Noncanonical effector functions of the T-memory-like T-PLL cell are shaped by cooperative TCL1A and TCR signaling

S Oberbeck; A Schrader; K Warner; D Jungherz; G Crispatzu; J von Jan; M Chmielewski; A Ianevski; H H Diebner; P Mayer; A Kondo Ados; L Wahnschaffe; T Braun; T A Müller; P Wagle; A Bouska; T Neumann; S Pützer; L Varghese; N Pflug; M Thelen; J Makalowski; N Riet; H J M Göx; G Rappl; J Altmüller; M Kotrová; T Persigehl; G Hopfinger; M L Hansmann; H Schlößer; S Stilgenbauer; J Dürig; D Mougiakakos; M von Bergwelt-Baildon; I Roeder; S Hartmann; M Hallek; R Moriggl; M Brüggemann; T Aittokallio; J Iqbal; S Newrzela; H Abken; M Herling

doi:10.1182/blood.2019003348

Noncanonical effector functions of the T-memory-like T-PLL cell are shaped by cooperative TCL1A and TCR signaling

S Oberbeck, A Schrader, K Warner, D Jungherz, G Crispatzu, J von Jan, M Chmielewski, A Ianevski, H H Diebner, P Mayer, A Kondo Ados, L Wahnschaffe, T Braun, T A Müller, P Wagle, A Bouska, T Neumann, S Pützer, L Varghese, N PflugM Thelen, J Makalowski, N Riet, H J M Göx, G Rappl, J Altmüller, M Kotrová, T Persigehl, G Hopfinger, M L Hansmann, H Schlößer, S Stilgenbauer, J Dürig, D Mougiakakos, M von Bergwelt-Baildon, I Roeder, S Hartmann, M Hallek, R Moriggl, M Brüggemann, T Aittokallio, J Iqbal, S Newrzela, H Abken, M Herling

Universitätsbibliothek

Publikation: Beitrag in Fachzeitschrift › Artikel › Peer-reviewed

Abstract

T-cell prolymphocytic leukemia (T-PLL) is a poor-prognostic neoplasm. Differentiation stage and immune-effector functions of the underlying tumor cell are insufficiently characterized. Constitutive activation of the T-cell leukemia 1A (TCL1A) oncogene distinguishes the (pre)leukemic cell from regular postthymic T cells. We assessed activation-response patterns of the T-PLL lymphocyte and interrogated the modulatory impact by TCL1A. Immunophenotypic and gene expression profiles revealed a unique spectrum of memory-type differentiation of T-PLL with predominant central-memory stages and frequent noncanonical patterns. Virtually all T-PLL expressed a T-cell receptor (TCR) and/or CD28-coreceptor without overrepresentation of specific TCR clonotypes. The highly activated leukemic cells also revealed losses of negative-regulatory TCR coreceptors (eg, CTLA4). TCR stimulation of T-PLL cells evoked higher-than-normal cell-cycle transition and profiles of cytokine release that resembled those of normal memory T cells. More activated phenotypes and higher TCL1A correlated with inferior clinical outcomes. TCL1A was linked to the marked resistance of T-PLL to activation- and FAS-induced cell death. Enforced TCL1A enhanced phospho-activation of TCR kinases, second-messenger generation, and JAK/STAT or NFAT transcriptional responses. This reduced the input thresholds for IL-2 secretion in a sensitizer-like fashion. Mice of TCL1A-initiated protracted T-PLL development resembled such features. When equipped with epitope-defined TCRs or chimeric antigen receptors, these Lckpr-hTCL1Atg T cells gained a leukemogenic growth advantage in scenarios of receptor stimulation. Overall, we propose a model of T-PLL pathogenesis in which TCL1A enhances TCR signals and drives the accumulation of death-resistant memory-type cells that use amplified low-level stimulatory input, and whose loss of negative coregulators additionally maintains their activated state. Treatment rationales are provided by combined interception in TCR and survival signaling.

