DNMT3A mutations define a unique biological and prognostic subgroup associated with cytotoxic T cells in PTCL-NOS

Tyler A. Herek; Alyssa Bouska; Waseem Lone; Sunandini Sharma; Catalina Amador; Tayla B. Heavican; Yuping Li; Qi Wei; Dylan Jochum; Timothy C. Greiner; Lynette Smith; Stefano Pileri; Andrew L. Feldman; Andreas Rosenwald; German Ott; Soon Thye Lim; Choon Kiat Ong; Joo Song; Elaine S. Jaffe; Gang Greg Wang; Louis Staudt; Lisa M. Rimsza; Julie Vose; Francesco d'Amore; Dennis D. Weisenburger; Wing C. Chan; Javeed Iqbal

doi:10.1182/blood.2021015019

DNMT3A mutations define a unique biological and prognostic subgroup associated with cytotoxic T cells in PTCL-NOS

Tyler A. Herek
, Alyssa Bouska
, Waseem Lone
, Sunandini Sharma
, Catalina Amador
, Tayla B. Heavican
, Yuping Li
, Qi Wei
, Dylan Jochum
, Timothy C. Greiner
, Lynette Smith
, Stefano Pileri
, Andrew L. Feldman
, Andreas Rosenwald
, German Ott
, Soon Thye Lim
, Choon Kiat Ong
, Joo Song
, Elaine S. Jaffe
, Gang Greg Wang

Louis Staudt, Lisa M. Rimsza, Julie Vose, Francesco d'Amore, Dennis D. Weisenburger, Wing C. Chan, Javeed Iqbal

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

38 Scopus citations

Abstract

Peripheral T-cell lymphomas (PTCLs) are heterogenous T-cell neoplasms often associated with epigenetic dysregulation. We investigated de novo DNA methyltransferase 3A (DNMT3A) mutations in common PTCL entities, including angioimmunoblastic T-cell lymphoma and novel molecular subtypes identified within PTCL–not otherwise specified (PTCL-NOS) designated as PTCL-GATA3 and PTCL-TBX21. DNMT3A-mutated PTCL-TBX21 cases showed inferior overall survival (OS), with DNMT3A-mutated residues skewed toward the methyltransferase domain and dimerization motif (S881–R887). Transcriptional profiling demonstrated significant enrichment of activated CD8⁺ T-cell cytotoxic gene signatures in the DNMT3A-mutant PTCL-TBX21 cases, which was further validated using immunohistochemistry. Genomewide methylation analysis of DNMT3A-mutant vs wild-type (WT) PTCL-TBX21 cases demonstrated hypomethylation in target genes regulating interferon-γ (IFN-γ), T-cell receptor signaling, and EOMES (eomesodermin), a master transcriptional regulator of cytotoxic effector cells. Similar findings were observed in a murine model of PTCL with Dnmt3a loss (in vivo) and further validated in vitro by ectopic expression of DNMT3A mutants (DNMT3A-R882, -Q886, and -V716, vs WT) in CD8⁺ T-cell line, resulting in T-cell activation and EOMES upregulation. Furthermore, stable, ectopic expression of the DNMT3A mutants in primary CD3⁺ T-cell cultures resulted in the preferential outgrowth of CD8⁺ T cells with DNMT3A^R882H mutation. Single-cell RNA sequencing(RNA-seq) analysis of CD3⁺ T cells revealed differential CD8+ T-cell subset polarization, mirroring findings in DNMT3A-mutated PTCL-TBX21 and validating the cytotoxic and T-cell memory transcriptional programs associated with the DNMT3A^R882H mutation. Our findings indicate that DNMT3A mutations define a cytotoxic subset in PTCL-TBX21 with prognostic significance and thus may further refine pathological heterogeneity in PTCL-NOS and suggest alternative treatment strategies for this subset.

Original language	English (US)
Pages (from-to)	1278-1290
Number of pages	13
Journal	Blood
Volume	140
Issue number	11
DOIs	https://doi.org/10.1182/blood.2021015019
State	Published - Sep 15 2022
Externally published	Yes

ASJC Scopus subject areas

Biochemistry
Immunology
Hematology
Cell Biology

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10.1182/blood.2021015019

Cite this

Herek, T. A., Bouska, A., Lone, W., Sharma, S., Amador, C., Heavican, T. B., Li, Y., Wei, Q., Jochum, D., Greiner, T. C., Smith, L., Pileri, S., Feldman, A. L., Rosenwald, A., Ott, G., Lim, S. T., Ong, C. K., Song, J., Jaffe, E. S., ... Iqbal, J. (2022). DNMT3A mutations define a unique biological and prognostic subgroup associated with cytotoxic T cells in PTCL-NOS. Blood, 140(11), 1278-1290. https://doi.org/10.1182/blood.2021015019

