TP53 mutation variant allele frequency of ≥10% is associated with poor prognosis in therapy-related myeloid neoplasms

Mithun Vinod Shah; Elizabeth Ngoc Hoa Tran; Syed Shah; Rakchha Chhetri; Anmol Baranwal; Dariusz Ladon; Carl Shultz; Aref Al-Kali; Anna L. Brown; Dong Chen; Hamish S. Scott; Patricia Greipp; Daniel Thomas; Hassan B. Alkhateeb; Deepak Singhal; Naseema Gangat; Sharad Kumar; Mrinal M. Patnaik; Christopher N. Hahn; Chung Hoow Kok; Ayalew Tefferi; Devendra K. Hiwase

doi:10.1038/s41408-023-00821-x

TP53 mutation variant allele frequency of ≥10% is associated with poor prognosis in therapy-related myeloid neoplasms

Mithun Vinod Shah, Elizabeth Ngoc Hoa Tran, Syed Shah, Rakchha Chhetri, Anmol Baranwal, Dariusz Ladon, Carl Shultz, Aref Al-Kali, Anna L. Brown, Dong Chen, Hamish S. Scott, Patricia Greipp, Daniel Thomas, Hassan B. Alkhateeb, Deepak Singhal, Naseema Gangat, Sharad Kumar, Mrinal M. Patnaik, Christopher N. Hahn, Chung Hoow KokAyalew Tefferi, Devendra K. Hiwase

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

Abstract

Revised diagnostic criteria for myeloid neoplasms (MN) issued by the International Consensus Classification (ICC) and the World Health Organization (WHO) recommended major change pertaining to TP53-mutated (TP53^mut) MN. However, these assertions have not been specifically examined in therapy-related myeloid neoplasm (t-MN), a subset enriched with TP53^mut. We analyzed 488 t-MN patients for TP53^mut. At least one TP53^mut with variant allele frequency (VAF) ≥ 2% with or without loss of TP53 locus was noted in 182 (37.3%) patients and 88.2% of TP53^mut t-MN had a VAF ≥10%. TP53^mut t-MN with VAF ≥ 10% had a distinct clinical and biological profile compared to both TP53^mut VAF < 10% and wild-type TP53 (TP53^wt) cases. Notably, TP53^mut VAF ≥ 10% had a significantly shorter survival compared to TP53^wt (8.3 vs. 21.6 months; P < 0.001), while the survival of TP53^mut VAF < 10% was comparable to TP53^wt. Within TP53^mut VAF ≥ 10% cohort, the inferior outcomes persisted irrespective of the single- or multi-hit status, co-mutation pattern, or treatments received. Finally, survival of TP53^mut patients was poor across all the blast categories and MDS patients with >10% blasts had inferior survival compared to <5%. In summary, TP53^mut VAF ≥10% signified a clinically and molecularly homogenous cohort regardless of the allelic status.

Original language	English (US)
Article number	51
Journal	Blood cancer journal
Volume	13
Issue number	1
DOIs	https://doi.org/10.1038/s41408-023-00821-x
State	Published - Dec 2023

ASJC Scopus subject areas

Hematology
Oncology

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10.1038/s41408-023-00821-x

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Shah, M. V., Tran, E. N. H., Shah, S., Chhetri, R., Baranwal, A., Ladon, D., Shultz, C., Al-Kali, A., Brown, A. L., Chen, D., Scott, H. S., Greipp, P., Thomas, D., Alkhateeb, H. B., Singhal, D., Gangat, N., Kumar, S., Patnaik, M. M., Hahn, C. N., ... Hiwase, D. K. (2023). TP53 mutation variant allele frequency of ≥10% is associated with poor prognosis in therapy-related myeloid neoplasms. Blood cancer journal, 13(1), [51]. https://doi.org/10.1038/s41408-023-00821-x

Shah, MV, Tran, ENH, Shah, S, Chhetri, R, Baranwal, A, Ladon, D, Shultz, C, Al-Kali, A, Brown, AL, Chen, D, Scott, HS, Greipp, P, Thomas, D, Alkhateeb, HB, Singhal, D, Gangat, N, Kumar, S, Patnaik, MM, Hahn, CN, Kok, CH, Tefferi, A & Hiwase, DK 2023, 'TP53 mutation variant allele frequency of ≥10% is associated with poor prognosis in therapy-related myeloid neoplasms', Blood cancer journal, vol. 13, no. 1, 51. https://doi.org/10.1038/s41408-023-00821-x

