FLT3 inhibitors as MRD-guided salvage treatment for molecular failure in FLT3 mutated AML

Jad Othman; Nicola Potter; Katya Mokretar; David Taussig; Anjum Khan; Pramila Krishnamurthy; Anne-Louise Latif; Paul Cahalin; James Aries; Mariam Amer; Edward Belsham; Eibhlin Conneally; Charles Craddock; Dominic Culligan; Mike Dennis; Caroline Duncan; Sylvie D Freeman; Caroline Furness; Amanda Gilkes; Paraskevi Gkreka; Katherine Hodgson; Wendy Ingram; Manish Jain; Andrew King; Steven Knapper; Panagiotis Kottaridis; Mary Frances McMullin; Unmesh Mohite; Loretta Ngu; Jenny O'Nions; Katharine Patrick; Tom Rider; Wing Roberts; Marianne Tang Severinsen; Neill Storrar; Tom Taylor; Nigel H Russell; Richard Dillon

doi:10.1038/s41375-023-01994-x

FLT3 inhibitors as MRD-guided salvage treatment for molecular failure in FLT3 mutated AML

Jad Othman, Nicola Potter, Katya Mokretar, David Taussig, Anjum Khan, Pramila Krishnamurthy, Anne-Louise Latif, Paul Cahalin, James Aries, Mariam Amer, Edward Belsham, Eibhlin Conneally, Charles Craddock, Dominic Culligan, Mike Dennis, Caroline Duncan, Sylvie D Freeman, Caroline Furness, Amanda Gilkes, Paraskevi GkrekaKatherine Hodgson, Wendy Ingram, Manish Jain, Andrew King, Steven Knapper, Panagiotis Kottaridis, Mary Frances McMullin, Unmesh Mohite, Loretta Ngu, Jenny O'Nions, Katharine Patrick, Tom Rider, Wing Roberts, Marianne Tang Severinsen, Neill Storrar, Tom Taylor, Nigel H Russell, Richard Dillon^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

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Abstract

Patients with FLT3-mutated AML have a high relapse rate and suboptimal outcomes. Many have co-mutations suitable for measurable residual disease (MRD) monitoring by RT-qPCR and those destined to relapse can be identified by high or rising levels of MRD, called molecular failure. This provides a window for pre-emptive intervention, but there is little evidence to guide treatment. The use of FLT3 inhibitors (FLT3i) appears attractive but their use has not yet been evaluated. We identified 56 patients treated with FLT3i at molecular failure. The FLT3 mutation was an ITD in 52, TKD in 7 and both in 3. Over half of patients had previously received midostaurin. Molecular failure occurred at a median 9.2 months from diagnosis and was treated with gilteritinib (n = 38), quizartinib (n = 7) or sorafenib (n = 11). 60% achieved a molecular response, with 45% reaching MRD negativity. Haematological toxicity was low, and 22 patients were bridged directly to allogeneic transplant with another 6 to donor lymphocyte infusion. 2-year overall survival was 80% (95%CI 69-93) and molecular event-free survival 56% (95%CI 44-72). High-sensitivity next-generation sequencing for FLT3-ITD at molecular failure identified patients more likely to benefit. FLT3i monotherapy for molecular failure is a promising strategy which merits evaluation in prospective studies.

Original language	English
Journal	Leukemia
Early online date	9 Aug 2023
DOIs	https://doi.org/10.1038/s41375-023-01994-x
Publication status	E-pub ahead of print - 9 Aug 2023

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Othman, J., Potter, N., Mokretar, K., Taussig, D., Khan, A., Krishnamurthy, P., Latif, A.-L., Cahalin, P., Aries, J., Amer, M., Belsham, E., Conneally, E., Craddock, C., Culligan, D., Dennis, M., Duncan, C., Freeman, S. D., Furness, C., Gilkes, A., ... Dillon, R. (2023). FLT3 inhibitors as MRD-guided salvage treatment for molecular failure in FLT3 mutated AML. Leukemia. Advance online publication. https://doi.org/10.1038/s41375-023-01994-x

