bims-hemali Biomed News
on Hematologic malignancies
Issue of 2026–03–22
forty papers selected by
Alexandros Alexandropoulos, Γενικό Νοσοκομείο Αθηνών Λαϊκό
  1. T315I-mutated chronic myeloid leukemia with blast crisis relapse 10 years after allo-HSCT: A case report of second transplantation combined with olverembatinib maintenance therapy.
  2. Catch them ALL?
  3. Nanotube vesicles: a new neutrophil inflammatory response.
  4. [Efficacy and safety analysis of BTK inhibitors combined with R-CHOP regimen in newly diagnosed double-expressor diffuse large B-cell lymphoma].
  5. Venetoclax Retreatment in Chronic Lymphocytic Leukemia is biologically rational and clinically effective.
  6. Fixed-Duration Subcutaneous Mosunetuzumab in Relapsed/Refractory Follicular Lymphoma: Pivotal Phase 2 Primary Analysis.
  7. HOD08 for low-risk pediatric Hodgkin lymphoma.
  8. Timing is everything: the CAR T-cell clock is ticking.
  9. Polatuzumab Vedotin Combined With R-ICE (PolaR-ICE) as Second-Line Therapy in Diffuse Large B-Cell Lymphoma.
  10. Carfilzomib, lenalidomide, and dexamethasone compared with lenalidomide treatment after autologous haematopoietic stem-cell transplantation in patients with multiple myeloma (ATLAS): primary analysis of a randomised, open-label, phase 3 trial.
  11. FBXO3-mediated DUSP9 ubiquitination promotes leukemia stem cell maintenance and tyrosine kinase inhibitor resistance in chronic myeloid leukemia.
  12. Prognostic value of interim PET-CT in follicular lymphoma.
  13. Elranatamab in Relapsed/Refractory Multiple Myeloma: Mechanisms, Clinical Evidence, and Emerging Perspectives.
  14. [Clinical Study on the Transition of First-Line Bortezomib Intole- rance to Carfilzomib in the Treatment of Multiple Myeloma].
  15. Real-World Evidence for Pembrolizumab Gemcitabine Vinorelbine and Liposomal Doxorubicin in Classical Hodgkin Lymphoma.
  16. Genomic profiling enables personalized strategies to overcome drug resistance in multiple myeloma.
  17. Final Report of a Phase II Study of Ibrutinib and Venetoclax in Previously Untreated Waldenström Macroglobulinemia.
  18. A phase I/II study of gilteritinib in combination with chemotherapy in newly diagnosed patients with AML in Asia: final analysis.
  19. Teclistamab plus daratumumab significantly boosts survival for patients with early RRMM: The MajesTEC-3 trial is the first to test a combination of a bispecific antibody in the setting of first to third relapse after initial treatment for multiple myeloma.
  20. Everybody gets a CAR! But do they need it?
  21. Daratumumab plus bortezomib and dexamethasone (Dara-VD) in newly diagnosed Mayo 2004 stage IIIA and IIIB light-chain amyloidosis: Long-term follow-up results from a prospective phase 2 study.
  22. Live-cell Pick-Seq (LiP-Seq): Interrogating ultra-rare mantle cell lymphoma persistent cells after CART19 therapy.
  23. Clonal dynamics of CH in CLL.
  24. [Research Progress of Megakaryocyte Morphology in the Prognosis of Primary Myelofibrosis--Review].
  25. Brief Report: Multi-Institution Real-World Analysis Evaluating Safety, Efficacy, and ctDNA Dynamics After Tarlatamab in Patients With Previously Treated SCLC and LCNEC.
  26. Correction: VEXAS: A review of current understandings and emerging treatment strategies.
  27. Mediastinal grey zone lymphomas: Results of the expert pathological review analysis of a case series enrolled in the multicentre BIOGZL-2020 study in Italy.
  28. Zanubrutinib in AL Amyloidosis Associated With Waldenström Macroglobulinemia and Other B-Cell Non-Hodgkin Lymphoma.
  29. MRD in multiple myeloma: the clinical perspective.
  30. Imatinib and nilotinib are equally successful in achieving therapy-free remission.
  31. [Clinical characteristics, treatment, and prognosis of double-hit multiple myeloma with concurrent 1q21+ and t (4;14)].
  32. Immunodeficiency-associated primary CNS lymphomas: An International Primary CNS Lymphoma Collaborative Group (IPCG) Study.
  33. Introduction to a review series on the new wave of targeted therapeutics for MPNs.
  34. Zanubrutinib enhances CD19 CAR T killing of B-cell lymphoma by inhibiting BTK phosphorylation, regulating PI3K/AKT/mTOR pathway, and promoting autophagy.
  35. Ph-Negative Acute Lymphoblastic Leukemia in the Older Adults: Biology, Therapeutic Strategies and Unmet Needs.
  36. VS-4718 enhances apoptosis induced by low-dose carfilzomib and overcomes carfilzomib resistance in PSMB5-mutated proteasome inhibitor resistant multiple myeloma.
  37. The Role of Microenvironment in Bispecific Antibodies Treatment in Multiple Myeloma.
  38. Restless legs syndrome in chronic myeloid leukemia: an overlooked condition with a significant impact on health-related quality of life.
  39. Phase 1b study of ABBV-744, a novel, selective BET inhibitor, as monotherapy in patients with myelofibrosis.
  40. [Research Progress in ALK+/- Anaplastic Large Cell Lymphoma--Review].
  1. Transpl Immunol. 2026 Mar 18. pii: S0966-3274(26)00039-0. [Epub ahead of print] 102381
    T315I-mutated chronic myeloid leukemia with blast crisis relapse 10 years after allo-HSCT: A case report of second transplantation combined with olverembatinib maintenance therapy.
    YuTing Zhu, JiaJuan Ji, Dan Luo, PeiWen Ding, YanQiu Zhao, Jie Liu, Dan Guo, ShengJin Fan.
      Chronic myeloid leukemia (CML) is a myeloproliferative neoplasm characterized by the presence of the Philadelphia chromosome and the resulting fusion proteins with abnormal tyrosine kinase activity. The treatment of CML includes allogeneic hematopoietic stem cell transplantation (allo-HSCT) and TKI drug therapy. The BCR::ABL1 T315I mutation in CML leads to resistance to first- and second-generation tyrosine kinase inhibitors (TKIs), but is sensitive to two third-generation TKIs, olverembatinib and ponatinib. Olverembatinib, an oral third-generation BCR::ABL1 TKI, has preclinical activity against T315I-mutated CML. Here, we present a case of a CML patient with the T315I mutation who experienced late relapse with blast crisis 10 years after allo-HSCT. Following hematologic recovery and achievement of major molecular response (MMR) through induction therapy, the patient underwent a second allo-HSCT from his haploidentical sister. After successful engraftment, the patient received regular consolidation maintenance therapy with olverembatinib.
    Keywords:  Allogeneic hematopoietic stem cell transplantation; Chronic myeloid leukemia; Late relapse; Olverembatinib; T315I
    DOI:  https://doi.org/10.1016/j.trim.2026.102381
  2. Blood. 2026 Mar 19. 147(12): 1253-1254
    Catch them ALL?
    Martin Schrappe.
      
    DOI:  https://doi.org/10.1182/blood.2025032168
  3. Blood. 2026 Mar 19. 147(12): 1249-1250
    Nanotube vesicles: a new neutrophil inflammatory response.
    Peter F Zipfel.
      
    DOI:  https://doi.org/10.1182/blood.2025032406
  4. Zhonghua Xue Ye Xue Za Zhi. 2026 Feb 14. 47(2): 139-145
    [Efficacy and safety analysis of BTK inhibitors combined with R-CHOP regimen in newly diagnosed double-expressor diffuse large B-cell lymphoma].
    J B Lu, L Cao, H L Liu, Y Miao, H R Shen, Y Xia, H Yin, Y X Cheng, J Y Li, L Fan.
