Molecular classification and identification of an aggressive signature in low-grade B-cell lymphomas

Melissa A. Hopper; Kerstin Wenzl; Keenan T. Hartert; Jordan E. Krull; Abigail R. Dropik; Joseph P. Novak; Michelle K. Manske; Ma Kayla R. Serres; Vivekananda Sarangi; Melissa C. Larson; Matthew J. Maurer; Zhi Zhang Yang; Jonas Paludo; Ellen D. McPhail; Thomas M. Habermann; Brian K. Link; Lisa M. Rimsza; Stephen M. Ansell; James R. Cerhan; Dragan Jevremovic; Anne J. Novak

doi:10.1002/hon.3187

Molecular classification and identification of an aggressive signature in low-grade B-cell lymphomas

Melissa A. Hopper, Kerstin Wenzl, Keenan T. Hartert, Jordan E. Krull, Abigail R. Dropik, Joseph P. Novak, Michelle K. Manske, Ma Kayla R. Serres, Vivekananda Sarangi, Melissa C. Larson, Matthew J. Maurer, Zhi Zhang Yang, Jonas Paludo, Ellen D. McPhail, Thomas M. Habermann, Brian K. Link, Lisa M. Rimsza, Stephen M. Ansell, James R. Cerhan, Dragan JevremovicAnne J. Novak

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

Abstract

Non-follicular low-grade B-cell lymphomas (LGBCL) are biologically diverse entities that share clinical and histologic features that make definitive pathologic categorization challenging. While most patients with LGBCL have an indolent course, some experience aggressive disease, highlighting additional heterogeneity across these subtypes. To investigate the potential for shared biology across subtypes, we performed RNA sequencing and applied machine learning approaches that identified five clusters of patients that grouped independently of subtype. One cluster was characterized by inferior outcome, upregulation of cell cycle genes, and increased tumor immune cell content. Integration of whole exome sequencing identified novel LGBCL mutations and enrichment of TNFAIP3 and BCL2 alterations in the poor survival cluster. Building on this, we further refined a transcriptomic signature associated with early clinical failure in two independent cohorts. Taken together, this study identifies unique clusters of LGBCL defined by novel gene expression signatures and immune profiles associated with outcome across diagnostic subtypes.

Original language	English (US)
Pages (from-to)	644-654
Number of pages	11
Journal	Hematological Oncology
Volume	41
Issue number	4
DOIs	https://doi.org/10.1002/hon.3187
State	Published - Oct 2023

Keywords

genetics
immune
lymphoma
signatures
transcriptomics

ASJC Scopus subject areas

Hematology
Oncology
Cancer Research

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10.1002/hon.3187

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Hopper, M. A., Wenzl, K., Hartert, K. T., Krull, J. E., Dropik, A. R., Novak, J. P., Manske, M. K., Serres, M. K. R., Sarangi, V., Larson, M. C., Maurer, M. J., Yang, Z. Z., Paludo, J., McPhail, E. D., Habermann, T. M., Link, B. K., Rimsza, L. M., Ansell, S. M., Cerhan, J. R., ... Novak, A. J. (2023). Molecular classification and identification of an aggressive signature in low-grade B-cell lymphomas. Hematological Oncology, 41(4), 644-654. https://doi.org/10.1002/hon.3187

Hopper, MA, Wenzl, K, Hartert, KT, Krull, JE, Dropik, AR, Novak, JP, Manske, MK, Serres, MKR, Sarangi, V, Larson, MC, Maurer, MJ, Yang, ZZ, Paludo, J, McPhail, ED , Habermann, TM, Link, BK, Rimsza, LM , Ansell, SM , Cerhan, JR, Jevremovic, D & Novak, AJ 2023, 'Molecular classification and identification of an aggressive signature in low-grade B-cell lymphomas', Hematological Oncology, vol. 41, no. 4, pp. 644-654. https://doi.org/10.1002/hon.3187