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title = "TP53 mutation variant allele frequency of ≥10% is associated with poor prognosis in therapy-related myeloid neoplasms",

abstract = "Revised diagnostic criteria for myeloid neoplasms (MN) issued by the International Consensus Classification (ICC) and the World Health Organization (WHO) recommended major change pertaining to TP53-mutated (TP53mut) MN. However, these assertions have not been specifically examined in therapy-related myeloid neoplasm (t-MN), a subset enriched with TP53mut. We analyzed 488 t-MN patients for TP53mut. At least one TP53mut with variant allele frequency (VAF) ≥ 2% with or without loss of TP53 locus was noted in 182 (37.3%) patients and 88.2% of TP53mut t-MN had a VAF ≥10%. TP53mut t-MN with VAF ≥ 10% had a distinct clinical and biological profile compared to both TP53mut VAF < 10% and wild-type TP53 (TP53wt) cases. Notably, TP53mut VAF ≥ 10% had a significantly shorter survival compared to TP53wt (8.3 vs. 21.6 months; P < 0.001), while the survival of TP53mut VAF < 10% was comparable to TP53wt. Within TP53mut VAF ≥ 10% cohort, the inferior outcomes persisted irrespective of the single- or multi-hit status, co-mutation pattern, or treatments received. Finally, survival of TP53mut patients was poor across all the blast categories and MDS patients with >10% blasts had inferior survival compared to <5%. In summary, TP53mut VAF ≥10% signified a clinically and molecularly homogenous cohort regardless of the allelic status.",

author = "Shah, {Mithun Vinod} and Tran, {Elizabeth Ngoc Hoa} and Syed Shah and Rakchha Chhetri and Anmol Baranwal and Dariusz Ladon and Carl Shultz and Aref Al-Kali and Brown, {Anna L.} and Dong Chen and Scott, {Hamish S.} and Patricia Greipp and Daniel Thomas and Alkhateeb, {Hassan B.} and Deepak Singhal and Naseema Gangat and Sharad Kumar and Patnaik, {Mrinal M.} and Hahn, {Christopher N.} and Kok, {Chung Hoow} and Ayalew Tefferi and Hiwase, {Devendra K.}",

note = "Funding Information: We are grateful to our patients, their families, Mayo Clinic Acute Leukemia and Myeloid Neoplasms Biobank, and South Australia Cancer Research Biobank (SACRB). Some of the data in this publication were produced in the Mayo Clinic Cytogenetics Core Laboratory, which in part, is supported by the Mayo Clinic Comprehensive Cancer Center Grant, funded by National Cancer Institute (P30CA15083). MVS was supported by Mayo Clinic Research Pipeline K2R Transition Award and Bridget Kiely Clinician Career Development in Transplant Research and Mayo Clinic, Rochester. SK was supported by a NHMRC Investigator Grant (GNT2007739). DT is supported by a CSL Centenary Fellowship, Medical Research Futures Fund, and Leukemia-Lymphoma Translational Research Program funding. DH was supported by a National Health and Medical Research Council (NHMRC)/Medical Research Future Fund (MRFF) Investigator Grant (MRF1195517), Cancer Australia, and Leukemia Foundation Australia. Funding Information: We are grateful to our patients, their families, Mayo Clinic Acute Leukemia and Myeloid Neoplasms Biobank, and South Australia Cancer Research Biobank (SACRB). Some of the data in this publication were produced in the Mayo Clinic Cytogenetics Core Laboratory, which in part, is supported by the Mayo Clinic Comprehensive Cancer Center Grant, funded by National Cancer Institute (P30CA15083). MVS was supported by Mayo Clinic Research Pipeline K2R Transition Award and Bridget Kiely Clinician Career Development in Transplant Research and Mayo Clinic, Rochester. SK was supported by a NHMRC Investigator Grant (GNT2007739). DT is supported by a CSL Centenary Fellowship, Medical Research Futures Fund, and Leukemia-Lymphoma Translational Research Program funding. DH was supported by a National Health and Medical Research Council (NHMRC)/Medical Research Future Fund (MRFF) Investigator Grant (MRF1195517), Cancer Australia, and Leukemia Foundation Australia. Publisher Copyright: {\textcopyright} 2023, Crown.",

year = "2023",

month = dec,

doi = "10.1038/s41408-023-00821-x",

language = "English (US)",

volume = "13",

journal = "Blood Cancer Journal",

issn = "2044-5385",

publisher = "Nature Publishing Group",

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TY - JOUR

T1 - TP53 mutation variant allele frequency of ≥10% is associated with poor prognosis in therapy-related myeloid neoplasms

AU - Shah, Mithun Vinod

AU - Tran, Elizabeth Ngoc Hoa

AU - Shah, Syed

AU - Chhetri, Rakchha

AU - Baranwal, Anmol

AU - Ladon, Dariusz

AU - Shultz, Carl

AU - Al-Kali, Aref

AU - Brown, Anna L.

AU - Chen, Dong

AU - Scott, Hamish S.

AU - Greipp, Patricia

AU - Thomas, Daniel

AU - Alkhateeb, Hassan B.

AU - Singhal, Deepak

AU - Gangat, Naseema

AU - Kumar, Sharad

AU - Patnaik, Mrinal M.

AU - Hahn, Christopher N.

AU - Kok, Chung Hoow

AU - Tefferi, Ayalew

AU - Hiwase, Devendra K.