Originalsprache	Englisch
Seiten (von - bis)	2786-2802
Seitenumfang	17
Fachzeitschrift	BLOOD
Jahrgang	136
Ausgabenummer	24
DOIs	https://doi.org/10.1182/blood.2019003348
Publikationsstatus	Veröffentlicht - 10 Dez. 2020

Bibliographische Notiz

Systematik der Wissenschaftszweige 2012

106 Biologie

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10.1182/blood.2019003348

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Oberbeck, S., Schrader, A., Warner, K., Jungherz, D., Crispatzu, G., von Jan, J., Chmielewski, M., Ianevski, A., Diebner, H. H., Mayer, P., Kondo Ados, A., Wahnschaffe, L., Braun, T., Müller, T. A., Wagle, P., Bouska, A., Neumann, T., Pützer, S., Varghese, L., ... Herling, M. (2020). Noncanonical effector functions of the T-memory-like T-PLL cell are shaped by cooperative TCL1A and TCR signaling. BLOOD, 136(24), 2786-2802. https://doi.org/10.1182/blood.2019003348

@article{d89fdfda602349fb97dba7e03967eab9,

title = "Noncanonical effector functions of the T-memory-like T-PLL cell are shaped by cooperative TCL1A and TCR signaling",

abstract = "T-cell prolymphocytic leukemia (T-PLL) is a poor-prognostic neoplasm. Differentiation stage and immune-effector functions of the underlying tumor cell are insufficiently characterized. Constitutive activation of the T-cell leukemia 1A (TCL1A) oncogene distinguishes the (pre)leukemic cell from regular postthymic T cells. We assessed activation-response patterns of the T-PLL lymphocyte and interrogated the modulatory impact by TCL1A. Immunophenotypic and gene expression profiles revealed a unique spectrum of memory-type differentiation of T-PLL with predominant central-memory stages and frequent noncanonical patterns. Virtually all T-PLL expressed a T-cell receptor (TCR) and/or CD28-coreceptor without overrepresentation of specific TCR clonotypes. The highly activated leukemic cells also revealed losses of negative-regulatory TCR coreceptors (eg, CTLA4). TCR stimulation of T-PLL cells evoked higher-than-normal cell-cycle transition and profiles of cytokine release that resembled those of normal memory T cells. More activated phenotypes and higher TCL1A correlated with inferior clinical outcomes. TCL1A was linked to the marked resistance of T-PLL to activation- and FAS-induced cell death. Enforced TCL1A enhanced phospho-activation of TCR kinases, second-messenger generation, and JAK/STAT or NFAT transcriptional responses. This reduced the input thresholds for IL-2 secretion in a sensitizer-like fashion. Mice of TCL1A-initiated protracted T-PLL development resembled such features. When equipped with epitope-defined TCRs or chimeric antigen receptors, these Lckpr-hTCL1Atg T cells gained a leukemogenic growth advantage in scenarios of receptor stimulation. Overall, we propose a model of T-PLL pathogenesis in which TCL1A enhances TCR signals and drives the accumulation of death-resistant memory-type cells that use amplified low-level stimulatory input, and whose loss of negative coregulators additionally maintains their activated state. Treatment rationales are provided by combined interception in TCR and survival signaling.",

keywords = "Animals, Humans, Immunologic Memory, Leukemia, Prolymphocytic, T-Cell/genetics, Mice, Mice, Knockout, Proto-Oncogene Proteins/genetics, Receptors, Antigen, T-Cell/genetics, Signal Transduction/genetics, T-Lymphocytes/immunology",

author = "S Oberbeck and A Schrader and K Warner and D Jungherz and G Crispatzu and {von Jan}, J and M Chmielewski and A Ianevski and Diebner, {H H} and P Mayer and {Kondo Ados}, A and L Wahnschaffe and T Braun and M{\"u}ller, {T A} and P Wagle and A Bouska and T Neumann and S P{\"u}tzer and L Varghese and N Pflug and M Thelen and J Makalowski and N Riet and G{\"o}x, {H J M} and G Rappl and J Altm{\"u}ller and M Kotrov{\'a} and T Persigehl and G Hopfinger and Hansmann, {M L} and H Schl{\"o}{\ss}er and S Stilgenbauer and J D{\"u}rig and D Mougiakakos and {von Bergwelt-Baildon}, M and I Roeder and S Hartmann and M Hallek and R Moriggl and M Br{\"u}ggemann and T Aittokallio and J Iqbal and S Newrzela and H Abken and M Herling",

