Longitudinal expression profiling identifies a poor risk subset of patients with ABC-type diffuse large B-cell lymphoma

Findlay Bewicke-Copley; Koorosh Korfi; Shamzah Araf; Brendan Hodkinson; Emil Kumar; Thomas Cummin; Margaret Ashton-Key; Sharon Barrans; Suzan van Hoppe; Cathy Burton; Mohamed Elshiekh; Simon Rule; Nicola Crosbie; Andrew Clear; Maria Calaminici; Hendrik Runge; Robert K. Hills; David W. Scott; Lisa M. Rimsza; Geetha Menon; Chulin Sha; John R. Davies; Ai Nagano; Andrew Davies; Daniel Painter; Alexandra Smith; John Gribben; Kikkeri N. Naresh; David R. Westhead; Jessica Okosun; Andrew Steele; Daniel J. Hodson; Sriram Balasubramanian; Peter Johnson; Jun Wang; Jude Fitzgibbon

doi:10.1182/bloodadvances.2022007536

Longitudinal expression profiling identifies a poor risk subset of patients with ABC-type diffuse large B-cell lymphoma

Findlay Bewicke-Copley, Koorosh Korfi, Shamzah Araf, Brendan Hodkinson, Emil Kumar, Thomas Cummin, Margaret Ashton-Key, Sharon Barrans, Suzan van Hoppe, Cathy Burton, Mohamed Elshiekh, Simon Rule, Nicola Crosbie, Andrew Clear, Maria Calaminici, Hendrik Runge, Robert K. Hills, David W. Scott, Lisa M. Rimsza, Geetha MenonChulin Sha, John R. Davies, Ai Nagano, Andrew Davies, Daniel Painter, Alexandra Smith, John Gribben, Kikkeri N. Naresh, David R. Westhead, Jessica Okosun, Andrew Steele, Daniel J. Hodson, Sriram Balasubramanian, Peter Johnson, Jun Wang, Jude Fitzgibbon

Laboratory Medicine and Pathology

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

Abstract

Despite the effectiveness of immuno-chemotherapy, 40% of patients with diffuse large B-cell lymphoma (DLBCL) experience relapse or refractory disease. Longitudinal studies have previously focused on the mutational landscape of relapse but fell short of providing a consistent relapse-specific genetic signature. In our study, we have focused attention on the changes in GEP accompanying DLBCL relapse using archival paired diagnostic/relapse specimens from 38 de novo patients with DLBCL. COO remained stable from diagnosis to relapse in 80% of patients, with only a single patient showing COO switching from activated B-cell–like (ABC) to germinal center B-cell–like (GCB). Analysis of the transcriptomic changes that occur following relapse suggest ABC and GCB relapses are mediated via different mechanisms. We developed a 30-gene discriminator for ABC–DLBCLs derived from relapse-associated genes that defined clinically distinct high- and low-risk subgroups in ABC–DLBCLs at diagnosis in datasets comprising both population-based and clinical trial cohorts. This signature also identified a population of <60-year–old patients with superior PFS and OS treated with ibrutinib–R-CHOP as part of the PHOENIX trial. Altogether this new signature adds to the existing toolkit of putative genetic predictors now available in DLBCL that can be readily assessed as part of prospective clinical trials.

Original language	English (US)
Pages (from-to)	845-855
Number of pages	11
Journal	Blood Advances
Volume	7
Issue number	5
DOIs	https://doi.org/10.1182/bloodadvances.2022007536
State	Published - Mar 14 2023

ASJC Scopus subject areas

Hematology

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10.1182/bloodadvances.2022007536

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Bewicke-Copley, F., Korfi, K., Araf, S., Hodkinson, B., Kumar, E., Cummin, T., Ashton-Key, M., Barrans, S., van Hoppe, S., Burton, C., Elshiekh, M., Rule, S., Crosbie, N., Clear, A., Calaminici, M., Runge, H., Hills, R. K., Scott, D. W., Rimsza, L. M., ... Fitzgibbon, J. (2023). Longitudinal expression profiling identifies a poor risk subset of patients with ABC-type diffuse large B-cell lymphoma. Blood Advances, 7(5), 845-855. https://doi.org/10.1182/bloodadvances.2022007536