Herek, TA, Bouska, A, Lone, W, Sharma, S, Amador, C, Heavican, TB, Li, Y, Wei, Q, Jochum, D, Greiner, TC, Smith, L, Pileri, S, Feldman, AL, Rosenwald, A, Ott, G, Lim, ST, Ong, CK, Song, J, Jaffe, ES, Wang, GG, Staudt, L, Rimsza, LM, Vose, J, d'Amore, F, Weisenburger, DD, Chan, WC & Iqbal, J 2022, 'DNMT3A mutations define a unique biological and prognostic subgroup associated with cytotoxic T cells in PTCL-NOS', Blood, vol. 140, no. 11, pp. 1278-1290. https://doi.org/10.1182/blood.2021015019

@article{a363e9c4e14f4f85b90ea0edc480f6a3,

title = "DNMT3A mutations define a unique biological and prognostic subgroup associated with cytotoxic T cells in PTCL-NOS",

abstract = "Peripheral T-cell lymphomas (PTCLs) are heterogenous T-cell neoplasms often associated with epigenetic dysregulation. We investigated de novo DNA methyltransferase 3A (DNMT3A) mutations in common PTCL entities, including angioimmunoblastic T-cell lymphoma and novel molecular subtypes identified within PTCL–not otherwise specified (PTCL-NOS) designated as PTCL-GATA3 and PTCL-TBX21. DNMT3A-mutated PTCL-TBX21 cases showed inferior overall survival (OS), with DNMT3A-mutated residues skewed toward the methyltransferase domain and dimerization motif (S881–R887). Transcriptional profiling demonstrated significant enrichment of activated CD8+ T-cell cytotoxic gene signatures in the DNMT3A-mutant PTCL-TBX21 cases, which was further validated using immunohistochemistry. Genomewide methylation analysis of DNMT3A-mutant vs wild-type (WT) PTCL-TBX21 cases demonstrated hypomethylation in target genes regulating interferon-γ (IFN-γ), T-cell receptor signaling, and EOMES (eomesodermin), a master transcriptional regulator of cytotoxic effector cells. Similar findings were observed in a murine model of PTCL with Dnmt3a loss (in vivo) and further validated in vitro by ectopic expression of DNMT3A mutants (DNMT3A-R882, -Q886, and -V716, vs WT) in CD8+ T-cell line, resulting in T-cell activation and EOMES upregulation. Furthermore, stable, ectopic expression of the DNMT3A mutants in primary CD3+ T-cell cultures resulted in the preferential outgrowth of CD8+ T cells with DNMT3AR882H mutation. Single-cell RNA sequencing(RNA-seq) analysis of CD3+ T cells revealed differential CD8+ T-cell subset polarization, mirroring findings in DNMT3A-mutated PTCL-TBX21 and validating the cytotoxic and T-cell memory transcriptional programs associated with the DNMT3AR882H mutation. Our findings indicate that DNMT3A mutations define a cytotoxic subset in PTCL-TBX21 with prognostic significance and thus may further refine pathological heterogeneity in PTCL-NOS and suggest alternative treatment strategies for this subset.",

author = "Herek, \{Tyler A.\} and Alyssa Bouska and Waseem Lone and Sunandini Sharma and Catalina Amador and Heavican, \{Tayla B.\} and Yuping Li and Qi Wei and Dylan Jochum and Greiner, \{Timothy C.\} and Lynette Smith and Stefano Pileri and Feldman, \{Andrew L.\} and Andreas Rosenwald and German Ott and Lim, \{Soon Thye\} and Ong, \{Choon Kiat\} and Joo Song and Jaffe, \{Elaine S.\} and Wang, \{Gang Greg\} and Louis Staudt and Rimsza, \{Lisa M.\} and Julie Vose and Francesco d'Amore and Weisenburger, \{Dennis D.\} and Chan, \{Wing C.\} and Javeed Iqbal",

note = "Publisher Copyright: {\textcopyright} 2022 American Society of Hematology",

year = "2022",

month = sep,

day = "15",

doi = "10.1182/blood.2021015019",

language = "English (US)",

volume = "140",

pages = "1278--1290",

journal = "Blood",

issn = "0006-4971",

publisher = "Elsevier B.V.",

number = "11",

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TY - JOUR

T1 - DNMT3A mutations define a unique biological and prognostic subgroup associated with cytotoxic T cells in PTCL-NOS

AU - Herek, Tyler A.

AU - Bouska, Alyssa

AU - Lone, Waseem

AU - Sharma, Sunandini

AU - Amador, Catalina

AU - Heavican, Tayla B.

AU - Li, Yuping

AU - Wei, Qi

AU - Jochum, Dylan

AU - Greiner, Timothy C.

AU - Smith, Lynette

AU - Pileri, Stefano

AU - Feldman, Andrew L.

AU - Rosenwald, Andreas

AU - Ott, German

AU - Lim, Soon Thye

AU - Ong, Choon Kiat

AU - Song, Joo

AU - Jaffe, Elaine S.

AU - Wang, Gang Greg

AU - Staudt, Louis

AU - Rimsza, Lisa M.

AU - Vose, Julie

AU - d'Amore, Francesco

AU - Weisenburger, Dennis D.