note = "{\textcopyright} 2020 by The American Society of Hematology.",

year = "2020",

month = dec,

day = "10",

doi = "10.1182/blood.2019003348",

language = "English",

volume = "136",

pages = "2786--2802",

journal = "BLOOD",

issn = "0006-4971",

publisher = "American Society of Hematology",

number = "24",

}

Oberbeck, S, Schrader, A, Warner, K, Jungherz, D, Crispatzu, G, von Jan, J, Chmielewski, M, Ianevski, A, Diebner, HH, Mayer, P, Kondo Ados, A, Wahnschaffe, L, Braun, T, Müller, TA, Wagle, P, Bouska, A, Neumann, T, Pützer, S, Varghese, L, Pflug, N, Thelen, M, Makalowski, J, Riet, N, Göx, HJM, Rappl, G, Altmüller, J, Kotrová, M, Persigehl, T, Hopfinger, G, Hansmann, ML, Schlößer, H, Stilgenbauer, S, Dürig, J, Mougiakakos, D, von Bergwelt-Baildon, M, Roeder, I, Hartmann, S, Hallek, M, Moriggl, R, Brüggemann, M, Aittokallio, T, Iqbal, J, Newrzela, S, Abken, H & Herling, M 2020, 'Noncanonical effector functions of the T-memory-like T-PLL cell are shaped by cooperative TCL1A and TCR signaling', BLOOD, Jg. 136, Nr. 24, S. 2786-2802. https://doi.org/10.1182/blood.2019003348

TY - JOUR

T1 - Noncanonical effector functions of the T-memory-like T-PLL cell are shaped by cooperative TCL1A and TCR signaling

