Clinical impact of NPM1-mutant molecular persistence after chemotherapy for acute myeloid leukemia

Ing S. Tiong; Richard Dillon; Adam Ivey; James A. Kuzich; Nisha Thiagarajah; Kirsty M. Sharplin; Chung Hoow Kok; Aditya Tedjaseputra; James P. Rowland; Carolyn S. Grove; Emad Abro; Jake Shortt; Devendra K. Hiwase; Ashish Bajel; Nicola E. Potter; Matthew L. Smith; Claire J. Hemmaway; Abin Thomas; Amanda F. Gilkes; Nigel H. Russell; Andrew H. Wei

doi:10.1182/bloodadvances.2021005455

Clinical impact of NPM1-mutant molecular persistence after chemotherapy for acute myeloid leukemia

Ing S. Tiong, Richard Dillon, Adam Ivey, James A. Kuzich, Nisha Thiagarajah, Kirsty M. Sharplin, Chung Hoow Kok, Aditya Tedjaseputra, James P. Rowland, Carolyn S. Grove, Emad Abro, Jake Shortt, Devendra K. Hiwase, Ashish Bajel, Nicola E. Potter, Matthew L. Smith, Claire J. Hemmaway, Abin Thomas, Amanda F. Gilkes, Nigel H. RussellAndrew H. Wei^*

^*Corresponding author for this work

Medical & Molecular Genetics

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

24 Citations (Scopus)

Abstract

Monitoring of NPM1 mutant (NPM1mut) measurable residual disease (MRD) in acute myeloid leukemia (AML) has an established role in patients who are treated with intensive chemotherapy. The European LeukemiaNet has defined molecular persistence at low copy number (MP-LCN) as an MRD transcript level ,1% to 2% with a ,1-log change between any 2 positive samples collected after the end of treatment (EOT). Because the clinical impact of MP-LCN is unknown, we sought to characterize outcomes in patients with persistent NPM1mut MRD after EOT and identify factors associated with disease progression. Consecutive patients with newly diagnosed NPM1mut AML who received $2 cycles of intensive chemotherapy were included if bone marrow was NPM1mut MRD positive at the EOT, and they were not transplanted in first complete remission. One hundred patients were followed for a median of 23.5 months; 42% remained free of progression at 1 year, either spontaneously achieving complete molecular remission (CRMRD2; 30%) or retaining a low-level NPM1mut transcript (12% for $12 months and 9% at last follow-up). Forty percent met the criteria for MP-LCN. Preemptive salvage therapy significantly prolonged relapse-free survival. Risk factors associated with disease progression were concurrent FLT3-internal tandem duplication at diagnosis and suboptimal MRD response (NPM1mut reduction ,4.4-log) at EOT.

Original language	English
Pages (from-to)	5107-5111
Number of pages	5
Journal	Blood Advances
Volume	5
DOIs	https://doi.org/10.1182/bloodadvances.2021005455
Publication status	Published - 14 Dec 2021

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Tiong, I. S., Dillon, R., Ivey, A., Kuzich, J. A., Thiagarajah, N., Sharplin, K. M., Kok, C. H., Tedjaseputra, A., Rowland, J. P., Grove, C. S., Abro, E., Shortt, J., Hiwase, D. K., Bajel, A., Potter, N. E., Smith, M. L., Hemmaway, C. J., Thomas, A., Gilkes, A. F., ... Wei, A. H. (2021). Clinical impact of NPM1-mutant molecular persistence after chemotherapy for acute myeloid leukemia. Blood Advances, 5, 5107-5111. https://doi.org/10.1182/bloodadvances.2021005455

@article{2dde994b2a4a44b2a95728b32626b8ed,

title = "Clinical impact of NPM1-mutant molecular persistence after chemotherapy for acute myeloid leukemia",

abstract = "Monitoring of NPM1 mutant (NPM1mut) measurable residual disease (MRD) in acute myeloid leukemia (AML) has an established role in patients who are treated with intensive chemotherapy. The European LeukemiaNet has defined molecular persistence at low copy number (MP-LCN) as an MRD transcript level ,1% to 2% with a ,1-log change between any 2 positive samples collected after the end of treatment (EOT). Because the clinical impact of MP-LCN is unknown, we sought to characterize outcomes in patients with persistent NPM1mut MRD after EOT and identify factors associated with disease progression. Consecutive patients with newly diagnosed NPM1mut AML who received $2 cycles of intensive chemotherapy were included if bone marrow was NPM1mut MRD positive at the EOT, and they were not transplanted in first complete remission. One hundred patients were followed for a median of 23.5 months; 42% remained free of progression at 1 year, either spontaneously achieving complete molecular remission (CRMRD2; 30%) or retaining a low-level NPM1mut transcript (12% for $12 months and 9% at last follow-up). Forty percent met the criteria for MP-LCN. Preemptive salvage therapy significantly prolonged relapse-free survival. Risk factors associated with disease progression were concurrent FLT3-internal tandem duplication at diagnosis and suboptimal MRD response (NPM1mut reduction ,4.4-log) at EOT.",

author = "Tiong, {Ing S.} and Richard Dillon and Adam Ivey and Kuzich, {James A.} and Nisha Thiagarajah and Sharplin, {Kirsty M.} and Kok, {Chung Hoow} and Aditya Tedjaseputra and Rowland, {James P.} and Grove, {Carolyn S.} and Emad Abro and Jake Shortt and Hiwase, {Devendra K.} and Ashish Bajel and Potter, {Nicola E.} and Smith, {Matthew L.} and Hemmaway, {Claire J.} and Abin Thomas and Gilkes, {Amanda F.} and Russell, {Nigel H.} and Wei, {Andrew H.}",

year = "2021",

month = dec,

day = "14",

doi = "10.1182/bloodadvances.2021005455",

language = "English",

volume = "5",

pages = "5107--5111",

journal = "Blood Advances",

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publisher = "American Society of Hematology",

