https://doi.org/10.55788/c6eac6b1
“Flow cytometric MRD assessment is prognostic of clinical outcomes in venetoclax combinations-treated patients with various AML mutations,” stated Mr Jad Othman (Guy’s and St Thomas’ NHS Foundation Trust, UK) [1,2]. The presented study aimed to determine whether MRD by qPCR is prognostic of clinical outcomes in patients with NPM1-mutated AML who achieved CR/CRi in the real-world on venetoclax plus either low-dose cytarabine or a hypomethylating agent.
In a cohort of 55 patients, the best MRD response rates in the first 6 months of therapy were as follows: MRD undetectable (46%), ≥4 log reduction (19%), <4 log reduction (35%). After a median follow-up of 24.3 months, the deepest MRD reduction within the first 6 months was strongly related to overall survival (OS; P=0.00027) and event-free survival (EFS; P<0.0001), favouring those with undetectable MRD over the other subgroups (see Figure). Mr Othman added that an MRD cut-off of <0.005 NPM1 copies/100 ABL was the best discriminator for OS (P<0.0001) and EFS (P<0.0001). Finally, it was noted that peripheral blood MRD, although less sensitive than bone marrow MRD, may be adequately sensitive to predict clinical outcomes.
Figure: Deepest MRD reduction within the first 6 months is strongly associated with outcomes [2]
OS, overall survival; EFS, event-free survival.
- Pratz KW, et al. J Clin Oncol. 2022;40(8):855–865.
- Othman J, et al. Molecular MRD Assessment Is Strongly Prognostic in Patients with NPM1¬ Mutated AML Receiving Venetoclax Based Non-Intensive Therapy. Abstract 840, ASH 64th Annual Meeting, 10–13 December 2022, New Orleans, LA, USA.
Copyright ©2023 Medicom Medical Publishers
Posted on
Table of Contents: ASH 2022
Featured articles
Acute Lymphoblastic Leukaemia
Blinatumomab candidate for standard-of-care in newly diagnosed B-ALL
High-dose methotrexate or standard interim maintenance in young patients with ALL?
Acute Myeloid Leukaemia
Excellent results for triplet regimen in FLT3-mutated AML
MRD by qPCR prognostic of outcomes in venetoclax-treated NPM1-mutated AML
Promising results for triplet therapy with magrolimab in AML
Should we use intensive chemotherapy prior to allo-HCT in relapsed/refractory AML?
Chronic Leukaemia
Zanubrutinib wins battle of BTK inhibitors in relapsed or refractory CLL/SLL
Ibrutinib plus venetoclax displays long-term benefits in CLL
Multiple Myeloma
Talquetamab further investigated in heavily pre-treated MM after promising phase 2 data
Promising results of elranatamab for MM in phase 2 MagnetisMM-3 trial
Deep and durable responses for quadruple therapy in smouldering MM
Ultra-sensitive MRD assessment in MM with BloodFlow
CAR-Hematotox score proves useful in relapsed/refractory MM
Head-to-head: VMP versus Rd in transplant-ineligible MM
Lymphoma
Ibrutinib added to ASCT improves clinical outcomes in mantle cell lymphoma
High-dose chemotherapy plus ASCT superior to standard immuno-chemotherapy in primary CNS lymphoma
Odronextamab has considerable anti-tumour effects in relapsed/refractory diffuse large B-cell lymphoma and follicular lymphoma
Excellent results for AFM13-complexed NK cells in CD30-positive lymphoma
CAR-Hematotox score predicts toxicity, infections, and clinical outcomes in MCL
Myeloproliferative Neoplasms
Efgartigimod successful in immune thrombocytopenia
INCA033989: novel investigational agent for CALR-mutated MPN
Ruxolitinib mediates clonal evolution of RAS pathway mutations in MPN
Immune Thrombocytopenia
Long-term risk for haematologic disease in persistent, isolated mild thrombocytopenia
Various Topics
C1 inhibitor deficiency linked to thrombosis
Durable responses to gene therapy in haemophilia A
Long-term benefits from beti-cel in transfusion-dependent β-thalassaemia
Neutrodiet: non-restricted diet is the preferred option after SCT
Iptacopan offers solution for patients with PNH and residual anaemia after standard-of-care
Novel therapy may replace standard-of-care prophylaxis for GVHD
LMWH does not result in higher live birth rates in women with inherited thrombophilia
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