      Objective: To evaluate the efficacy and safety of Bruton tyrosine kinase inhibitor (BTKi) combined with R-CHOP regimen in newly diagnosed double-expressor diffuse large B-cell lymphoma (DE-DLBCL) . Methods: A retrospective analysis was conducted on 95 patients with DLBCL meeting DE criteria by immunohistochemistry (MYC protein expression ≥ 40% , BCL-2 protein expression ≥ 50% ) treated at the First Affiliated Hospital of Nanjing Medical University between June 2021 and June 2024. Among them, 35 patients received BTKi (zanubrutinib, orelabrutinib, acalabrutinib) combined with R-CHOP (BTKi + R-CHOP group) , and 60 received R-CHOP regimen alone (R-CHOP group) . Outcomes included objective response rate (ORR) , complete response (CR) rate, progression-free survival (PFS) , overall survival (OS) , and safety. Results: The median age of the BTKi+R-CHOP group was 61 (range, 29-73) years. At the end of induction therapy, the BTKi+R-CHOP group had a higher ORR (94.3% vs 71.7% , P=0.008) and CR rate (91.4% vs 65.0% , P=0.006) than the R-CHOP group. After a median follow-up of 30 (range, 6-47) months, the 1- and 2-year PFS rates in the BTKi+R-CHOP group were 88.5% (95% CI: 78.5% -99.8% ) and 85.1% (95% CI: 73.8% -98.1% ) , respectively, and the 1- and 2-year OS rate was 94.3% (95% CI: 86.9% -100% ) . In the R-CHOP group, the 1-year and 2-year progression-free survival (PFS) rates were 61.7% (95% CI: 50.5% -75.3% ) and 48.8% (95% CI: 37.4% -63.6% ) , respectively; the 1-year and 2-year overall survival (OS) rates were 80.0% (95% CI: 70.5% -90.8% ) and 65.1% (95% CI: 53.7% -78.8% ) , respectively. Between-group differences were significant for both PFS (P=0.002) and OS (P=0.010) . Subgroup analyses showed high ORRs across clinical subgroups in the BTKi+R-CHOP group (all ORR>85% ) . Grade ≥ 3 adverse events primarily included neutropenia (28.6% ) and pulmonary infection (14.3% ) ; no fatal bleeding or cardiovascular events occurred. Conclusion: BTKi combined with R-CHOP significantly improved response rates and survival in patients with DE-DLBCL, with manageable safety.
    Keywords:  Bruton tyrosine kinase inhibitor; Efficacy; Lymphoma, large B-cell, diffuse; R-CHOP; Safety
    DOI:  https://doi.org/10.3760/cma.j.cn121090-20250811-00375
  5. Blood Adv. 2026 Mar 17. pii: bloodadvances.2026019871. [Epub ahead of print]
    Venetoclax Retreatment in Chronic Lymphocytic Leukemia is biologically rational and clinically effective.
    Mathias Castonguay, Mary Ann Anderson, Philip A Thompson, John F Seymour.
      Venetoclax therapy has evolved from continuous monotherapy to fixed-duration (FD) and measurable residual disease (MRD)-guided combination regimens in frontline and relapsed/refractory chronic lymphocytic leukemia (CLL). Compared with continuous therapy, FD regimens are associated with a lower incidence of emergence of BCL2 mutations and distinct mechanisms of relapse, supporting the rationale for investigating venetoclax-based combination retreatment strategies. In this review, we summarize the key studies for venetoclax rechallenge and discuss the available clinical evidence. To date, ten abstracts or published manuscripts have reported on venetoclax retreatment, as continuous monotherapy or with FD/MRD guided combinations with anti-CD20 monoclonal antibodies (rituximab, obinutuzumab) or covalent Bruton tyrosine kinase inhibitors (ibrutinib, acalabrutinib). Patient and disease characteristics were heterogeneous across studies, with a substantial proportion of patients with high-risk disease (IGHV-unmutated or del17p/TP53 mutations). The median time off venetoclax following initial therapy ranged from 9 to 90 months. Reported overall response rates to retreatment ranged from 72% to 100%, and undetectable MRD rates in peripheral blood from 32% to 92%. Median progression-free survival, when available, ranged from 23 to 58 months. Optimal patient selection remains to be defined, but the depth of the initial venetoclax response and time to progression from last venetoclax exposure may predict rechallenge efficacy and are incorporated in new clinical trial criteria allowing previous FD venetoclax treatment.
    DOI:  https://doi.org/10.1182/bloodadvances.2026019871
  6. Am J Hematol. 2026 Mar 20.
    Fixed-Duration Subcutaneous Mosunetuzumab in Relapsed/Refractory Follicular Lymphoma: Pivotal Phase 2 Primary Analysis.
    Nancy L Bartlett, Laurie H Sehn, Sarit Assouline, Pratyush Giri, John Kuruvilla, Stephen J Schuster, Sung-Soo Yoon, Keith Fay, Georg Hess, Martin Dreyling, Norma C Gutierrez, Eva Cybulski, Fidelis Sabalvaro, Elicia Penuel, Vanda Teodoro, Samuel Tracy, Denison Kuruvilla, Joseph Chen, Volker Wiebking, Michael C Wei, L Elizabeth Budde.
      Mosunetuzumab is approved as an intravenous (IV) formulation for relapsed/refractory (R/R) follicular lymphoma (FL) after ≥ 2 prior therapies. A subcutaneous (SC) formulation, aiming to improve patient safety and convenience, has been developed. We report the primary analysis of pharmacokinetics (PK), efficacy, and safety of mosunetuzumab SC (N = 94; median follow-up: 26.1 months) at the recommended Phase 2 dose (Cycle [C]1 Day [D]1: 5 mg; C1D8 and D15, and C2D1 onwards: 45 mg) in patients with R/R FL after ≥ 2 prior therapies, alongside data from a within-study comparator cohort of mosunetuzumab IV in a similar patient population (N = 90; median follow-up: 22.5 months). The co-primary PK endpoints (Ctrough and AUC) were met, demonstrating non-inferior exposure of mosunetuzumab SC versus IV (observed Ctrough[C3]: geometric mean ratio [GMR] 1.39 [90% confidence interval (CI): 1.20-1.61]; AUC0-84: GMR 1.06 [90% CI: 0.92-1.21]). Mosunetuzumab SC efficacy was consistent with IV: overall response rate, 76.6% (95% CI: 66.7-84.7); complete response rate, 61.7% (95% CI: 51.1-71.5); median duration of complete response, 34.6 months (95% CI: 20.7-not evaluable [NE]); and median progression-free survival, 23.7 months (95% CI: 14.6-NE). Mosunetuzumab SC demonstrated a favorable safety profile versus mosunetuzumab IV with a numerically lower rate (29.8% vs. 44.4%) and severity (grade ≥ 2: 9.6% vs. 18.9%) of cytokine release syndrome (CRS) events. Mosunetuzumab SC combines the benefits of short administration time, fixed-duration treatment, outpatient accessibility, and low CRS rate, offering clinically meaningful improvements in patient convenience and safety. Trial Registration: www.clinicaltrials.gov: NCT02500407.
    Keywords:  bispecific antibody; follicular lymphoma; subcutaneous mosunetuzumab
    DOI:  https://doi.org/10.1002/ajh.70225
  7. Blood. 2026 Mar 19. 147(12): 1381
    HOD08 for low-risk pediatric Hodgkin lymphoma.
      
    DOI:  https://doi.org/10.1182/blood.2026033607
  8. Blood. 2026 Mar 19. 147(12): 1246-1247
    Timing is everything: the CAR T-cell clock is ticking.
    Gloria Iacoboni.
      
    DOI:  https://doi.org/10.1182/blood.2025032675
  9. Am J Hematol. 2026 Mar 17.
    Polatuzumab Vedotin Combined With R-ICE (PolaR-ICE) as Second-Line Therapy in Diffuse Large B-Cell Lymphoma.
    Geoffrey Shouse, Matthew Matasar, Lu Chen, Jennifer Crombie, Jonathon Cohen, Ranjana Advani, Ann LaCasce, Leslie Popplewell, Sandrine Puverel, Lacolle Peters, Shari Daniels, James Godfrey, Matthew Mei, Swetha Thiruvengadam, Lihua E Budde, Liana Nikolaenko, Steven T Rosen, Larry W Kwak, Stephen J Forman, Alex F Herrera.
      Salvage chemoimmunotherapy followed by autologous stem cell transplantation (ASCT) remains a standard therapy for relapsed/refractory (r/r) diffuse large B-cell lymphoma (DLBCL) who relapse > 1 year after frontline treatment. We evaluated the safety and efficacy of polatuzumab vedotin (Pola) combined with R-ICE salvage chemotherapy, followed by post-ASCT Pola maintenance, aiming to improve complete response (CR) rates and enhance post-ASCT outcomes in r/r DLBCL. Notably, the study's accrual period predated the approvals of second-line CAR T cell therapies. Forty-one patients were enrolled and received PolaR-ICE. Adverse effects of the combination were consistent with those observed with Pola and R-ICE chemotherapy with no new toxicity signals observed and were most commonly hematologic and gastrointestinal. The overall response rate after salvage was 88% with a CR rate of 56%. Twenty-two patients (56%) went on to receive autologous stem cell transplant and 16 (39%) received Pola consolidation. At a median follow-up of 25 months (range: 18-21), the 2-year PFS of all patients treated with PolaR-ICE (n = 41) was 49.9% (95% CI: 31.7-65.7) and 2-year OS was 75.0% (95% CI: 58.5-85.8). Patients with relapse ≤ 12 months of initial therapy achieved a 2-year PFS of 36.4% (90% CI: 17.1-56.0) versus 80.0% (95% CI: 40.9-94.6) among patients with relapse ≥ 12 months. Our findings demonstrate that Pola-RICE is a safe and effective salvage regimen for r/r DLBCL, which can be considered for patients with late relapse or in areas where CAR T access may be limited. Trial Registration: ClinicalTrials.gov identifier: NCT04665765.