N1 - Funding Information: We are grateful to our patients, their families, Mayo Clinic Acute Leukemia and Myeloid Neoplasms Biobank, and South Australia Cancer Research Biobank (SACRB). Some of the data in this publication were produced in the Mayo Clinic Cytogenetics Core Laboratory, which in part, is supported by the Mayo Clinic Comprehensive Cancer Center Grant, funded by National Cancer Institute (P30CA15083). MVS was supported by Mayo Clinic Research Pipeline K2R Transition Award and Bridget Kiely Clinician Career Development in Transplant Research and Mayo Clinic, Rochester. SK was supported by a NHMRC Investigator Grant (GNT2007739). DT is supported by a CSL Centenary Fellowship, Medical Research Futures Fund, and Leukemia-Lymphoma Translational Research Program funding. DH was supported by a National Health and Medical Research Council (NHMRC)/Medical Research Future Fund (MRFF) Investigator Grant (MRF1195517), Cancer Australia, and Leukemia Foundation Australia. Funding Information: We are grateful to our patients, their families, Mayo Clinic Acute Leukemia and Myeloid Neoplasms Biobank, and South Australia Cancer Research Biobank (SACRB). Some of the data in this publication were produced in the Mayo Clinic Cytogenetics Core Laboratory, which in part, is supported by the Mayo Clinic Comprehensive Cancer Center Grant, funded by National Cancer Institute (P30CA15083). MVS was supported by Mayo Clinic Research Pipeline K2R Transition Award and Bridget Kiely Clinician Career Development in Transplant Research and Mayo Clinic, Rochester. SK was supported by a NHMRC Investigator Grant (GNT2007739). DT is supported by a CSL Centenary Fellowship, Medical Research Futures Fund, and Leukemia-Lymphoma Translational Research Program funding. DH was supported by a National Health and Medical Research Council (NHMRC)/Medical Research Future Fund (MRFF) Investigator Grant (MRF1195517), Cancer Australia, and Leukemia Foundation Australia. Publisher Copyright: © 2023, Crown.

PY - 2023/12

Y1 - 2023/12

N2 - Revised diagnostic criteria for myeloid neoplasms (MN) issued by the International Consensus Classification (ICC) and the World Health Organization (WHO) recommended major change pertaining to TP53-mutated (TP53mut) MN. However, these assertions have not been specifically examined in therapy-related myeloid neoplasm (t-MN), a subset enriched with TP53mut. We analyzed 488 t-MN patients for TP53mut. At least one TP53mut with variant allele frequency (VAF) ≥ 2% with or without loss of TP53 locus was noted in 182 (37.3%) patients and 88.2% of TP53mut t-MN had a VAF ≥10%. TP53mut t-MN with VAF ≥ 10% had a distinct clinical and biological profile compared to both TP53mut VAF < 10% and wild-type TP53 (TP53wt) cases. Notably, TP53mut VAF ≥ 10% had a significantly shorter survival compared to TP53wt (8.3 vs. 21.6 months; P < 0.001), while the survival of TP53mut VAF < 10% was comparable to TP53wt. Within TP53mut VAF ≥ 10% cohort, the inferior outcomes persisted irrespective of the single- or multi-hit status, co-mutation pattern, or treatments received. Finally, survival of TP53mut patients was poor across all the blast categories and MDS patients with >10% blasts had inferior survival compared to <5%. In summary, TP53mut VAF ≥10% signified a clinically and molecularly homogenous cohort regardless of the allelic status.

AB - Revised diagnostic criteria for myeloid neoplasms (MN) issued by the International Consensus Classification (ICC) and the World Health Organization (WHO) recommended major change pertaining to TP53-mutated (TP53mut) MN. However, these assertions have not been specifically examined in therapy-related myeloid neoplasm (t-MN), a subset enriched with TP53mut. We analyzed 488 t-MN patients for TP53mut. At least one TP53mut with variant allele frequency (VAF) ≥ 2% with or without loss of TP53 locus was noted in 182 (37.3%) patients and 88.2% of TP53mut t-MN had a VAF ≥10%. TP53mut t-MN with VAF ≥ 10% had a distinct clinical and biological profile compared to both TP53mut VAF < 10% and wild-type TP53 (TP53wt) cases. Notably, TP53mut VAF ≥ 10% had a significantly shorter survival compared to TP53wt (8.3 vs. 21.6 months; P < 0.001), while the survival of TP53mut VAF < 10% was comparable to TP53wt. Within TP53mut VAF ≥ 10% cohort, the inferior outcomes persisted irrespective of the single- or multi-hit status, co-mutation pattern, or treatments received. Finally, survival of TP53mut patients was poor across all the blast categories and MDS patients with >10% blasts had inferior survival compared to <5%. In summary, TP53mut VAF ≥10% signified a clinically and molecularly homogenous cohort regardless of the allelic status.

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TP53 mutation variant allele frequency of ≥10% is associated with poor prognosis in therapy-related myeloid neoplasms

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