Inhibitor-Based Therapeutic Advances.
    Simhadri Goud Gundrathi, Bharat Kumar Reddy Sanapalli, Shrestha Palit, Dilep Kumar Sigalapalli, Ashwini Deshpande, Vidyasrilekha Sanapalli.
      Bruton's tyrosine kinase (BTK) plays a pivotal role in intracellular signaling within B-cells, governing development, differentiation, and survival, and is an integral target in treating B-cell malignancies and autoimmune disorders. The impact on B-cell receptor, Toll-like receptor, and chemokine receptor pathways establishes its therapeutic interest. This review integrates existing studies on BTK functional roles in immunology and BTK inhibitors (BTKis) targeting. Literature was ascertained by searching prominent databases such as PubMed, Embase, Web of Science and Google scholar for BTK's molecular biology, the history of BTKis and their clinical significance. The review addresses mechanisms of resistance, particularly the C481S mutation, which impedes covalent inhibition but is abrogated by non-covalent BTKis like pirtobrutinib, including BTK's application in autoimmune and inflammatory disorders, and discusses the importance of further long-term safety and efficacy in chronic diseases. BTK inhibitors have proven to be an essential part of targeted therapy for B-cell cancer, and continuing advances are addressing challenges like drug resistance and side effects. However, major challenges like the emergence of novel resistance mutations, the need for accurate biomarkers to direct therapy, and the continuing challenge of controlling drug-associated toxicities and maintaining costs under control still pertain. Ongoing research is essential to fully realize the therapeutic potential of BTK inhibitors and integrate them into personalized regimens for cancer and immune diseases alike.
    Keywords:  BTK inhibitors; Bruton's tyrosine kinase; B‐cell receptor signaling; autoimmune diseases; targeted therapy
    DOI:  https://doi.org/10.1002/cbf.70174
  27. Haematologica. 2026 Jan 22.
    Optimal management of elderly/old Ph+ acute lymphoblastic leukemia patients.
    Robin Foà, Sabina Chiaretti, Felicetto Ferrara, Giovanni Pizzolo.
      Philadelphia-positive acute lymphoblastic leukemia (Ph+ ALL) is today a curable disease. In the real life, too many adult ALL patients are not adequately worked up at diagnosis and treated, and this occurs in particular in elderly/old individuals. We hereby discuss, through representative case descriptions, how Ph+ ALL patients diagnosed in their seventh, eight and nineth decade of life through a timely, accurate and personalized tyrosine kinase inhibitor (TKI) administration, in the absence of systemic chemotherapy, can experience long-lived responses, minimal residual disease negativity, and a good quality of life. To an extent that stopping TKI administration can also be considered. This perspective article represents a proof of concept that nowadays even in elderly/old Ph+ ALL the disease can be cured or kept under prolonged control if adequately managed.
    DOI:  https://doi.org/10.3324/haematol.2025.300060
  28. Br J Haematol. 2026 Jan 22.
    A comprehensive analysis of pirtobrutinib in Chinese patients with chronic lymphocytic leukaemia/small lymphocytic lymphoma (CLL/SLL): Results from the phase 3 study BRUIN CLL-321.
    Shuhua Yi, Jiang Cao, Ru Feng, Keshu Zhou, Lihua Qiu, Fei Li, Hai Yan Yang, Hui Zhou, Wuhan Hui, Jie Cui, He Huang, Jiankun Zhu, Xiuhui Ye, Jeff Sharman, Lugui Qiu.
      BRUIN CLL-321 is the first prospective, randomized study conducted in covalent BTK inhibitor (cBTKi) pretreated chronic lymphocytic leukaemia/small lymphocytic lymphoma (CLL/SLL) patients. In this heavily pretreated population, pirtobrutinib significantly improved progression-free survival (PFS) compared to investigator's choice (IC) of idelalisib/rituximab (IdelaR) or bendamustine/rituximab (BendaR). This report presents results from Chinese patients enrolled in BRUIN CLL-321, who were randomized 1:1 to pirtobrutinib (200 mg once daily) or IC of BendaR (idelalisib is not approved in China). End-points included independent review committee (IRC)-assessed PFS, investigator (INV)-assessed PFS, overall survival (OS), event-free survival (EFS), time to next treatment (TTNT) and safety. Among 40 Chinese patients (pirtobrutinib n = 19; BendaR n = 21), IRC-assessed PFS favoured pirtobrutinib (stratified hazard ratio [HR] = 0.281; 95% confidence interval [CI], 0.070-1.125, nominal p = 0.0554), with median PFS not reached versus 10.6 months with BendaR; INV-assessed PFS supported these findings. TTNT (HR = 0.150; 95% CI, 0.031-0.728) and EFS (HR = 0.322; 95% CI, 0.094-1.101) were also improved. A trend towards OS benefit was observed (HR = 0.343; 95% CI, 0.031-3.787). Pirtobrutinib showed a favourable safety profile, with fewer grade ≥3 treatment-emergent adverse events (36.8% vs. 93.3%) and serious adverse events (15.8% vs. 46.7%). These findings support pirtobrutinib as a clinically active and tolerable option for cBTKi-pretreated Chinese CLL/SLL population.
    Keywords:  CLL/SLL; China; cBTKi‐pretreated; pirtobrutinib
    DOI:  https://doi.org/10.1111/bjh.70334
  29. Ann Hematol. 2026 Jan 23. 105(2): 56
    Safety and efficacy of a pre-phase with dexamethasone followed by fractionated R-CHOP in diffuse large B-cell lymphoma patients with gastrointestinal involvement at diagnosis.
    Ke Cui, Jiangbo Wan, Zhichao Li, Jie Zhao, Yun Qin, Siguo Hao, Fang Huang.
      
    Keywords:  Acute gastrointestinal hemorrhage; Diffuse large B-cell lymphoma; Gastrointestinal involvement; Perforation; R-CHOP
    DOI:  https://doi.org/10.1007/s00277-026-06824-5
  30. BMC Cancer. 2026 Jan 21.
    Synergistic apoptosis induction in myelodysplastic syndrome cells by azacitidine and PIM-2 inhibitors via nuclear factor-kappa B pathway inhibition.
    Yixuan Guo, Zhaoyun Liu, Wenhui Lei, Xiaohan Liu, Chun Yang, Kai Ding, Rong Fu.
       BACKGROUND: We aimed to characterise the molecular effects of treating myelodysplastic syndrome (MDS) cells with the DNA methyltransferase inhibitor azacitidine and an PIM-2 inhibitor, focusing on their potential synergistic effects.
    METHODS: MDS cells were subjected to proliferation assays to assess the effects of each drug independently and in combination. The synergy of the drugs in promoting the apoptosis of MDS cells via NF-κB signalling pathway inhibition was evaluated.
    RESULTS: Our results suggested that azacitidine and the PIM-2 inhibitor have synergistic effects in inhibiting the proliferation and inducing the apoptosis of MDS cells. Furthermore, the combined application of azacitidine and PIM-2 inhibitor synergistically inhibited the NF-κB pathway, resulting in the induction of apoptosis in MDS cells.
    CONCLUSION: Administration of a small molecule PIM-2 inhibitor in combination with the epigenetic drug azacitidine is one of the effective ways to treat MDS. Our study lays a foundation for future clinical trials in patients with MDS.
    Keywords:  Apoptosis; Azacitidine; Myelodysplastic syndrome; NF-κB pathway; PIM-2 inhibitor
    DOI:  https://doi.org/10.1186/s12885-025-14657-0
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