    Keywords:  DLBCL; autologous stem cell transplant; polatuzumab vedotin; relapsed/refractory
    DOI:  https://doi.org/10.1002/ajh.70282
  10. Lancet Haematol. 2026 Mar 11. pii: S2352-3026(26)00011-6. [Epub ahead of print]
    Carfilzomib, lenalidomide, and dexamethasone compared with lenalidomide treatment after autologous haematopoietic stem-cell transplantation in patients with multiple myeloma (ATLAS): primary analysis of a randomised, open-label, phase 3 trial.
    Dominik Dytfeld, Tomasz Wróbel, Krzysztof Jamroziak, Tadeusz Kubicki, Paweł Robak, Anna Puła, Adam Walter-Croneck, Jarosław Czyż, Agata Tyczyńska, Agnieszka Druzd-Sitek, Krzysztof Giannopoulos, Adam Nowicki, Tomasz Szczepaniak, Anna Łojko-Dankowska, Magdalena Matuszak, Lidia Gil, Bartosz Puła, Justyna Rybka, Maciej Majcherek, Lidia Usnarska-Zubkiewicz, Łukasz Szukalski, Agnieszka Końska, Jan Maciej Zaucha, Jan Walewski, Damian Mikulski, Olga Czabak, Tadeusz Robak, Oscar B Lahoud, Jeffrey A Zonder, Jennifer H Cooperrider, Benjamin A Derman, Theodore Karrison, Andrzej J Jakubowiak.
       BACKGROUND: Lenalidomide maintenance has long been a preferred treatment after autologous haematopoietic stem-cell transplantation (HSCT) in patients with multiple myeloma. Multidrug treatments are emerging as an alternative to lenalidomide alone. We aimed to compare carfilzomib-lenalidomide-dexamethasone with lenalidomide alone in patients with multiple myeloma after autologous HSCT.
    METHODS: ATLAS was an investigator-initiated, multicentre, open-label, phase 3, randomised, superiority trial conducted at 12 academic and clinical centres in the USA and Poland. Patients aged 18 years or older with newly diagnosed multiple myeloma with at least stable disease after autologous HSCT and an Eastern Cooperative Oncology Group performance status of 0 or 1 were randomly assigned (1:1) using permuted blocks of sizes four and six and a web-based system to receive carfilzomib-lenalidomide-dexamethasone (28-day cycles of carfilzomib 20 mg/m2 administered intravenously in cycle 1 on days 1 and 2 then 36 mg/m2 on days 1, 2, 8, 9, 15, and 16 in cycles 1-4 and 36 mg/m2 on days 1, 2, 15, and 16 from cycle 5 to 36; lenalidomide 25 mg administered orally on days 1-21; and dexamethasone 20 mg administered orally on days 1, 8, 15, and 22) or lenalidomide (10 mg administered orally for the first three cycles and then at the best tolerated dose [≤15 mg for 28 days in 28-day cycles]). Randomisation was stratified by response to previous treatment at trial entry (less than very good partial response vs very good partial response or better), cytogenetic risk factors (presence vs absence of any of del[13], t[4;14][p16;q32], t[14;16][q32;q23], del[17][p13.1], or hypodiploidy), and site location (USA vs Poland). Patients in the carfilzomib-lenalidomide-dexamethasone group with standard cytogenetic risk were switched to lenalidomide maintenance after cycle 8 if no measurable residual disease (MRD) was detected after cycle 6. The primary endpoint was progression-free survival in all randomly assigned patients. The safety analysis population included all randomly assigned patients who received at least one dose of the assigned treatment. This study was registered with ClinicalTrials.gov (NCT02659293) and EudraCT (2015-002380-42) and is completed.
    FINDINGS: Between June 10, 2016, and Oct 21, 2020, 196 patients consented and were screened for eligibility, 180 of whom were enrolled and randomly assigned to carfilzomib-lenalidomide-dexamethasone (n=92) or lenalidomide (n=88). 85 (47%) patients were female and 95 (53%) were male; 167 (93%) were White. At a median follow-up of 69 months (IQR 57-77), 4-year progression-free survival was 67·5% (95% CI 56·2-76·4) in the carfilzomib-lenalidomide-dexamethasone group and 38·0% (27·6-48·2) in the lenalidomide group (p<0·0001; median progression-free survival 72·8 months [58·4-not estimable] vs 37·3 months [30·6-44·7]; hazard ratio 0·46 [95% CI 0·30-0·70]; log-rank p=0·0002). The most common grade 3-4 adverse events were neutropenia (44 [48%] of 91 patients in the carfilzomib-lenalidomide-dexamethasone group vs 51 [59%] of 87 in the lenalidomide group) and thrombocytopenia (12 [13%] vs five [6%]). Serious adverse events occurred in 27 (30%) patients in the carfilzomib-lenalidomide-dexamethasone group and 20 (23%) in the lenalidomide group. Two deaths in the carfilzomib-lenalidomide-dexamethasone group due to lung infections and two deaths in the lenalidomide group due to COVID-19 and heart failure were considered possibly related to treatment by the investigators.
    INTERPRETATION: The enhanced efficacy of carfilzomib-lenalidomide-dexamethasone treatment following autologous HSCT in patients with newly diagnosed multiple myeloma, assessed within a framework of de-escalation based on MRD status and individual risk, supports strategies for maintenance therapy intensification in this setting.
    FUNDING: Amgen and Celgene (Bristol Myers Squibb).
    DOI:  https://doi.org/10.1016/S2352-3026(26)00011-6
  11. Cell Rep Med. 2026 Mar 17. pii: S2666-3791(26)00103-5. [Epub ahead of print]7(3): 102686
    FBXO3-mediated DUSP9 ubiquitination promotes leukemia stem cell maintenance and tyrosine kinase inhibitor resistance in chronic myeloid leukemia.
    Xudong Li, Shiyu Zuo, Yanli Zhang, Zexing Liu, Na Shen, Qingqing Ma, Mingxia Sun, Binglei Zhang, Mengjia Li, Hong Huang, Mengya Gao, Zhenghua Huang, Huifang Zhao, Yilin Chen, Fengcai Gao, Wenjuan Fan, Zhen Zhang, Yuhan Hu, Yu An, Siyue Li, Miao Liu, Yupeng Liu, Yuxuan Liu, Chaoge Li, Yiguo Zhang, Yingmei Li, Weijie Cao, Fang Wang, Yongping Song, Linping Xu, Zhilei Bian, Wei Li.
      Eradicating leukemia stem cells (LSCs) and overcoming tyrosine kinase inhibitor (TKI) resistance is urgent for chronic myeloid leukemia (CML) treatment. We find that F-box protein 3 (FBXO3) is highly upregulated in CD34+ CML stem cells from TKI-resistant patients and identify it as an innovative CML-LSC marker via single-cell RNA sequencing (scRNA-seq). FBXO3 deficiency induces apoptosis and reduces proliferation of CML cell lines and LSCs in vitro and in vivo, with minimal effects on normal CD34+ hematopoietic stem cells (HSCs). Mechanistically, FBXO3 interacts with DUSP9 to promote its ubiquitination and activate the MAPK pathway, critical for CML cell activity. DUSP9 knockdown partially reverses FBXO3-deficiency-mediated LSC elimination. Furthermore, FBXO3 inhibitor monotherapy or combination with imatinib effectively eradicates CML-LSCs, overcomes TKI resistance, and spares normal hematopoiesis. Collectively, our findings highlight FBXO3's role in CML progression and support combining FBXO3 inhibitors with TKIs for durable LSC elimination.
    Keywords:  CML-LSCs; DUSP9; FBXO3; TKI resistance; chronic myeloid leukemia
    DOI:  https://doi.org/10.1016/j.xcrm.2026.102686
  12. Med Clin (Barc). 2026 Mar 18. pii: S0025-7753(26)00061-8. [Epub ahead of print]166(5): 107411
    Prognostic value of interim PET-CT in follicular lymphoma.
    Sunil Lakhwani, Marta Díaz-López, Dolores Cabello-García, Carolina De Bonis-Braun, María José Rodríguez-Salazar, Belén Pérez-Pinilla, Alejandro Martín-Martín, Miguel T Hernández.
       BACKGROUND: Interim positron emission tomography-computed tomography (iPET) has shown prognostic value in high-avidity lymphomas, like diffuse large B-cell lymphoma and Hodgkin lymphoma. However, its role in follicular lymphoma (FL) remains unclear.