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title = "FLT3 inhibitors as MRD-guided salvage treatment for molecular failure in FLT3 mutated AML",

abstract = "Patients with FLT3-mutated AML have a high relapse rate and suboptimal outcomes. Many have co-mutations suitable for measurable residual disease (MRD) monitoring by RT-qPCR and those destined to relapse can be identified by high or rising levels of MRD, called molecular failure. This provides a window for pre-emptive intervention, but there is little evidence to guide treatment. The use of FLT3 inhibitors (FLT3i) appears attractive but their use has not yet been evaluated. We identified 56 patients treated with FLT3i at molecular failure. The FLT3 mutation was an ITD in 52, TKD in 7 and both in 3. Over half of patients had previously received midostaurin. Molecular failure occurred at a median 9.2 months from diagnosis and was treated with gilteritinib (n = 38), quizartinib (n = 7) or sorafenib (n = 11). 60% achieved a molecular response, with 45% reaching MRD negativity. Haematological toxicity was low, and 22 patients were bridged directly to allogeneic transplant with another 6 to donor lymphocyte infusion. 2-year overall survival was 80% (95%CI 69-93) and molecular event-free survival 56% (95%CI 44-72). High-sensitivity next-generation sequencing for FLT3-ITD at molecular failure identified patients more likely to benefit. FLT3i monotherapy for molecular failure is a promising strategy which merits evaluation in prospective studies.",

author = "Jad Othman and Nicola Potter and Katya Mokretar and David Taussig and Anjum Khan and Pramila Krishnamurthy and Anne-Louise Latif and Paul Cahalin and James Aries and Mariam Amer and Edward Belsham and Eibhlin Conneally and Charles Craddock and Dominic Culligan and Mike Dennis and Caroline Duncan and Freeman, {Sylvie D} and Caroline Furness and Amanda Gilkes and Paraskevi Gkreka and Katherine Hodgson and Wendy Ingram and Manish Jain and Andrew King and Steven Knapper and Panagiotis Kottaridis and McMullin, {Mary Frances} and Unmesh Mohite and Loretta Ngu and Jenny O'Nions and Katharine Patrick and Tom Rider and Wing Roberts and Severinsen, {Marianne Tang} and Neill Storrar and Tom Taylor and Russell, {Nigel H} and Richard Dillon",

note = "{\textcopyright} 2023. The Author(s).",

year = "2023",

month = aug,

day = "9",

doi = "10.1038/s41375-023-01994-x",

language = "English",

journal = "Leukemia",

issn = "0887-6924",

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Othman, J, Potter, N, Mokretar, K, Taussig, D, Khan, A, Krishnamurthy, P, Latif, A-L, Cahalin, P, Aries, J, Amer, M, Belsham, E, Conneally, E, Craddock, C, Culligan, D, Dennis, M, Duncan, C, Freeman, SD, Furness, C, Gilkes, A, Gkreka, P, Hodgson, K, Ingram, W, Jain, M, King, A, Knapper, S, Kottaridis, P, McMullin, MF, Mohite, U, Ngu, L, O'Nions, J, Patrick, K, Rider, T, Roberts, W, Severinsen, MT, Storrar, N, Taylor, T, Russell, NH & Dillon, R 2023, 'FLT3 inhibitors as MRD-guided salvage treatment for molecular failure in FLT3 mutated AML', Leukemia. https://doi.org/10.1038/s41375-023-01994-x

TY - JOUR

T1 - FLT3 inhibitors as MRD-guided salvage treatment for molecular failure in FLT3 mutated AML

