The phase 2 TUSCANY trial included patients with newly diagnosed AML to investigate the investigational drug tuspetinib [1]. “This agent is a potent oral kinase inhibitor targeting SYK, FLT3, JAK1/2, RSK1/2, and mutant KIT kinases that drive dysregulated proliferation in AML,” explained Dr Gabriel Mannis (Stanford University, CA, USA). Participants received a combination of standard-dose azacitidine and venetoclax plus tuspetinib in a range of 40–120 mg daily for 21–28 days per 28-day cycle. The current analysis reported data from 10 participants.
Tuspetinib appeared to be very well-tolerated. There were no non-haematological serious adverse events (AEs), and diarrhoea was the most common non-haematological AE, occurring in approximately 20% of the participants. Grade ≥3 haematologic AEs such as anaemia (57.1%) and neutropenia (42.9%) were frequently observed. Dr Mannis emphasised that the research team had not seen QTc prolongation, CPK elevations, differentiation syndrome, or prolonged myelosuppression in cycle 1 in the absence of AML. Furthermore, the composite complete remission rate was 85.7%. “Next to this, 3 patients were MRD-negative at the time of the analysis, one of whom was a patient with TP53-mutated complex-karyotype disease,” explained Dr Mannis.
“Although it is very early, it appears that tuspetinib can be added to standard-of-care dosing of venetoclax and azacitidine without prolonged myelosuppression or undue toxicity,” decided Dr Mannis. “The treatment regimen was associated with encouraging anti-tumour activity, and we look forward to seeing more results in the future.”
- Daver N, et al. TUSCANY study of safety and efficacy of tuspetinib plus standard of care venetoclax and azacitidine in study participants with newly diagnosed AML ineligible for induction chemotherapy. S139, EHA2025 Congress, 12–15 June, Milan, Italy.
Copyright ©2025 Medicom Medical Publishers
Posted on
Table of Contents: EHA 2025
Featured articles
Letter from the Editor
Non-Malignant Haematology
Promising safety and efficacy data for novel anti-CD38 treatment in ITP
Novel investigational gene-editing therapy for TDT and SCD
HSCT may reduce risk of ocular complications in SCD
Are PBSCs a viable source for haplo-HSCT in SCD?
Multiple Myeloma/Plasma Cell Disorders
Large pooled analysis reveals prognostic utility of circulating tumour cells in MM
RedirecTT-1: Dual antigen-targeting treatment associated with promising efficacy in EMD myeloma
Prognostic impact of circulating tumour cells in AL amyloidosis
IRAKLIA: Novel isatuximab delivery system improves patient satisfaction in MM
MagnetisMM-6: Excellent early results of elranatamab in MM
MIDAS: Is ASCT needed in MM after reaching MRD-negativity with IsaKRD?
Novel trispecific antibody may be a game-changer for relapsed/refractory MMF
Lymphoma
GAIA/CLL13: Positive 5-year efficacy outcomes for GIV in CLL
ELM-2: Survival benefit for patients with FL on odronextamab
inMIND: Positive phase 3 results for tafasitamab combination in FL
Unravelling real-world safety and effectiveness of axi-cel in LBCL
STARGLO: Long-term clinical benefits of Glofit-GemOx over R-GemOx in DLBCL
ECHO: Older patients with high-risk MCL benefit from acalabrutinib added to BR
POLARGO: Pola-R-GemOx delivers overall survival benefit in second-line DLBCL
Acute Leukaemia (AML and ALL)
Refined AML risk prediction by improved understanding of genetics
TUSCANY: Promising data for the addition of tuspetinib in untreated chemo-ineligible AML
Chemogenomic profiling appears reliable strategy to improve outcomes in T-ALL/ETP-ALL
Dasatinib does not cross the finish line in the phase 3 AML study
Myeloid Neoplasms
ASC4START: asciminib showed superior tolerability to nilotinib in CML
Encouraging results for new mutation-specific targeted therapy in CALR-mutated ET
Improving diagnosis, classification, and prognosis of MDN with an AI-based model
SURPASS-ET: Ropeg meets primary endpoint in essential thrombocythemia
MANIFEST-2: Sustained benefits of pelabresib plus ruxolitinib in myelofibrosis
Stem Cell Transplantation
Targeted anti-thymocyte globulin dosing improves transplantation outcomes
HCT Frailty Scale may refine the allo-HCT selection process
Ravulizumab shows tolerability and efficacy in HSCT-thrombotic microangiopathy
ALLG BM12 CAST: improved GRFS through novel GVHD prophylaxis
site created by:
© 2024 Medicom Medical Publishers. All rights reserved. Terms and Conditions | Privacy Policy
HEAD OFFICE
Laarderhoogtweg 25
1101 EB Amsterdam
The Netherlands
T: +31 85 4012 560
E: publishers@medicom-publishers.com