    METHODS: We conducted a retrospective observational study including patients with grades 1-3a FL treated with frontline chemoimmunotherapy between 2012 and 2014 at our institution, who underwent iPET after the fourth treatment cycle. All PET-CT were re-evaluated to assign Deauville 5-point scale (D5PS) and we considered complete metabolic response (CMR) when D5PS was 1-3. Primary endpoints were progression-free survival (PFS) and overall survival (OS).
    RESULTS: Of the 38 patients included, 63.2% (24/38) achieved CMR on iPET. All the patients who were in CMR on iPET, were also in CMR at the end of treatment PET-CT. However, among the 14 patients without CMR on iPET, only 4 patients achieved CMR at end of treatment PET-CT and 5 patients had progressive disease. After a median follow-up of 87.6 months (range 11.0-129.8), achieving CMR was associated with longer PFS (p<0.001; HR 0.08; 95% CI 0.03-0.24) and longer OS (p=0.012; HR 0.24; 95% CI 0.07-0.80).
    CONCLUSIONS: In this single-center study with long follow-up, iPET evaluated by D5PS predicted PFS and OS in FL.
    Keywords:  Deauville score; Follicular lymphoma; Interim PET-CT; Linfoma folicular; PET-TC intermedio; Prognosis; Pronóstico
    DOI:  https://doi.org/10.1016/j.medcli.2026.107411
  13. Eur J Haematol. 2026 Mar 18.
    Elranatamab in Relapsed/Refractory Multiple Myeloma: Mechanisms, Clinical Evidence, and Emerging Perspectives.
    Maria Eugenia Alvaro, Enrica Antonia Martino, Santino Caserta, Mamdouh Skafi, Antonella Bruzzese, Nicola Amodio, Eugenio Lucia, Virginia Olivito, Caterina Labanca, Francesco Mendicino, Ernesto Vigna, Fortunato Morabito, Massimo Gentile.
      Relapsed and refractory multiple myeloma (RRMM) remains associated with poor outcomes, particularly in patients exposed or refractory to proteasome inhibitors, immunomodulatory agents, and anti-CD38 monoclonal antibodies. Targeting B-cell maturation antigen (BCMA) has emerged as an effective therapeutic strategy, prompting the development of bispecific antibodies that redirect T-cell cytotoxicity toward malignant plasma cells. Elranatamab is a humanized BCMA × CD3 bispecific antibody that has demonstrated clinically meaningful activity in heavily pretreated RRMM. This review summarizes and critically appraises available evidence on elranatamab, focusing on its mechanism of action, clinical efficacy, safety profile, patient-reported outcomes, and comparative positioning within the evolving BCMA-directed treatment landscape. Across studies, elranatamab has shown high response rates, durable disease control, and manageable toxicity, with predominantly low-grade cytokine release syndrome and limited neurotoxicity when administered with step-up dosing. Emerging data indicate preserved efficacy in patients previously exposed to BCMA-targeted therapies and feasibility in selected high-risk populations, including those with severe renal impairment. Nevertheless, uncertainties remain regarding optimal sequencing, long-term survival benefit, infection risk management, and mechanisms of resistance. Overall, elranatamab represents a valuable addition to the therapeutic armamentarium for RRMM. Ongoing studies and real-world experience will be critical to refine its positioning, identify patients most likely to benefit, and define its role in combination strategies.
    Keywords:  BCMA; Elranatamab; bispecific antibodies; immunotherapy; multiple myeloma; relapsed refractory disease
    DOI:  https://doi.org/10.1111/ejh.70167
  14. Zhongguo Shi Yan Xue Ye Xue Za Zhi. 2026 Feb;34(1): 115-121
    [Clinical Study on the Transition of First-Line Bortezomib Intole- rance to Carfilzomib in the Treatment of Multiple Myeloma].
    Ying Yao, Xiao-Lan Shi, Pan-Feng Wang, Yun Xu, Shuang Yan, Jia-Jia Meng, Yu-Xin Jiang, Peng Wang, Jing Wang, Xiao Ma, Cheng-Cheng Fu, De-Pei Wu, Ling-Zhi Yan.
       OBJECTIVE: To evaluate the feasibility of in-class transition(iCT) first-line bortezomib intolerance to carfilzomib in the treatment of patients with multiple myeloma(MM).
    METHODS: It was retrospectively collected that the clinical data of MM patients who transitioned to carfilzomib due to intolerance, such as ≥grade 1 painful peripheral neuropathy (PN), during the treatment with first-line bortezomib-based triple regimens in the First Affiliated Hospital of Soochow University and Soochow Hopes Hematology Hospital from March 2023 to January 2025, and their safety and efficacy were analyzed.
    RESULTS: A total of 23 MM patients were included. The cohort had a median age of 63 (46-75) years. The median treatment cycle of bortezomib before iCT was 4 (1-6). Among the causes of intolerance, there were 22 cases of PN and 1 case of diarrhea. With a median follow-up of 10(2-23) months, at 1 month, 2 months and 4 months, 1/22, 3/22, and 12/20 of patients reduced by one grade in PN after transition. At 4 months after transition, all patients' peripheral neuropathic pain symptoms had disappeared. After 2 months of transition, there was a significant decrease in overall neuropathy limitations scale (ONLS) and total neuropathy score (TNS) scores compared to baseline (P <0.001). After carfilzomib treatment, the decrease in grade≥3 neutropenia from 21.7% to 17.4%(P=0.021).The additional non-hematological toxicity was transient, with grade 1-2 hypertension(47.8%) and QTcF prolongation(13.0%). In terms of efficacy analysis, the conversion rate of ≥CR increased from 30.4% to 69.5% (P=0.047), and the sCR rate and mininal residual disease (MRD) negative conversion rate both increased from 30.4% to 65.2% (P=0.026).
    CONCLUSION: The transition of first-line bortezomib intolerance to carfilzomib can significantly improve symptoms such as PN and deepen remission.
    Keywords:  multiple myeloma; bortezomib; carfilzomib; peripheral meuropathy; in-class transition(iCT)
    DOI:  https://doi.org/10.19746/j.cnki.issn.1009-2137.2026.01.016
  15. Blood Adv. 2026 Mar 19. pii: bloodadvances.2025018267. [Epub ahead of print]
    Real-World Evidence for Pembrolizumab Gemcitabine Vinorelbine and Liposomal Doxorubicin in Classical Hodgkin Lymphoma.
    Grace Baek, Gaurav Varma, Samuel Yamshon, Herman J van Besien, Nancy L Bartlett, Marcus P Watkins, Harsh R Shah, Kelsey Baron, Reid W Merryman, Ayo Samuel Falade, Jakub Svoboda, Sara Prischak, Christopher R D'Angelo, Joe D Lukowski, Ranjana H Advani, Austin H Yeung, Maya C Rosenberg, Jenna M Voutsinas, Mengyang Di, Ryan C Lynch, Christina Poh, Vikram Raghunathan, Mazyar Shadman, Stephen D Smith, Brian G Till, Chaitra S Ujjani, Catherine Diefenbach, Ajay K Gopal.
      
    DOI:  https://doi.org/10.1182/bloodadvances.2025018267
  16. Discov Oncol. 2026 Mar 14.
    Genomic profiling enables personalized strategies to overcome drug resistance in multiple myeloma.
    Fengbo Zeng, Azin Taki.
      
    Keywords:  Genomic profiling; Immunomodulatory drug; Multiple myeloma; Plasma cell
    DOI:  https://doi.org/10.1007/s12672-026-04812-9
  17. Am J Hematol. 2026 Mar 15.
    Final Report of a Phase II Study of Ibrutinib and Venetoclax in Previously Untreated Waldenström Macroglobulinemia.
    Jorge J Castillo, Andrew R Branagan, Alberto Guijosa, Gottfried von Keudell, Andres Ramirez-Gamero, Hannah Chory, Margaret Kobs, Nina Budano, Julia Nguyen, Alexandra Eurell, Courtney Boyajian, Kirsten Meid, Maria Luisa Guerrera, Amanda Kofides, Shirong Liu, Xia Liu, Nicholas Tsakmaklis, Zachary R Hunter, Christopher J Patterson, Steven P Treon, Shayna Sarosiek.
      The BTK inhibitor ibrutinib and the BCL-2 antagonist venetoclax are active therapies as single agents in Waldenström macroglobulinemia (WM). In this phase 2 study, we sought to investigate the combination of ibrutinib and venetoclax as a 2-year fixed-duration, oral-based, chemotherapy-free regimen in symptomatic, treatment-naive WM patients. All patients had MYD88 mutations, 17 (38%) had CXCR4 mutations, and 4 (9%) had TP53 alterations. Following enrollment of 45 patients, treatment and enrollment were stopped due to the occurrence of ventricular arrhythmias in 4 (9%), which included two grade 5 events. The median treatment time was 10 cycles, each lasting 28 days. Follow-up continued after protocol treatment was terminated. The very good partial response/complete response (VGPR/CR) rate was 42%, and it was lower in patients with CXCR4 (29% vs. 50%) or TP53 (25% vs. 44%) mutations. With a median follow-up of 49 months, the median progression-free survival (PFS) was 36 months (range 28-42). The median treatment-free survival (TFS) and overall survival (OS) were not reached, and the 4-year TFS and OS rates were 73% and 91%, respectively. The median PFS after end of therapy (PFS-EOT) was 29 months. TP53 mutations were associated with inferior PFS, TFS, and PFS-EOT, while CXCR4 mutations did not adversely impact these outcomes. Given the deep and durable responses seen in this study, concurrent BTK and BCL-2 inhibition warrants further development in WM. TP53 mutations emerged as an adverse factor in WM in this combination study.