Bewicke-Copley, F, Korfi, K, Araf, S, Hodkinson, B, Kumar, E, Cummin, T, Ashton-Key, M, Barrans, S, van Hoppe, S, Burton, C, Elshiekh, M, Rule, S, Crosbie, N, Clear, A, Calaminici, M, Runge, H, Hills, RK, Scott, DW, Rimsza, LM, Menon, G, Sha, C, Davies, JR, Nagano, A, Davies, A, Painter, D, Smith, A, Gribben, J, Naresh, KN, Westhead, DR, Okosun, J, Steele, A, Hodson, DJ, Balasubramanian, S, Johnson, P, Wang, J & Fitzgibbon, J 2023, 'Longitudinal expression profiling identifies a poor risk subset of patients with ABC-type diffuse large B-cell lymphoma', Blood Advances, vol. 7, no. 5, pp. 845-855. https://doi.org/10.1182/bloodadvances.2022007536

@article{b8227891cfe846368632701d0f8e299b,

title = "Longitudinal expression profiling identifies a poor risk subset of patients with ABC-type diffuse large B-cell lymphoma",

abstract = "Despite the effectiveness of immuno-chemotherapy, 40% of patients with diffuse large B-cell lymphoma (DLBCL) experience relapse or refractory disease. Longitudinal studies have previously focused on the mutational landscape of relapse but fell short of providing a consistent relapse-specific genetic signature. In our study, we have focused attention on the changes in GEP accompanying DLBCL relapse using archival paired diagnostic/relapse specimens from 38 de novo patients with DLBCL. COO remained stable from diagnosis to relapse in 80% of patients, with only a single patient showing COO switching from activated B-cell–like (ABC) to germinal center B-cell–like (GCB). Analysis of the transcriptomic changes that occur following relapse suggest ABC and GCB relapses are mediated via different mechanisms. We developed a 30-gene discriminator for ABC–DLBCLs derived from relapse-associated genes that defined clinically distinct high- and low-risk subgroups in ABC–DLBCLs at diagnosis in datasets comprising both population-based and clinical trial cohorts. This signature also identified a population of <60-year–old patients with superior PFS and OS treated with ibrutinib–R-CHOP as part of the PHOENIX trial. Altogether this new signature adds to the existing toolkit of putative genetic predictors now available in DLBCL that can be readily assessed as part of prospective clinical trials.",

author = "Findlay Bewicke-Copley and Koorosh Korfi and Shamzah Araf and Brendan Hodkinson and Emil Kumar and Thomas Cummin and Margaret Ashton-Key and Sharon Barrans and {van Hoppe}, Suzan and Cathy Burton and Mohamed Elshiekh and Simon Rule and Nicola Crosbie and Andrew Clear and Maria Calaminici and Hendrik Runge and Hills, {Robert K.} and Scott, {David W.} and Rimsza, {Lisa M.} and Geetha Menon and Chulin Sha and Davies, {John R.} and Ai Nagano and Andrew Davies and Daniel Painter and Alexandra Smith and John Gribben and Naresh, {Kikkeri N.} and Westhead, {David R.} and Jessica Okosun and Andrew Steele and Hodson, {Daniel J.} and Sriram Balasubramanian and Peter Johnson and Jun Wang and Jude Fitzgibbon",

note = "Publisher Copyright: {\textcopyright} 2023 by The American Society of Hematology.",

year = "2023",

month = mar,

day = "14",

doi = "10.1182/bloodadvances.2022007536",

language = "English (US)",

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T1 - Longitudinal expression profiling identifies a poor risk subset of patients with ABC-type diffuse large B-cell lymphoma