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Tiong, IS, Dillon, R , Ivey, A, Kuzich, JA, Thiagarajah, N, Sharplin, KM, Kok, CH, Tedjaseputra, A, Rowland, JP, Grove, CS, Abro, E, Shortt, J, Hiwase, DK, Bajel, A, Potter, NE, Smith, ML, Hemmaway, CJ, Thomas, A, Gilkes, AF, Russell, NH & Wei, AH 2021, 'Clinical impact of NPM1-mutant molecular persistence after chemotherapy for acute myeloid leukemia', Blood Advances, vol. 5, pp. 5107-5111. https://doi.org/10.1182/bloodadvances.2021005455

TY - JOUR

T1 - Clinical impact of NPM1-mutant molecular persistence after chemotherapy for acute myeloid leukemia

AU - Tiong, Ing S.

AU - Dillon, Richard

AU - Ivey, Adam

AU - Kuzich, James A.

AU - Thiagarajah, Nisha

AU - Sharplin, Kirsty M.

AU - Kok, Chung Hoow

AU - Tedjaseputra, Aditya

AU - Rowland, James P.

AU - Grove, Carolyn S.

AU - Abro, Emad

AU - Shortt, Jake

AU - Hiwase, Devendra K.

AU - Bajel, Ashish

AU - Potter, Nicola E.

AU - Smith, Matthew L.

AU - Hemmaway, Claire J.

AU - Thomas, Abin

AU - Gilkes, Amanda F.

AU - Russell, Nigel H.

AU - Wei, Andrew H.

PY - 2021/12/14

Y1 - 2021/12/14

N2 - Monitoring of NPM1 mutant (NPM1mut) measurable residual disease (MRD) in acute myeloid leukemia (AML) has an established role in patients who are treated with intensive chemotherapy. The European LeukemiaNet has defined molecular persistence at low copy number (MP-LCN) as an MRD transcript level ,1% to 2% with a ,1-log change between any 2 positive samples collected after the end of treatment (EOT). Because the clinical impact of MP-LCN is unknown, we sought to characterize outcomes in patients with persistent NPM1mut MRD after EOT and identify factors associated with disease progression. Consecutive patients with newly diagnosed NPM1mut AML who received $2 cycles of intensive chemotherapy were included if bone marrow was NPM1mut MRD positive at the EOT, and they were not transplanted in first complete remission. One hundred patients were followed for a median of 23.5 months; 42% remained free of progression at 1 year, either spontaneously achieving complete molecular remission (CRMRD2; 30%) or retaining a low-level NPM1mut transcript (12% for $12 months and 9% at last follow-up). Forty percent met the criteria for MP-LCN. Preemptive salvage therapy significantly prolonged relapse-free survival. Risk factors associated with disease progression were concurrent FLT3-internal tandem duplication at diagnosis and suboptimal MRD response (NPM1mut reduction ,4.4-log) at EOT.

AB - Monitoring of NPM1 mutant (NPM1mut) measurable residual disease (MRD) in acute myeloid leukemia (AML) has an established role in patients who are treated with intensive chemotherapy. The European LeukemiaNet has defined molecular persistence at low copy number (MP-LCN) as an MRD transcript level ,1% to 2% with a ,1-log change between any 2 positive samples collected after the end of treatment (EOT). Because the clinical impact of MP-LCN is unknown, we sought to characterize outcomes in patients with persistent NPM1mut MRD after EOT and identify factors associated with disease progression. Consecutive patients with newly diagnosed NPM1mut AML who received $2 cycles of intensive chemotherapy were included if bone marrow was NPM1mut MRD positive at the EOT, and they were not transplanted in first complete remission. One hundred patients were followed for a median of 23.5 months; 42% remained free of progression at 1 year, either spontaneously achieving complete molecular remission (CRMRD2; 30%) or retaining a low-level NPM1mut transcript (12% for $12 months and 9% at last follow-up). Forty percent met the criteria for MP-LCN. Preemptive salvage therapy significantly prolonged relapse-free survival. Risk factors associated with disease progression were concurrent FLT3-internal tandem duplication at diagnosis and suboptimal MRD response (NPM1mut reduction ,4.4-log) at EOT.

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U2 - 10.1182/bloodadvances.2021005455

DO - 10.1182/bloodadvances.2021005455

M3 - Article

C2 - 34555849

AN - SCOPUS:85121721973

SN - 2473-9529

VL - 5

SP - 5107

EP - 5111

JO - Blood Advances

JF - Blood Advances

ER -

Clinical impact of NPM1-mutant molecular persistence after chemotherapy for acute myeloid leukemia

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