    DOI:  https://doi.org/10.1002/ajh.70285
  18. Ther Adv Hematol. 2026 ;17 20406207261419953
    A phase I/II study of gilteritinib in combination with chemotherapy in newly diagnosed patients with AML in Asia: final analysis.
    Masashi Sawa, Toshihiro Miyamoto, Hee-Je Kim, Yasushi Hiramatsu, June-Won Cheong, Takayuki Ikezoe, Tomoki Naoe, Koichi Akashi, Satoshi Morita, Masanori Kosako, Masaki Shimura, Wataru Terada, Takeshi Kadokura, Jason Hill, Shuichi Miyawaki, Stanley C Gill, Alexandra Heinloth, Nahla Hasabou.
       Background: Mutations in the FMS-like tyrosine kinase 3 (FLT3) gene are present in approximately 30% of patients with newly diagnosed (ND) acute myeloid leukemia (AML), and are associated with worse therapy outcomes compared to the general AML population. Gilteritinib, a selective oral FLT3 inhibitor, is a promising treatment option for this patient population.
    Objectives: To assess the safety and efficacy of gilteritinib in combination with induction and consolidation chemotherapy in Asian patients with ND, FLT3-mutated (FLT3 mut+) AML.
    Design: This study was a phase I/II open-label, single-arm study. Herein, we present the final results from phase II.
    Methods: A total of 84 patients were enrolled in 33 centers across Japan, Korea, and Taiwan. All patients enrolled in phase II received induction and consolidation therapy with gilteritinib 120 mg/day plus chemotherapy (induction: ⩽2 cycles, idarubicin/cytarabine once-daily; consolidation: ⩽4 cycles, cytarabine twice-daily) followed by maintenance with gilteritinib 120 mg/day monotherapy (⩽26 cycles). The primary efficacy endpoint was the complete remission (CR) rate after induction therapy.
    Results: The primary endpoint of CR rate after induction was 50.0% (90% CI: 40.4-59.6). Gilteritinib in combination with chemotherapy achieved high composite CR (CRc; 86.6%, 95% CI: 77.3-93.1) rates after induction. The overall survival (OS) rate at 3 years was 71.6%, and the median OS was 48.2 months; however, due to the immaturity of the data, the median OS should be interpreted with caution. In addition, 51.2% of patients underwent hematopoietic stem cell transplantation during the study period. The safety profile of gilteritinib was as expected, and no new safety signals were identified.
    Conclusion: Induction and consolidation with gilteritinib plus chemotherapy, and maintenance with gilteritinib monotherapy were well tolerated in ND patients in Asia with FLT3 mut+ AML and had favorable efficacy compared with historical data.
    Trial registration: This trial was registered with the ClinicalTrials.gov identifier NCT02310321.
    Keywords:  Asia; FLT3 mutations; acute myeloid leukemia; combination therapy; gilteritinib; maintenance; transplant-eligible
    DOI:  https://doi.org/10.1177/20406207261419953
  19. Cancer. 2026 Mar 15. 132(6): e70299
    Teclistamab plus daratumumab significantly boosts survival for patients with early RRMM: The MajesTEC-3 trial is the first to test a combination of a bispecific antibody in the setting of first to third relapse after initial treatment for multiple myeloma.
    Leah Lawrence.
      
    DOI:  https://doi.org/10.1002/cncr.70299
  20. Blood. 2026 Mar 19. 147(12): 1244-1246
    Everybody gets a CAR! But do they need it?
    Nirav N Shah.
      
    DOI:  https://doi.org/10.1182/blood.2025031976
  21. Br J Haematol. 2026 Mar 18.
    Daratumumab plus bortezomib and dexamethasone (Dara-VD) in newly diagnosed Mayo 2004 stage IIIA and IIIB light-chain amyloidosis: Long-term follow-up results from a prospective phase 2 study.
    Gao Xue-Min, Xu Chengyang, Gao Ya-Juan, Guan Ai, Xu Yi, Chang Long, Shen Kai-Ni, Li Jian.
      Anti-CD38 monoclonal antibodies dramatically improve the prognosis in immunoglobulin light-chain (AL) amyloidosis, yet patients with end-stage (Mayo 2004 IIIB) disease are typically excluded from prospective trials. To evaluate the daratumumab plus bortezomib and dexamethasone (Dara-VD) regimen in Mayo 2004 stage III patients, we conducted a prospective phase 2 trial including 20 stage IIIA and 20 stage IIIB patients. The long-term follow-up results are reported here. The 24-month haematological complete response (CR) and very good partial response (VGPR) rate were 52.5% and 12.5% respectively. Organ responses improved after 12 months; the 24-month cardiac CR and VGPR rates were 15.0% and 35.0%. After a median follow-up of 50.9 months, 16 patients died and 10 patients had progressive diseases. The median overall survival (OS) had not been reached in either group, with a 4-year OS rate of 60.0% (95% confidence interval [CI]: 45.2%-75.2%). The median event-free survival (EFS) was 33.5 months (95% CI 21.0-46.0 months), with a 4-year EFS rate of 37.5% (95% CI: 24.3-54.7). No significant difference in OS or EFS was observed between stage IIIA and IIIB patients. In conclusion, the strong anti-plasma cell regimen Dara-VD provides comparable long-term responses and prognosis for Mayo stage IIIB patients.
    Keywords:  AL amyloidosis; Mayo 2004 stage IIIA and IIIB; daratumumab‐based treatment; efficacy; survival
    DOI:  https://doi.org/10.1111/bjh.70445
  22. Blood Adv. 2026 Mar 19. pii: bloodadvances.2025016688. [Epub ahead of print]
    Live-cell Pick-Seq (LiP-Seq): Interrogating ultra-rare mantle cell lymphoma persistent cells after CART19 therapy.
    Ran Xu, Gongwei Wu, Siobhan Rice, Matthew Booker, Jenalyn Celine Weekes, Hayden Luke Bell, Yifei Gao, Ajit J Nirmal, Huiyun Liu, Zoe Ciantra, Qingyu Luo, Amanda L Fortune, Karley Whalen, Timothy Matthew Guanci, Yifei Wan, Abner Louissaint, Joshua J Nordberg, Jia-Ren Lin, Michael T Hemann, Scott R Manalis, Philippe Armand, Eric L Smith, Caron A Jacobson, Michael Tolstorukov, Mark A Murakami, Peter K Sorger, David M Weinstock, Li Song, Andrew A Lane.
      Many cancer therapies induce high response rates, with some resulting in undetectable disease as assessed using standard clinical assays. This is particularly true in leukemia and lymphoma, where patients often achieve deep remission yet ultimately suffer relapse. This highlights a critical need to better understand the ultra-rare persistent cells that survive therapy but remain inaccessible to current techniques. Here we developed Live-cell Pick-Seq (LiP-Seq), an advanced platform leveraging multiplexed live-cell imaging to identify and retrieve individual target cells for downstream analysis. LiP-Seq enables high-resolution transcriptomic profiling of single, viable lymphoma cells present at frequencies as low as 10-6, providing a technological window into the biology of these elusive reservoirs. Applying this method to mantle cell lymphoma (MCL) patients following CD19 CAR-T cell therapy, we identified a recurrent upregulation of the immune modulator IFITM2 in the persistent cell fraction. Functional validation demonstrated that IFITM2 overexpression conferred protection against CAR T-cell cytotoxicity in vitro, implicating it as a potential survival mechanism under therapeutic pressure. Our results provide a first transcriptomic characterization of viable, ultra-rare persistent cells via LiP-Seq, establishing a new paradigm for identifying and targeting features that may enable treatment evasion.
    DOI:  https://doi.org/10.1182/bloodadvances.2025016688
  23. Blood. 2026 Mar 19. 147(12): 1247-1249
    Clonal dynamics of CH in CLL.
    Sarah Hanache, Koichi Takahashi.
      
    DOI:  https://doi.org/10.1182/blood.2025032522
  24. Zhongguo Shi Yan Xue Ye Xue Za Zhi. 2026 Feb;34(1): 293-297
    [Research Progress of Megakaryocyte Morphology in the Prognosis of Primary Myelofibrosis--Review].