AU - Oberbeck, S

AU - Schrader, A

AU - Warner, K

AU - Jungherz, D

AU - Crispatzu, G

AU - von Jan, J

AU - Chmielewski, M

AU - Ianevski, A

AU - Diebner, H H

AU - Mayer, P

AU - Kondo Ados, A

AU - Wahnschaffe, L

AU - Braun, T

AU - Müller, T A

AU - Wagle, P

AU - Bouska, A

AU - Neumann, T

AU - Pützer, S

AU - Varghese, L

AU - Pflug, N

AU - Thelen, M

AU - Makalowski, J

AU - Riet, N

AU - Göx, H J M

AU - Rappl, G

AU - Altmüller, J

AU - Kotrová, M

AU - Persigehl, T

AU - Hopfinger, G

AU - Hansmann, M L

AU - Schlößer, H

AU - Stilgenbauer, S

AU - Dürig, J

AU - Mougiakakos, D

AU - von Bergwelt-Baildon, M

AU - Roeder, I

AU - Hartmann, S

AU - Hallek, M

AU - Moriggl, R

AU - Brüggemann, M

AU - Aittokallio, T

AU - Iqbal, J

AU - Newrzela, S

AU - Abken, H

AU - Herling, M

PY - 2020/12/10

Y1 - 2020/12/10

N2 - T-cell prolymphocytic leukemia (T-PLL) is a poor-prognostic neoplasm. Differentiation stage and immune-effector functions of the underlying tumor cell are insufficiently characterized. Constitutive activation of the T-cell leukemia 1A (TCL1A) oncogene distinguishes the (pre)leukemic cell from regular postthymic T cells. We assessed activation-response patterns of the T-PLL lymphocyte and interrogated the modulatory impact by TCL1A. Immunophenotypic and gene expression profiles revealed a unique spectrum of memory-type differentiation of T-PLL with predominant central-memory stages and frequent noncanonical patterns. Virtually all T-PLL expressed a T-cell receptor (TCR) and/or CD28-coreceptor without overrepresentation of specific TCR clonotypes. The highly activated leukemic cells also revealed losses of negative-regulatory TCR coreceptors (eg, CTLA4). TCR stimulation of T-PLL cells evoked higher-than-normal cell-cycle transition and profiles of cytokine release that resembled those of normal memory T cells. More activated phenotypes and higher TCL1A correlated with inferior clinical outcomes. TCL1A was linked to the marked resistance of T-PLL to activation- and FAS-induced cell death. Enforced TCL1A enhanced phospho-activation of TCR kinases, second-messenger generation, and JAK/STAT or NFAT transcriptional responses. This reduced the input thresholds for IL-2 secretion in a sensitizer-like fashion. Mice of TCL1A-initiated protracted T-PLL development resembled such features. When equipped with epitope-defined TCRs or chimeric antigen receptors, these Lckpr-hTCL1Atg T cells gained a leukemogenic growth advantage in scenarios of receptor stimulation. Overall, we propose a model of T-PLL pathogenesis in which TCL1A enhances TCR signals and drives the accumulation of death-resistant memory-type cells that use amplified low-level stimulatory input, and whose loss of negative coregulators additionally maintains their activated state. Treatment rationales are provided by combined interception in TCR and survival signaling.

AB - T-cell prolymphocytic leukemia (T-PLL) is a poor-prognostic neoplasm. Differentiation stage and immune-effector functions of the underlying tumor cell are insufficiently characterized. Constitutive activation of the T-cell leukemia 1A (TCL1A) oncogene distinguishes the (pre)leukemic cell from regular postthymic T cells. We assessed activation-response patterns of the T-PLL lymphocyte and interrogated the modulatory impact by TCL1A. Immunophenotypic and gene expression profiles revealed a unique spectrum of memory-type differentiation of T-PLL with predominant central-memory stages and frequent noncanonical patterns. Virtually all T-PLL expressed a T-cell receptor (TCR) and/or CD28-coreceptor without overrepresentation of specific TCR clonotypes. The highly activated leukemic cells also revealed losses of negative-regulatory TCR coreceptors (eg, CTLA4). TCR stimulation of T-PLL cells evoked higher-than-normal cell-cycle transition and profiles of cytokine release that resembled those of normal memory T cells. More activated phenotypes and higher TCL1A correlated with inferior clinical outcomes. TCL1A was linked to the marked resistance of T-PLL to activation- and FAS-induced cell death. Enforced TCL1A enhanced phospho-activation of TCR kinases, second-messenger generation, and JAK/STAT or NFAT transcriptional responses. This reduced the input thresholds for IL-2 secretion in a sensitizer-like fashion. Mice of TCL1A-initiated protracted T-PLL development resembled such features. When equipped with epitope-defined TCRs or chimeric antigen receptors, these Lckpr-hTCL1Atg T cells gained a leukemogenic growth advantage in scenarios of receptor stimulation. Overall, we propose a model of T-PLL pathogenesis in which TCL1A enhances TCR signals and drives the accumulation of death-resistant memory-type cells that use amplified low-level stimulatory input, and whose loss of negative coregulators additionally maintains their activated state. Treatment rationales are provided by combined interception in TCR and survival signaling.

KW - Animals

KW - Humans

KW - Immunologic Memory

KW - Leukemia, Prolymphocytic, T-Cell/genetics

KW - Mice

KW - Mice, Knockout

KW - Proto-Oncogene Proteins/genetics

KW - Receptors, Antigen, T-Cell/genetics

KW - Signal Transduction/genetics

KW - T-Lymphocytes/immunology

U2 - 10.1182/blood.2019003348

DO - 10.1182/blood.2019003348

M3 - Article

C2 - 33301031

SN - 0006-4971

VL - 136

SP - 2786

EP - 2802

JO - BLOOD

JF - BLOOD

IS - 24

ER -