AU - Chan, Wing C.

AU - Iqbal, Javeed

PY - 2022/9/15

Y1 - 2022/9/15

N2 - Peripheral T-cell lymphomas (PTCLs) are heterogenous T-cell neoplasms often associated with epigenetic dysregulation. We investigated de novo DNA methyltransferase 3A (DNMT3A) mutations in common PTCL entities, including angioimmunoblastic T-cell lymphoma and novel molecular subtypes identified within PTCL–not otherwise specified (PTCL-NOS) designated as PTCL-GATA3 and PTCL-TBX21. DNMT3A-mutated PTCL-TBX21 cases showed inferior overall survival (OS), with DNMT3A-mutated residues skewed toward the methyltransferase domain and dimerization motif (S881–R887). Transcriptional profiling demonstrated significant enrichment of activated CD8+ T-cell cytotoxic gene signatures in the DNMT3A-mutant PTCL-TBX21 cases, which was further validated using immunohistochemistry. Genomewide methylation analysis of DNMT3A-mutant vs wild-type (WT) PTCL-TBX21 cases demonstrated hypomethylation in target genes regulating interferon-γ (IFN-γ), T-cell receptor signaling, and EOMES (eomesodermin), a master transcriptional regulator of cytotoxic effector cells. Similar findings were observed in a murine model of PTCL with Dnmt3a loss (in vivo) and further validated in vitro by ectopic expression of DNMT3A mutants (DNMT3A-R882, -Q886, and -V716, vs WT) in CD8+ T-cell line, resulting in T-cell activation and EOMES upregulation. Furthermore, stable, ectopic expression of the DNMT3A mutants in primary CD3+ T-cell cultures resulted in the preferential outgrowth of CD8+ T cells with DNMT3AR882H mutation. Single-cell RNA sequencing(RNA-seq) analysis of CD3+ T cells revealed differential CD8+ T-cell subset polarization, mirroring findings in DNMT3A-mutated PTCL-TBX21 and validating the cytotoxic and T-cell memory transcriptional programs associated with the DNMT3AR882H mutation. Our findings indicate that DNMT3A mutations define a cytotoxic subset in PTCL-TBX21 with prognostic significance and thus may further refine pathological heterogeneity in PTCL-NOS and suggest alternative treatment strategies for this subset.

AB - Peripheral T-cell lymphomas (PTCLs) are heterogenous T-cell neoplasms often associated with epigenetic dysregulation. We investigated de novo DNA methyltransferase 3A (DNMT3A) mutations in common PTCL entities, including angioimmunoblastic T-cell lymphoma and novel molecular subtypes identified within PTCL–not otherwise specified (PTCL-NOS) designated as PTCL-GATA3 and PTCL-TBX21. DNMT3A-mutated PTCL-TBX21 cases showed inferior overall survival (OS), with DNMT3A-mutated residues skewed toward the methyltransferase domain and dimerization motif (S881–R887). Transcriptional profiling demonstrated significant enrichment of activated CD8+ T-cell cytotoxic gene signatures in the DNMT3A-mutant PTCL-TBX21 cases, which was further validated using immunohistochemistry. Genomewide methylation analysis of DNMT3A-mutant vs wild-type (WT) PTCL-TBX21 cases demonstrated hypomethylation in target genes regulating interferon-γ (IFN-γ), T-cell receptor signaling, and EOMES (eomesodermin), a master transcriptional regulator of cytotoxic effector cells. Similar findings were observed in a murine model of PTCL with Dnmt3a loss (in vivo) and further validated in vitro by ectopic expression of DNMT3A mutants (DNMT3A-R882, -Q886, and -V716, vs WT) in CD8+ T-cell line, resulting in T-cell activation and EOMES upregulation. Furthermore, stable, ectopic expression of the DNMT3A mutants in primary CD3+ T-cell cultures resulted in the preferential outgrowth of CD8+ T cells with DNMT3AR882H mutation. Single-cell RNA sequencing(RNA-seq) analysis of CD3+ T cells revealed differential CD8+ T-cell subset polarization, mirroring findings in DNMT3A-mutated PTCL-TBX21 and validating the cytotoxic and T-cell memory transcriptional programs associated with the DNMT3AR882H mutation. Our findings indicate that DNMT3A mutations define a cytotoxic subset in PTCL-TBX21 with prognostic significance and thus may further refine pathological heterogeneity in PTCL-NOS and suggest alternative treatment strategies for this subset.

UR - https://www.scopus.com/pages/publications/85138080064

UR - https://www.scopus.com/pages/publications/85138080064#tab=citedBy

U2 - 10.1182/blood.2021015019

DO - 10.1182/blood.2021015019

M3 - Article

C2 - 35639959

AN - SCOPUS:85138080064

SN - 0006-4971

VL - 140

SP - 1278

EP - 1290

JO - Blood

JF - Blood

IS - 11

ER -

DNMT3A mutations define a unique biological and prognostic subgroup associated with cytotoxic T cells in PTCL-NOS

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