    Zhi-Kang Zheng, Jian Huang.
      Primary myelofibrosis (PMF) is a myeloproliferative neoplasm (MPN) characterized by malignancy derived from hematopoietic stem cells. Compared with polycythemia vera (PV) and essential thrombocythemia (ET), PMF shows a worse clinical prognosis. Therefore, it is essential to explore biological markers for early identification and intervention to delay the process of the disease. Megakaryocytes (MK) play a central role in the pathogenesis and disease progression of PMF. The thrombophilia, the aggravation of myelofibrosis and the transformation to acute myeloid leukemia (AML) in patients with PMF are closely related to the morphological characteristics of MK.Changes in MK morphology are not only regulated by inflammatory mediators, but also influenced by specific genetic factors. This article will review the mechanism of MK morphological changes in PMF and the latest research progress on the prognosis of PMF with MK morphology, so as to provide reference for early clinical diagnosis and treatment.
    Keywords:  morphology of megakaryocytes; primary myelofibrosis; gene; inflammation; prognosis
    DOI:  https://doi.org/10.19746/j.cnki.issn.1009-2137.2026.01.043
  25. JTO Clin Res Rep. 2026 Apr;7(4): 100933
    Brief Report: Multi-Institution Real-World Analysis Evaluating Safety, Efficacy, and ctDNA Dynamics After Tarlatamab in Patients With Previously Treated SCLC and LCNEC.
    Graeme Fenton, Annie L Zhang, Sharon Zhong, Curtis Tatsuoka, Michelle Sittig, Alexandra Simms, Ranee Mehra, Afshin Dowlati, Taofeek K Owonikoko, Katherine Scilla, Melinda Hsu, Samuel Rosner.
      Tarlatamab, a bispecific T-cell engager targeting delta-like ligand 3 and CD3 on T cells, has generated impressive treatment response rates in relapsed extensive-stage SCLC and large cell neuroendocrine carcinoma. We performed a retrospective, multi-institutional analysis of 48 patients who received tarlatamab as standard of care to assess how safety and efficacy outcomes translate into real-world practice. Rates of cytokine release syndrome and immune effector cell-associated neurotoxicity syndrome were 54% and 33%, respectively, with most being grades 1 to 2 in severity (100% and 87.5%). Of the 30 patients included in our efficacy analysis, the best overall response rate was 67% and disease control rate was 73%. With median follow-up of 5.7 months, median progression-free survival was 4.9 months (95% confidence interval: 4-not reached) and median overall survival was not reached (95% confidence interval: 4.8-not reached). Nine patients underwent molecular response assessment, with circulating tumor DNA trends corresponding with radiographic response. In this multicenter cohort study, tarlatamab continued to demonstrate encouraging response rates and progression-free survival; however, differences were observed in rates and timing of key treatment-associated toxicities compared with previous trial data.
    Keywords:  Bispecific antibody; Real-world; Small cell lung cancer; Survival analysis; Tarlatamab; ctDNA
    DOI:  https://doi.org/10.1016/j.jtocrr.2025.100933
  26. Front Immunol. 2026 ;17 1807170
    Correction: VEXAS: A review of current understandings and emerging treatment strategies.
    Robert Holden, Yogeshraj Jeelall, Andrew McLean-Tooke, Kylan Pathmanathan, David Nolan.
      [This corrects the article DOI: 10.3389/fimmu.2025.1644404.].
    Keywords:  VEXAS; VEXAS syndrome; autoinflamatory diseases; myelodyslastic syndromes; myeloid cells
    DOI:  https://doi.org/10.3389/fimmu.2026.1807170
  27. Br J Haematol. 2026 Mar 17.
    Mediastinal grey zone lymphomas: Results of the expert pathological review analysis of a case series enrolled in the multicentre BIOGZL-2020 study in Italy.
    Elena Sabattini, Stefano Ascani, Sabino Ciavarella, Arianna Di Napoli, Fabio Facchetti, Stefano Lazzi, Lorenzo Leoncini, Luisa Lorenzi, Marco Lucioni, Giovanna Motta, Nassi Luca, Alice Parisi, Marco Paulli, Stefano Pileri, Maurilio Ponzoni, Claudio Tripodo, Simona Righi, Claudio Agostinelli.
      Mediastinal grey zone lymphoma (MGZL) is a rare disease with overlapping features between classical Hodgkin lymphoma (CHL) and primary mediastinal large B-cell lymphoma (PMBL). The recent classifications limit the disease to mediastinal cases. Epstein-Barr virus (EBV) is negative in most instances. Predominant resemblance to CHL (MGZL-HL) or primary mediastinal B-cell lymphoma (MGZL-PMBL) can commonly be defined, although mixed features do occur. The morpho-phenotypic heterogeneity of MGZL has significantly affected diagnostic reproducibility also among experts and the proposed diagnostic criteria turned out less concrete than for other lymphomas. Seventy GZL cases were collected from 14 Italian centres and slides reviewed by expert haematopathologists: 17 samples were confirmed according to current classification criteria, the residual being reclassified, mostly as CHL and PMBL, which well reflects the diagnostic challenge. By applying six B-cell markers, MGZL-HL commonly expressed ≥4 B-antigens in ≥50% neoplastic cells at moderate-strong intensity; MGZL-PMBL expressed less B-cell markers than expected (average 3.4 per case, in ≥50% neoplastic cells) at variable intensity. Overall, morphology, number of positive B-cell markers, staining intensity and percentage of positive neoplastic cells are features that must be considered collectively, case by case, trying to adhere to the recent classification criteria, being aware that not all cases may easily be included.
    Keywords:  B‐cell markers; Hodgkin; grey zone; lymphoma; mediastinal
    DOI:  https://doi.org/10.1111/bjh.70432
  28. Am J Hematol. 2026 Mar 16.
    Zanubrutinib in AL Amyloidosis Associated With Waldenström Macroglobulinemia and Other B-Cell Non-Hodgkin Lymphoma.
    Wouter Verhaar, Flores Weverling, Jahanzaib Khwaja, Despina Trajanova, Martine Chamuleau, Kirsty Cuthill, Shirley D'Sa, Paul A F Geerts, Kaz Groen, Troels Hammer, Marie José Kersten, Ida B Kristensen, Suzanne Lentzsch, Sophie Bernelot Moens, Amy Song, Andre J Vlot, Peter E Westerweel, Ute Hegenbart, Stefan Schönland, Ashutosh Wechalekar, Monique C Minnema, Josephine M I Vos.
      
    DOI:  https://doi.org/10.1002/ajh.70267
  29. Front Oncol. 2025 ;15 1740112
    MRD in multiple myeloma: the clinical perspective.
    Tommaso Caravita di Toritto, Angela Rago.
      Minimal residual disease (MRD) has emerged as a key prognostic factor in multiple myeloma (MM), allowing a more accurate evaluation of treatment efficacy beyond conventional complete remission. High-sensitivity techniques, including next-generation flow cytometry (NGF), next-generation sequencing (NGS), and allele-specific oligonucleotide quantitative PCR, enable detection of residual disease at levels of 10-5-10-6. Achieving MRD negativity is consistently associated with prolonged progression-free survival (PFS) and overall survival (OS) across different disease settings. In 2024, the U.S. Food and Drug Administration Oncologic Drugs Advisory Committee unanimously recognized MRD negativity as a primary endpoint in MM clinical trials, reinforcing its role as a validated surrogate of clinical benefit. This review summarizes current MRD detection methods and discusses how MRD assessment, interpreted in the context of recent pivotal clinical trials, may provide a practical framework to guide future treatment strategies in MM.
    Keywords:  MRD; flow cytometry; minimal residual disease; multiple myeloma; next-generation sequencing; progression-free survival
    DOI:  https://doi.org/10.3389/fonc.2025.1740112
  30. Blood Cancer J. 2026 Mar 17. pii: 30. [Epub ahead of print]16(1):
    Imatinib and nilotinib are equally successful in achieving therapy-free remission.
    Fang Cheng, Yu Wang, Yunfan Yang, Xin Du, Yu Zhu, Jianyu Weng, Na Xu, Jian Huang, Zhenfang Liu, Hongbo Ren, Huifang Zhao, Huanling Zhu, Qian Jiang, Yanli Zhang, Weiming Li.
      
    DOI:  https://doi.org/10.1038/s41408-026-01462-6
  31. Zhonghua Xue Ye Xue Za Zhi. 2026 Feb 14. 47(2): 123-129
    [Clinical characteristics, treatment, and prognosis of double-hit multiple myeloma with concurrent 1q21+ and t (4;14)].
    Y Guo, N Qiao, Y Tao, K M Liu, H Y Ouyang, Y F Liu, Y Wang, W P Zhang, J Q Mi.