AU - Othman, Jad

AU - Potter, Nicola

AU - Mokretar, Katya

AU - Taussig, David

AU - Khan, Anjum

AU - Krishnamurthy, Pramila

AU - Latif, Anne-Louise

AU - Cahalin, Paul

AU - Aries, James

AU - Amer, Mariam

AU - Belsham, Edward

AU - Conneally, Eibhlin

AU - Craddock, Charles

AU - Culligan, Dominic

AU - Dennis, Mike

AU - Duncan, Caroline

AU - Freeman, Sylvie D

AU - Furness, Caroline

AU - Gilkes, Amanda

AU - Gkreka, Paraskevi

AU - Hodgson, Katherine

AU - Ingram, Wendy

AU - Jain, Manish

AU - King, Andrew

AU - Knapper, Steven

AU - Kottaridis, Panagiotis

AU - McMullin, Mary Frances

AU - Mohite, Unmesh

AU - Ngu, Loretta

AU - O'Nions, Jenny

AU - Patrick, Katharine

AU - Rider, Tom

AU - Roberts, Wing

AU - Severinsen, Marianne Tang

AU - Storrar, Neill

AU - Taylor, Tom

AU - Russell, Nigel H

AU - Dillon, Richard

PY - 2023/8/9

Y1 - 2023/8/9

N2 - Patients with FLT3-mutated AML have a high relapse rate and suboptimal outcomes. Many have co-mutations suitable for measurable residual disease (MRD) monitoring by RT-qPCR and those destined to relapse can be identified by high or rising levels of MRD, called molecular failure. This provides a window for pre-emptive intervention, but there is little evidence to guide treatment. The use of FLT3 inhibitors (FLT3i) appears attractive but their use has not yet been evaluated. We identified 56 patients treated with FLT3i at molecular failure. The FLT3 mutation was an ITD in 52, TKD in 7 and both in 3. Over half of patients had previously received midostaurin. Molecular failure occurred at a median 9.2 months from diagnosis and was treated with gilteritinib (n = 38), quizartinib (n = 7) or sorafenib (n = 11). 60% achieved a molecular response, with 45% reaching MRD negativity. Haematological toxicity was low, and 22 patients were bridged directly to allogeneic transplant with another 6 to donor lymphocyte infusion. 2-year overall survival was 80% (95%CI 69-93) and molecular event-free survival 56% (95%CI 44-72). High-sensitivity next-generation sequencing for FLT3-ITD at molecular failure identified patients more likely to benefit. FLT3i monotherapy for molecular failure is a promising strategy which merits evaluation in prospective studies.

AB - Patients with FLT3-mutated AML have a high relapse rate and suboptimal outcomes. Many have co-mutations suitable for measurable residual disease (MRD) monitoring by RT-qPCR and those destined to relapse can be identified by high or rising levels of MRD, called molecular failure. This provides a window for pre-emptive intervention, but there is little evidence to guide treatment. The use of FLT3 inhibitors (FLT3i) appears attractive but their use has not yet been evaluated. We identified 56 patients treated with FLT3i at molecular failure. The FLT3 mutation was an ITD in 52, TKD in 7 and both in 3. Over half of patients had previously received midostaurin. Molecular failure occurred at a median 9.2 months from diagnosis and was treated with gilteritinib (n = 38), quizartinib (n = 7) or sorafenib (n = 11). 60% achieved a molecular response, with 45% reaching MRD negativity. Haematological toxicity was low, and 22 patients were bridged directly to allogeneic transplant with another 6 to donor lymphocyte infusion. 2-year overall survival was 80% (95%CI 69-93) and molecular event-free survival 56% (95%CI 44-72). High-sensitivity next-generation sequencing for FLT3-ITD at molecular failure identified patients more likely to benefit. FLT3i monotherapy for molecular failure is a promising strategy which merits evaluation in prospective studies.

U2 - 10.1038/s41375-023-01994-x

DO - 10.1038/s41375-023-01994-x

M3 - Article

C2 - 37558736

SN - 0887-6924

JO - Leukemia

JF - Leukemia

ER -

FLT3 inhibitors as MRD-guided salvage treatment for molecular failure in FLT3 mutated AML

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