AU - Bewicke-Copley, Findlay

AU - Korfi, Koorosh

AU - Araf, Shamzah

AU - Hodkinson, Brendan

AU - Kumar, Emil

AU - Cummin, Thomas

AU - Ashton-Key, Margaret

AU - Barrans, Sharon

AU - van Hoppe, Suzan

AU - Burton, Cathy

AU - Elshiekh, Mohamed

AU - Rule, Simon

AU - Crosbie, Nicola

AU - Clear, Andrew

AU - Calaminici, Maria

AU - Runge, Hendrik

AU - Hills, Robert K.

AU - Scott, David W.

AU - Rimsza, Lisa M.

AU - Menon, Geetha

AU - Sha, Chulin

AU - Davies, John R.

AU - Nagano, Ai

AU - Davies, Andrew

AU - Painter, Daniel

AU - Smith, Alexandra

AU - Gribben, John

AU - Naresh, Kikkeri N.

AU - Westhead, David R.

AU - Okosun, Jessica

AU - Steele, Andrew

AU - Hodson, Daniel J.

AU - Balasubramanian, Sriram

AU - Johnson, Peter

AU - Wang, Jun

AU - Fitzgibbon, Jude

PY - 2023/3/14

Y1 - 2023/3/14

N2 - Despite the effectiveness of immuno-chemotherapy, 40% of patients with diffuse large B-cell lymphoma (DLBCL) experience relapse or refractory disease. Longitudinal studies have previously focused on the mutational landscape of relapse but fell short of providing a consistent relapse-specific genetic signature. In our study, we have focused attention on the changes in GEP accompanying DLBCL relapse using archival paired diagnostic/relapse specimens from 38 de novo patients with DLBCL. COO remained stable from diagnosis to relapse in 80% of patients, with only a single patient showing COO switching from activated B-cell–like (ABC) to germinal center B-cell–like (GCB). Analysis of the transcriptomic changes that occur following relapse suggest ABC and GCB relapses are mediated via different mechanisms. We developed a 30-gene discriminator for ABC–DLBCLs derived from relapse-associated genes that defined clinically distinct high- and low-risk subgroups in ABC–DLBCLs at diagnosis in datasets comprising both population-based and clinical trial cohorts. This signature also identified a population of <60-year–old patients with superior PFS and OS treated with ibrutinib–R-CHOP as part of the PHOENIX trial. Altogether this new signature adds to the existing toolkit of putative genetic predictors now available in DLBCL that can be readily assessed as part of prospective clinical trials.

AB - Despite the effectiveness of immuno-chemotherapy, 40% of patients with diffuse large B-cell lymphoma (DLBCL) experience relapse or refractory disease. Longitudinal studies have previously focused on the mutational landscape of relapse but fell short of providing a consistent relapse-specific genetic signature. In our study, we have focused attention on the changes in GEP accompanying DLBCL relapse using archival paired diagnostic/relapse specimens from 38 de novo patients with DLBCL. COO remained stable from diagnosis to relapse in 80% of patients, with only a single patient showing COO switching from activated B-cell–like (ABC) to germinal center B-cell–like (GCB). Analysis of the transcriptomic changes that occur following relapse suggest ABC and GCB relapses are mediated via different mechanisms. We developed a 30-gene discriminator for ABC–DLBCLs derived from relapse-associated genes that defined clinically distinct high- and low-risk subgroups in ABC–DLBCLs at diagnosis in datasets comprising both population-based and clinical trial cohorts. This signature also identified a population of <60-year–old patients with superior PFS and OS treated with ibrutinib–R-CHOP as part of the PHOENIX trial. Altogether this new signature adds to the existing toolkit of putative genetic predictors now available in DLBCL that can be readily assessed as part of prospective clinical trials.

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Longitudinal expression profiling identifies a poor risk subset of patients with ABC-type diffuse large B-cell lymphoma

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