      Objective: To analyze the clinical characteristics, therapeutic regimens, and prognosis of double-hit multiple myeloma (DHMM) patients with concurrent 1q21 copy number gain (1q21+) and t (4;14) , and to explore effective strategies to improve outcomes of this high-risk subgroup. Methods: A retrospective analysis was performed on 96 newly diagnosed DHMM patients with both 1q21+ and t (4;14) admitted to Ruijin Hospital Affiliated to Shanghai Jiao Tong University School of Medicine from September 2014 to September 2024. Baseline clinical characteristics, prognosis, and independent prognostic factors were evaluated. A logistic regression model was used to analyze the correlation between induction regimens, autologous hematopoietic stem cell transplantation (auto-HSCT) , and minimal residual disease (MRD) negativity. Results: The median age of the 96 DHMM patients was 62 (range: 36-79) years. Among them, 50 cases (52% ) were at R2-ISS stage Ⅳ, 11 cases (11% ) had concurrent del (17p) , 35 cases (36% ) underwent auto-HSCT, 39 cases (41% ) received triple-agent induction therapy with proteasome inhibitor (PI) , immunomodulatory drug (IMiD) and anti-CD38 monoclonal antibody (CD38Ab) , 25 cases (26% ) achieved MRD-negative complete response (CR) . The clone size of 1q21+ was positively correlated with that of t (4;14) (r=0.46, P<0.001) , while the clonal burden of 1q21+ was significantly lower than that of t (4;14) . With a median follow-up of 36 (range: 6-126) months, the median progression-free survival (PFS) was 26 (95% CI: 22-50) months, and the estimated median overall survival (OS) was 4.3 (95% CI: 2.1-6.4) years. Extramedullary relapse occurred in 22 cases (23% ) . Multivariate analysis showed that newly diagnosed extramedullary involvement of soft tissue was an independent risk factor for both PFS and OS (all P<0.05) . Del (17p) shortened PFS, whereas MRD negativity significantly prolonged PFS. Both triple-agent induction therapy (PI+IMiD+CD38Ab) and auto-HSCT improved the MRD-negative rate (all P<0.05) . Conclusion: DHMM patients with concurrent 1q21+ and t (4;14) exhibit aggressive clinical features and poor prognosis. Triple-agent induction therapy (PI+IMiD+CD38Ab) and auto-HSCT are associated with MRD negativity and improved PFS, but achieving long-term survival remains challenging for these patients.
    Keywords:  1q21 gain/amplification; Antibodies, monoclonal; Hematopoietic stem cell transplantation; Multiple myeloma; Prognosis; t (4;14)
    DOI:  https://doi.org/10.3760/cma.j.cn121090-20250520-00238
  32. Blood. 2026 Mar 17. pii: blood.2025031869. [Epub ahead of print]
    Immunodeficiency-associated primary CNS lymphomas: An International Primary CNS Lymphoma Collaborative Group (IPCG) Study.
    Leon D Kaulen, Lakshmi Nayak, Philipp Karschnia, Imke Kraai, Daniela Raffaela Galluzzo, Fleur A de Groot, Matthew Witterholt, Laura Donovan, Sita Bhella, Luis P Kuschel, Christopher P Fox, Sabine Seidel, James Paterson, Benjamin Richter, Karan S Dixit, Thomas Zeyen, Juan Pablo Alderuccio, Silvia Montoto, Outi Kuittinen, Benjamin-Leon Traub, Sofia Doubrovinskaia, Hannah Rohdjess, Katharina Mueller, Roelien Enting, Jeroen de Bresser, Hanne Kuitunen, Fabio M Iwamoto, Alvaro J Alencar, Ulrich Herrlinger, Michael Platten, Kate Cwynarski, Joe S Mendez, Patrick Roth, Louisa von Baumgarten, Anca Prica, Govind Bhagat, Kathryn Lurain, David Schiff, Joost Sp Vermaat, Joachim Baehring, Marcel Nijland, Jörg Dietrich, Tracy T Batchelor, Wolfgang Wick.
      Immunodeficiency-associated primary CNS lymphoma (ID-PCNSL) represents a clinicopathologically distinct PCNSL subtype, for which large studies and prognostic models are lacking. To address this gap, the International PCNSL Collaborative Group conducted an international retrospective multi-center study, integrating clinical, radiological, and pathological data from 308 ID-PCNSL, diagnosed at 23 participating sites in 7 countries. Pre-existing immunodeficiency included administration of immunosuppressants for transplantation (41.2%) or autoimmunity (36.7%), and HIV infection (21.7%). All tumors were diffuse large B-cell lymphomas, with Epstein-Barr virus (EBV) detected in 79.2%. Immune reconstitution together with rituximab-methotrexate-(RM)-based chemotherapy was associated with highest response rates and prolonged progression-free survival, irrespective of immunodeficiency subtype and EBV status. Survival outcomes were highly variable with a 54-month median overall survival. Multivariable Cox regression identified age (per year increment HR: 1.05 (95%-CI:1.02-1.07); p < 0.001), Karnofsky Performance status (KPS) < 70 (HR: 3.10 (95%-CI:1.67-5.87); p < 0.001), EBV positivity (HR: 3.26 (95%-CI:1.47-7.33); p = 0.004) as prognostic factors for OS. A prognostic score was developed based on the sum of these adverse variables (age > 60 years, KPS < 70, EBV positivity). Stratification by this score yielded median survival times of 135, 29, and 3 months in patients with up to one, two and three unfavorable markers (p < 0.0001). It allowed improved prognostic stratification of ID-PCNSL as compared to the well-established MSKCC and IELSG models developed for immunocompetent PCNSL. Collectively, this large international cohort defines clinicobiologic features of ID-PCNSL and introduces an easily applicable prognostic system with potential to guide future management.
    DOI:  https://doi.org/10.1182/blood.2025031869
  33. Blood. 2026 Mar 19. 147(12): 1239-1242
    Introduction to a review series on the new wave of targeted therapeutics for MPNs.
    Jason Gotlib.
      
    DOI:  https://doi.org/10.1182/blood.2025032534
  34. Blood Sci. 2026 Jun;8(2): e00276
    Zanubrutinib enhances CD19 CAR T killing of B-cell lymphoma by inhibiting BTK phosphorylation, regulating PI3K/AKT/mTOR pathway, and promoting autophagy.
    Hao Yao, Ling Qiu, Shi-Hui Ren, Dan Chen, Meng-Jiao Li, Bai-Tao Dou, Nan Zhang, Xiao Wang, Yi Su, Alex H Chang, Fang-Yi Fan.
      Anti-CD19 chimeric antigen receptor T cells (CAR T) still have many limitations, including insufficient clinical efficacy. Zanubrutinib is a second-generation Bruton tyrosine kinase (BTK) inhibitor with higher drug potency, and it is not clear whether it has an enhanced killing effect of CD19 CAR T on B-cell lymphoma. Therefore, this study will investigate the role and mechanism of zanubrutinib in CD19 CAR T therapy against B-cell lymphoma. B-cell lymphoma cells Daudi were proportionally co-cultured with CD19 CAR T and intervened using different concentrations of zanubrutinib, and the changes of cell viability, apoptosis, autophagy, and phosphoinositide 3-kinase (PI3K)/protein kinase B (AKT)/mechanistic target of rapamycin (mTOR) pathway-related factors were assessed using the Cell Counting Kit-8 (CCK-8) assay, flow cytometry, Western blotting, transmission electron microscopy, and immunofluorescence staining. Also, the effect of zanubrutinib on the sensitivity of B-cell lymphoma mice to CAR T-cell therapy was observed. The results showed that zanubrutinib increased the sensitivity of B-cell lymphoma to CD19 CAR T-cells, promoted apoptosis and autophagy, and inhibited BTK phosphorylation and the PI3K/AKT/mTOR signaling pathway. Zanubrutinib can promote the killing of B-cell lymphoma by CD19 CAR T. Collectively, zanubrutinib enhances CD19 CAR T killing of B-cell lymphoma by inhibiting BTK phosphorylation, regulating PI3K/AKT/mTOR pathway, and promoting autophagy.
    Keywords:  B-cell lymphoma; CD19 CAR T; PI3K/AKT/mTOR signaling pathway; Zanubrutinib
    DOI:  https://doi.org/10.1097/BS9.0000000000000276
  35. Eur J Haematol. 2026 Mar 15.
    Ph-Negative Acute Lymphoblastic Leukemia in the Older Adults: Biology, Therapeutic Strategies and Unmet Needs.
    Antonella Bruzzese, Ernesto Vigna, Enrica Antonia Martino, Santino Caserta, Francesco Mendicino, Maria Eugenia Alvaro, Caterina Labanca, Eugenio Lucia, Virginia Olivito, Marco Fiorillo, Nicola Amodio, Fortunato Morabito, Massimo Gentile.
