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

被引：26

作者：

Othman, Jad ^{[1
,2
,3
]}

Potter, Nicola ^{[1
]}

Mokretar, Katya ^{[4
]}

Taussig, David ^{[5
]}

Khan, Anjum ^{[6
]}

Krishnamurthy, Pramila ^{[7
]}

Latif, Anne-Louise ^{[8
]}

Cahalin, Paul ^{[9
]}

Aries, James ^{[10
]}

Amer, Mariam ^{[11
]}

Belsham, Edward ^{[12
]}

Conneally, Eibhlin ^{[13
]}

Craddock, Charles ^{[14
]}

Culligan, Dominic ^{[15
]}

Dennis, Mike ^{[16
]}

Duncan, Caroline ^{[17
]}

Freeman, Sylvie D. ^{[18
]}

Furness, Caroline ^{[5
]}

Gilkes, Amanda ^{[19
]}

Gkreka, Paraskevi ^{[20
]}

Hodgson, Katherine ^{[21
]}

Ingram, Wendy ^{[22
]}

Jain, Manish ^{[6
]}

King, Andrew ^{[23
]}

Knapper, Steven ^{[24
]}

Kottaridis, Panagiotis ^{[25
]}

McMullin, Mary Frances ^{[26
]}

Mohite, Unmesh ^{[27
]}

Ngu, Loretta ^{[28
]}

O'Nions, Jenny ^{[25
,29
]}

Patrick, Katharine

Rider, Tom ^{[30
,31
]}

Roberts, Wing ^{[32
]}

Severinsen, Marianne Tang ^{[33
]}

Storrar, Neill ^{[34
]}

Taylor, Tom ^{[35
]}

Russell, Nigel H. ^{[2
]}

Dillon, Richard ^{[1
,2
]}

机构：

[1] Kings Coll London, Dept Med & Mol Genet, London, England

[2] Guys & St ThomasNHS Fdn Trust, London, England

[3] Univ Sydney, Fac Med & Hlth, Sydney, NSW, Australia

[4] Synnovis, Canc Genet, London, England

[5] Royal Marsden NHS Fdn Trust, London, England

[6] Leeds Teaching Hosp NHS Trust, Leeds, England

[7] Kings Coll Hosp London, London, England

[8] Queen Elizabeth Univ Hosp, Glasgow, Scotland

[9] Blackpool Teaching Hosp NHS Fdn Trust, Blackpool, England

[10] Queen Mary Univ London, Barts Canc Inst, London, England

[11] Univ Hosp Southampton, Southampton, England

[12] Portsmouth Hosp NHS Trust, Portsmouth, England

[13] St James Hosp, Dublin, Ireland

[14] Univ Hosp Birmingham, Birmingham, England

[15] Aberdeen Royal Infirm, Aberdeen, Scotland

[16] Christie NHS Fdn Trust, Manchester, England

[17] Raigmore Hosp, Inverness, Scotland

[18] Univ Birmingham, Inst Immunol & Immunotherapy, Birmingham, Scotland

[19] Cardiff Univ, Dept Haematol, Cardiff, Wales

[20] Princess Royal Univ Hosp, London, England

[21] Univ Hosp Leicester, Leicester, England

[22] Univ Hosp Wales, Cardiff, Wales

[23] Addenbrookes Hosp, Cambridge, England

[24] Cardiff Univ, Sch Med, Cardiff, Wales

[25] Univ Coll London Hosp NHS Fdn Trust, London, England

[26] Queens Univ, Belfast, North Ireland

[27] Singleton Hosp, Sketty, Wales

[28] Royal Devon & Exeter NHS Fdn Trust, Exeter, England

[29] Sheffield Childrens NHS Fdn Trust, Sheffield, England

[30] Royal Sussex Cty Hosp, Brighton, England

[31] Royal Sussex Cty Hosp, Hove, England

[32] Great North Childrens Hosp, Newcastle Upon Tyne, England

[33] Aalborg Univ Hosp, Clin Canc Res Ctr, Dept Hematol, Aalborg, Denmark

[34] NHS Lothian, Edinburgh, Scotland

[35] Nottingham Univ Hosp, Nottingham, England

来源：

LEUKEMIA | 2023年 / 37卷 / 10期

关键词：

ACUTE MYELOID-LEUKEMIA; INTERNAL TANDEM DUPLICATION; MINIMAL RESIDUAL DISEASE; RELAPSE; CHEMOTHERAPY; TRANSPLANTATION; VENETOCLAX; IMPACT;

D O I：

10.1038/s41375-023-01994-x

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

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.

引用

页码：2066 / 2072

页数：7

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