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

Blood. 2020 Dec 10;136(24):2786-2802. doi: 10.1182/blood.2019003348.

Authors

S Oberbeck^{1

2

3}, A Schrader^{1

2

3}, K Warner^{1

4}, D Jungherz^{1

2

3}, G Crispatzu^{1

2

3}, J von Jan^{1

2

3}, M Chmielewski^{1

2

3}, A Ianevski⁵, H H Diebner⁶, P Mayer^{1

2

3}, A Kondo Ados^{1

2

3}, L Wahnschaffe^{1

2

3}, T Braun^{1

2

3}, T A Müller^{1

2

3}, P Wagle², A Bouska⁷, T Neumann^{1

2

3}, S Pützer^{1

2

3}, L Varghese^{1

2

3}, N Pflug¹, M Thelen^{1

3}, J Makalowski^{1

3}, N Riet^{1

3}, H J M Göx^{1

2}, G Rappl^{1

3}, J Altmüller⁸, M Kotrová⁹, T Persigehl¹⁰, G Hopfinger¹¹, M L Hansmann⁴, H Schlößer³, S Stilgenbauer¹², J Dürig¹³, D Mougiakakos¹⁴, M von Bergwelt-Baildon¹⁵, I Roeder⁶, S Hartmann⁴, M Hallek^{1

2

3}, R Moriggl^{16

17}, M Brüggemann⁹, T Aittokallio⁵, J Iqbal⁷, S Newrzela⁴, H Abken¹⁸, M Herling^{1

2

3}

Affiliations

¹ Department I of Internal Medicine, Center for Integrated Oncology Aachen-Bonn-Cologne-Duesseldorf.
² CECAD Center of Excellence on Cellular Stress Responses in Aging-Associated Diseases, and.
³ Center for Molecular Medicine Cologne, University of Cologne (UoC), Cologne, Germany.
⁴ Senckenberg Institute of Pathology, Goethe University, Frankfurt am Main, Germany.
⁵ Institute for Molecular Medicine Finland, University of Helsinki, Helsinki, Finland.
⁶ Faculty of Medicine Carl Gustav Carus, Institute for Medical Informatics and Biometry Dresden, Technische Universität Dresden, Dresden, Germany.
⁷ Department of Pathology and Microbiology, University of Nebraska Medical Center, Omaha, NE.
⁸ Cologne Center for Genomics, Institute of Human Genetics, UoC, Cologne, Germany.
⁹ Medical Department II of Hematology and Oncology, University Hospital of Schleswig Holstein, Campus Kiel, Kiel, Germany.
¹⁰ Department of Radiology, UoC, Cologne, Germany.
¹¹ Center for Oncology and Hematology, Kaiser-Franz-Josef-Spital, Vienna, Austria.
¹² Department III of Internal Medicine, University Hospital Ulm, Ulm, Germany.
¹³ Clinic for Hematology, University Hospital Essen, Essen, Germany.
¹⁴ Department of Medicine 5, Hematology, and Oncology, University Hospital Erlangen, Erlangen, Germany.
¹⁵ Department of Medicine III, University Hospital LMU Munich, Munich, Germany.
¹⁶ Institute of Animal Breeding and Genetics, University of Veterinary Medicine, Vienna, Austria.
¹⁷ Ludwig Boltzmann Institute for Cancer Research, Medical University of Vienna, Vienna, Austria; and.
¹⁸ RCI Regensburg Center for Interventional Immunology, Regensburg, Germany.

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.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

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

Substances

Proto-Oncogene Proteins
Receptors, Antigen, T-Cell
TCL1A protein, human

Abstract

Publication types

MeSH terms

Substances

Grants and funding