      Acute lymphoblastic leukaemia (ALL) in older adults represents a growing clinical challenge, driven by an ageing population, adverse disease biology, and reduced tolerance to intensive chemotherapy. Although pediatric-inspired regimens have improved outcomes in younger adults with Philadelphia chromosome (Ph)-negative ALL, survival in older patients remains poor, with high rates of treatment-related toxicity, early death, and relapse. Age-related comorbidities, impaired organ function, and unfavorable cytogenetic and molecular features, including low hypodiploidy and TP53 mutations, further compromise prognosis. In this context, monoclonal antibodies such as blinatumomab and inotuzumab ozogamicin (InO), used alone or in combination with reduced-intensity chemotherapy, have emerged as promising frontline approaches capable of deep remissions with improved tolerability. Moreover, CAR T-cell therapy is increasingly recognized as a potentially effective strategy for relapsed/refractory disease in selected older adults, particularly in the setting of low disease burden, with acceptable safety in carefully monitored cohorts. However, issues such as antigen loss, lineage switch, the management of T-cell ALL, and the optimal sequencing of immunotherapies remain unresolved. Across all treatment strategies, comprehensive geriatric assessment appears more informative than performance status alone in predicting tolerability and outcome, supporting its integration into trial design and routine decision-making. Overall, the refinement of immunotherapeutic approaches, coupled with biologically and geriatrically tailored treatment algorithms, offers the most promising avenue to improve long-term outcomes for older patients with ALL.
    Keywords:  CAR T‐cell therapy; acute lymphoblastic leukemia; geriatric assessment; monoclonal antibodies; older adults
    DOI:  https://doi.org/10.1111/ejh.70169
  36. Sci Rep. 2026 Mar 16. pii: 9197. [Epub ahead of print]16(1):
    VS-4718 enhances apoptosis induced by low-dose carfilzomib and overcomes carfilzomib resistance in PSMB5-mutated proteasome inhibitor resistant multiple myeloma.
    Ellen Leich-Zbat, Sofia Catalina Heredia-Guerrero, Marietheres Evers, Thorsten Stühmer, Tina Grieb, Hilka Rauert-Wunderlich, Ralf C Bargou, Andreas Rosenwald, Manik Chatterjee, Daniela Brünnert.
      
    Keywords:  Carfilzomib; Multiple myeloma; PYK2; Proteasome inhibitor resistance; Proteasome inhibitors; VS-4718
    DOI:  https://doi.org/10.1038/s41598-026-43205-4
  37. Eur J Haematol. 2026 Mar 19.
    The Role of Microenvironment in Bispecific Antibodies Treatment in Multiple Myeloma.
    Serena Barachini, Raffaella Cassano Cassano, Francesca Ronca, Iacopo Petrini, Sara Galimberti, Gabriele Buda.
      Multiple myeloma (MM) is a clonal plasma cell malignancy that remains largely incurable despite major therapeutic advances. T-cell-redirecting bispecific antibodies (BsAbs) and chimeric antigen receptor T (CAR-T) cells have recently emerged as highly effective therapies in relapsed/refractory MM, inducing deep responses even in heavily pretreated patients. However, disease relapse, limited durability of response, and treatment-related toxicities remain frequent, underscoring the need to better understand mechanisms of resistance. Accumulating evidence indicates that the tumor microenvironment (TME) plays a central role in shaping BsAb efficacy in MM. Immunosuppressive cellular components, including regulatory T-cells, myeloid-derived suppressor cells, and dysfunctional antigen-presenting cells, as well as inhibitory cytokines, hypoxia, and metabolic constraints within the TME, profoundly impair T-cell activation, expansion, and persistence following BsAb engagement. In addition, chronic CD3 stimulation within the TME may promote T-cell exhaustion, contributing to suboptimal responses and disease progression. This review focuses on the dynamic interplay between BsAbs and the MM TME, highlighting how microenvironment-driven immune suppression, antigen escape, and impaired T-cell fitness influence clinical outcomes. We further discuss emerging strategies designed to overcome these barriers, including rational combination approaches, immunomodulatory agents, and next-generation trispecific antibodies that enhance co-stimulation or dual-antigen targeting. Understanding and therapeutically modulating the TME represents a critical step toward improving the depth, durability, and safety of BsAb-based therapies in MM.
    Keywords:  bispecific antibodies; drug resistance; multiple myeloma; tumor microenvironment
    DOI:  https://doi.org/10.1111/ejh.70168
  38. Ann Hematol. 2026 Mar 19. pii: 190. [Epub ahead of print]105(4):
    Restless legs syndrome in chronic myeloid leukemia: an overlooked condition with a significant impact on health-related quality of life.
    Turgut Gürer, Ulgar Boran Günay, Berkay Kılıç, Ayşegül Akkan Suzan, Duygu Seyhan Erdoğan, Deniz Özmen, Tuğrul Elverdi, Ayşe Salihoğlu, Ayşegül Gündüz, Muhlis Cem Ar, Zafer Başlar, Ahmet Emre Eşkazan.
      
    Keywords:  Chronic myeloid leukemia; Quality of life; Restless legs syndrome; Symptom burden; Tyrosine kinase inhibitor
    DOI:  https://doi.org/10.1007/s00277-026-06832-5
  39. Blood Adv. 2026 Mar 17. pii: bloodadvances.2025018695. [Epub ahead of print]
    Phase 1b study of ABBV-744, a novel, selective BET inhibitor, as monotherapy in patients with myelofibrosis.
    John O Mascarenhas, Laura Maria Fogliatto, Steven D Green, Ignacio Corvalan, Elie Traer, Keita Kirito, Hun S Chuah, Kazuki Sakatoku, Rasmus T Hoeg, Mohamad Khawandanah, David Lavie, Zoë Hunter, David Quinn, Yizhuo Wang, Jason G Harb, Jiuhong Zha, Uriel M Malyankar, Ellen K Ritchie.
      Janus kinase inhibitors (JAKi) are standard of care for patients with myelofibrosis (MF) but can be associated with treatment-limiting cytopenias and do not modify underlying disease. Novel treatments targeting other clinically relevant pathways are needed. Inhibitors of bromodomain (BD) and extra-terminal domain (BET) proteins are a promising class of drugs that have demonstrated the ability to modulate key pathways involved in inflammation, fibrosis, and apoptosis. ABBV-744 is a novel small molecule that targets the BDII domain of BET proteins and has previously been shown to be well tolerated when administered daily at doses of 120 mg and 180 mg to patients with acute myeloid leukemia. We report the outcomes of a multicenter, open-label phase 1b study of ABBV-744 in patients with MF who received 1 or more prior lines of therapy, including a JAKi. The primary objective was safety, including dose-limiting toxicities (DLTs). Secondary endpoints included a reduction in spleen volume of ≥35% (SVR35), ≥50% reduction in total symptom score (TSS50), objective response rate, and pharmacokinetics. All 21 patients experienced at least 1 treatment-emergent adverse event, and 11 patients experienced a DLT. The most common events leading to DLTs were thrombocytopenia (33%) and anemia (24%). SVR35 was attained in 24% of patients at Week 12 and 33% at Week 24. TSS50 was reported for 29% of patients at 12 weeks and 19% at Week 24. These outcomes are noteworthy in this heavily pretreated population considering the advanced disease state and limited treatment options for this patient population. (NCT04454658).
    DOI:  https://doi.org/10.1182/bloodadvances.2025018695
  40. Zhongguo Shi Yan Xue Ye Xue Za Zhi. 2026 Feb;34(1): 302-305
    [Research Progress in ALK+/- Anaplastic Large Cell Lymphoma--Review].
    Cheng-Kan DU, Wen-Hao Weng.
      Anaplastic large cell lymphoma (ALCL) is a rare CD30-positive T-cell non-Hodgkin lymphoma, primarily classified into two subtypes: ALK-positive ( ALK +) and ALK-negative ( ALK -). ALK + ALCL is commonly seen in younger patients and characterized by rapid progression, with the majority of patients achieving complete remission after chemotherapy. In contrast, ALK -ALCL generally affects older patients, presenting with similar clinical features but a poorer prognosis. Genetic rearrangements, such as DUSP22 and TP63, have a significant impact on patient survival. The current treatment regimen primarily involves CHOP, but its efficacy is limited, especially in relapsed cases. Consequently, there is an urgent need to improve frontline and salvage treatment options. Future research should focus on the integration of targeted therapies with molecular mechanisms to enhance therapeutic outcomes and survival rates. Understanding the subtypes and molecular characteristics of ALCL is essential for optimizing therapeutic strategies. Therefore, this review summarizes recent research advances on ALK +/- ALCL to provide insights for optimizing treatment approaches.
    Keywords:  anaplastic large cell lymphoma; ALK gene; immune phenotype; clinical characteristics; treatment
    DOI:  https://doi.org/10.19746/j.cnki.issn.1009-2137.2026.01.045
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