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title = "Molecular classification and identification of an aggressive signature in low-grade B-cell lymphomas",

abstract = "Non-follicular low-grade B-cell lymphomas (LGBCL) are biologically diverse entities that share clinical and histologic features that make definitive pathologic categorization challenging. While most patients with LGBCL have an indolent course, some experience aggressive disease, highlighting additional heterogeneity across these subtypes. To investigate the potential for shared biology across subtypes, we performed RNA sequencing and applied machine learning approaches that identified five clusters of patients that grouped independently of subtype. One cluster was characterized by inferior outcome, upregulation of cell cycle genes, and increased tumor immune cell content. Integration of whole exome sequencing identified novel LGBCL mutations and enrichment of TNFAIP3 and BCL2 alterations in the poor survival cluster. Building on this, we further refined a transcriptomic signature associated with early clinical failure in two independent cohorts. Taken together, this study identifies unique clusters of LGBCL defined by novel gene expression signatures and immune profiles associated with outcome across diagnostic subtypes.",

keywords = "genetics, immune, lymphoma, signatures, transcriptomics",

author = "Hopper, {Melissa A.} and Kerstin Wenzl and Hartert, {Keenan T.} and Krull, {Jordan E.} and Dropik, {Abigail R.} and Novak, {Joseph P.} and Manske, {Michelle K.} and Serres, {Ma Kayla R.} and Vivekananda Sarangi and Larson, {Melissa C.} and Maurer, {Matthew J.} and Yang, {Zhi Zhang} and Jonas Paludo and McPhail, {Ellen D.} and Habermann, {Thomas M.} and Link, {Brian K.} and Rimsza, {Lisa M.} and Ansell, {Stephen M.} and Cerhan, {James R.} and Dragan Jevremovic and Novak, {Anne J.}",

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year = "2023",

month = oct,

doi = "10.1002/hon.3187",

language = "English (US)",

volume = "41",

pages = "644--654",

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AU - Hopper, Melissa A.

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AU - Dropik, Abigail R.

AU - Novak, Joseph P.

AU - Manske, Michelle K.

AU - Serres, Ma Kayla R.

AU - Sarangi, Vivekananda

AU - Larson, Melissa C.

AU - Maurer, Matthew J.

AU - Yang, Zhi Zhang

AU - Paludo, Jonas

AU - McPhail, Ellen D.

AU - Habermann, Thomas M.

AU - Link, Brian K.

AU - Rimsza, Lisa M.

AU - Ansell, Stephen M.

AU - Cerhan, James R.

AU - Jevremovic, Dragan

AU - Novak, Anne J.

PY - 2023/10

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N2 - Non-follicular low-grade B-cell lymphomas (LGBCL) are biologically diverse entities that share clinical and histologic features that make definitive pathologic categorization challenging. While most patients with LGBCL have an indolent course, some experience aggressive disease, highlighting additional heterogeneity across these subtypes. To investigate the potential for shared biology across subtypes, we performed RNA sequencing and applied machine learning approaches that identified five clusters of patients that grouped independently of subtype. One cluster was characterized by inferior outcome, upregulation of cell cycle genes, and increased tumor immune cell content. Integration of whole exome sequencing identified novel LGBCL mutations and enrichment of TNFAIP3 and BCL2 alterations in the poor survival cluster. Building on this, we further refined a transcriptomic signature associated with early clinical failure in two independent cohorts. Taken together, this study identifies unique clusters of LGBCL defined by novel gene expression signatures and immune profiles associated with outcome across diagnostic subtypes.

AB - Non-follicular low-grade B-cell lymphomas (LGBCL) are biologically diverse entities that share clinical and histologic features that make definitive pathologic categorization challenging. While most patients with LGBCL have an indolent course, some experience aggressive disease, highlighting additional heterogeneity across these subtypes. To investigate the potential for shared biology across subtypes, we performed RNA sequencing and applied machine learning approaches that identified five clusters of patients that grouped independently of subtype. One cluster was characterized by inferior outcome, upregulation of cell cycle genes, and increased tumor immune cell content. Integration of whole exome sequencing identified novel LGBCL mutations and enrichment of TNFAIP3 and BCL2 alterations in the poor survival cluster. Building on this, we further refined a transcriptomic signature associated with early clinical failure in two independent cohorts. Taken together, this study identifies unique clusters of LGBCL defined by novel gene expression signatures and immune profiles associated with outcome across diagnostic subtypes.

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KW - lymphoma

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Molecular classification and identification of an aggressive signature in low-grade B-cell lymphomas

Abstract

Keywords

ASJC Scopus subject areas

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