Acute myeloid leukemia (AML) is a polyclonal malignancy marked by high relapse rates despite initial morphologic remission. Although measurable residual disease (MRD) is an established prognostic tool, increasing evidence supports a role for pre-emptive, MRD-directed therapy. AML monitoring is hampered by absence of a universal MRD marker, necessitating a more personalized approach. NPM1 is suited to an MRD-directed strategy as the mutation is AML-defining and monitoring methods highly sensitive. Critically, rising NPM1mut levels portend clinical relapse with high fidelity and recent studies demonstrate that venetoclax-based regimens induce rapid and deep MRD responses in a high proportion of patients with NPM1mut MRD relapse. The range of MRD-directed treatment options are expanding and include FLT3 and menin inhibitors for MRD relapse driven by FLT3-ITD and KMT2A rearrangements, respectively. To overcome the logistical issue of multiple MRD markers and associated therapies, we have developed a multi-target, multi-arm platform trial named INTERCEPT. Novel features include the potential to adaptively expand the range of MRD markers and directed therapies, seamless transition of patients from a local to centralized MRD monitoring framework, a clinical decision rules approach to allocate treatment in a hierarchical and pre-specified manner, creation of parallel protocol appendices to enable multiple industry partners to co-exist with commercial independence, and development of approaches to minimize the "MRD relapse to treatment" time interval. The future success of MRD-directed therapy will depend on rapid diagnostic turnaround, coordinated logistics and innovative clinical trial designs able to keep pace with advances in MRD-detection technologies and associated targeted therapies.
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October 17, 2025
MRD intervention in AML: A new therapeutic horizon Open Access
Clinical Trials & Observations
Andrew H Wei,
Peter MacCallum Cancer Centre and Royal Melbourne Hospital, Melbourne, Australia
* Corresponding Author; email: wei.a@wehi.edu.au
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Harry J Iland,
Harry J Iland
Royal Prince Alfred Hospital, Camperdown, Australia
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Courtney D. DiNardo,
Courtney D. DiNardo
The University of Texas MD Anderson Cancer Center, Houston, Texas, United States
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John Reynolds
John Reynolds
Alfred Health and Monash University, Melbourne, VIC, Australia
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Blood blood.2025029010.
Article history
Submitted:
July 24, 2025
Revision Received:
September 8, 2025
Accepted:
September 18, 2025
Citation
Andrew H Wei, Harry J Iland, Courtney D. DiNardo, John Reynolds; MRD intervention in AML: A new therapeutic horizon. Blood 2025; blood.2025029010. doi: https://doi.org/10.1182/blood.2025029010
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