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ERANET-PLL

ERANET-PLL

Richard Moriggl (ORCID: 0000-0003-0918-9463)
  • Grant DOI 10.55776/I4157
  • Funding program International - Multilateral Initiatives
  • Status ended
  • Start May 1, 2019
  • End October 31, 2022
  • Funding amount € 287,396
  • Project website

ERA-NET: TRANSCAN

Disciplines

Biology (30%); Medical-Theoretical Sciences, Pharmacy (70%)

Keywords

    T cell, Leukemia, STAT, Targeted Drug, Metabolomics, Systemsbiology

Abstract Final report

Rationale: T-PLL is the most frequent mature T-cell leukemia, yet it occurs at an incidence of 0.6/Mio in the EU. Its chemotherapy resistance translates into an average patient survival of <20 months. There are no approved drugs for T-PLL and numerous exploratory or comparative trials to test novel options are not feasible. First inhibitor screens, piloted by our teams, uncovered promising, but also differential sensitivities. However, we are still far from informed implementation of new molecular knowledge into clinical application. This is mostly due to lack of integration of available multi-level profiling data and a rudimentary understanding of their functional impact. Moreover, gene- regulatory, particularly epigenetic changes and metabolic cellular states, both also known to influence treatment responses in cancer, have not been addressed in T-PLL. Overall, we miss a concept of how drug activity patterns relate to T-PLLs molecular landscape. Hypothesis: Integration of genomic, epigenetic, and phenotypic data will allow predictions of differential compound sensitivities, which in conjunction with clinical information will aid in individual treatment decisions and future trial designs. Aims / Methods: The 5 teams of ERANET-PLL will capitalize on unique prerequisites, e.g. a large repository of well-annotated material, an open registry, or T-PLL animal models. We will analyze to which degree genomic and epigenetic alterations as well as basal and inhibitor-induced metabolic signatures dictate differential substance activities. Bio-computational modelling will integrate these genotypic and phenotypic dimensions towards prediction tools of in- vitro drug sensitivities and synergies. Drug candidates will be validated in various preclinical systems. The extracted set of molecular strata will finally be interrogated in a prospective interventional study. Expected Results: Biomarkers that discern T-PLL patient subsets based on vulnerabilities towards targeted compounds.

T-cell prolymphocytic leukemia (T-PLL) is the main mature T-cell leukemia in middle Europe, still a rare, but severe form of leukemia characterized by limited response to conventional chemotherapy and short overall survival. A targeted therapy against main drivers of T-PLL and how they promote proliferation and survival with changed cancer cell metabolism lacks currently behind in this mature T-cell cancer. The aim of ERANET-PLL was to discover and evaluate novel therapeutic approaches for this disease entity. The Moriggl group helped to explore new drugs for mature T-cell neoplasias and to work jointly also on pre-clinical evaluation of cancer cell metabolism. We have used state-of-the-art genetic, epigenetic, histo-pathology, pharmacologic and metabolic approaches to improve our understanding of T-PLL. We also profiled and studied collections of T-PLL patient material, T-cell cancer lines and drug libraries. We achieved many high profile publications in internataional peer-reviewed journals and we also disseminated results to the public or to patient interest groups.

Research institution(s)
  • Veterinärmedizinische Universität Wien - 100%
International project participants
  • Emmanuel Bachy, Centre Hospitalier Universitaire de Lyon - France
  • Ingo Röder, Technische Universität Dresden - Germany
  • Marco Herling, Universität Köln - Germany

Research Output

  • 911 Citations
  • 26 Publications
Publications
  • 2020
    Title Thyroid and androgen receptor signaling are antagonized by µ-Crystallin in prostate cancer
    DOI 10.1002/ijc.33332
    Type Journal Article
    Author Aksoy O
    Journal International Journal of Cancer
    Pages 731-747
    Link Publication
  • 2020
    Title Noncanonical effector functions of the T-memory–like T-PLL cell are shaped by cooperative TCL1A and TCR signaling
    DOI 10.1182/blood.2019003348
    Type Journal Article
    Author Oberbeck S
    Journal Blood
    Pages 2786-2802
    Link Publication
  • 2019
    Title Structural and functional consequences of the STAT5BN642H driver mutation
    DOI 10.1038/s41467-019-10422-7
    Type Journal Article
    Author De Araujo E
    Journal Nature Communications
    Pages 2517
    Link Publication
  • 2019
    Title Direct Targeting Options for STAT3 and STAT5 in Cancer
    DOI 10.3390/cancers11121930
    Type Journal Article
    Author Orlova A
    Journal Cancers
    Pages 1930
    Link Publication
  • 2019
    Title High activation of STAT5A drives peripheral T-cell lymphoma and leukemia
    DOI 10.3324/haematol.2019.216986
    Type Journal Article
    Author Maurer B
    Journal Haematologica
    Pages 435-447
    Link Publication
  • 2019
    Title Structural Implications of STAT3 and STAT5 SH2 Domain Mutations
    DOI 10.3390/cancers11111757
    Type Journal Article
    Author De Araujo E
    Journal Cancers
    Pages 1757
    Link Publication
  • 2022
    Title High Efficacy and Drug Synergy of HDAC6-Selective Inhibitor NN-429 in Natural Killer (NK)/T-Cell Lymphoma
    DOI 10.3390/ph15111321
    Type Journal Article
    Author Garcha H
    Journal Pharmaceuticals
    Pages 1321
    Link Publication
  • 2022
    Title Blocking STAT3/5 through direct or upstream kinase targeting in leukemic cutaneous T-cell lymphoma
    DOI 10.15252/emmm.202115200
    Type Journal Article
    Author Sorger H
    Journal EMBO Molecular Medicine
    Link Publication
  • 2021
    Title Development of HDAC Inhibitors Exhibiting Therapeutic Potential in T-Cell Prolymphocytic Leukemia
    DOI 10.1021/acs.jmedchem.1c00420
    Type Journal Article
    Author Toutah K
    Journal Journal of Medicinal Chemistry
    Pages 8486-8509
    Link Publication
  • 2020
    Title STAT5 is Expressed in CD34+/CD38- Stem Cells and Serves as a Potential Molecular Target in Ph-Negative Myeloproliferative Neoplasms
    DOI 10.3390/cancers12041021
    Type Journal Article
    Author Hadzijusufovic E
    Journal Cancers
    Pages 1021
    Link Publication
  • 2020
    Title Advances in covalent kinase inhibitors
    DOI 10.1039/c9cs00720b
    Type Journal Article
    Author Abdeldayem A
    Journal Chemical Society Reviews
    Pages 2617-2687
  • 2020
    Title The neonatal microenvironment programs innate ?d T cells through the transcription factor STAT5
    DOI 10.1172/jci131241
    Type Journal Article
    Author Kadekar D
    Journal Journal of Clinical Investigation
    Pages 2496-2508
    Link Publication
  • 2021
    Title A hydride transfer complex reprograms NAD metabolism and bypasses senescence
    DOI 10.1016/j.molcel.2021.08.028
    Type Journal Article
    Author Igelmann S
    Journal Molecular Cell
  • 2021
    Title Down-regulation of A20 promotes immune escape of lung adenocarcinomas
    DOI 10.1126/scitranslmed.abc3911
    Type Journal Article
    Author Breitenecker K
    Journal Science Translational Medicine
    Link Publication
  • 2021
    Title Oncogenic Kinase Cascades Induce Molecular Mechanisms That Protect Leukemic Cell Models from Lethal Effects of De Novo dNTP Synthesis Inhibition
    DOI 10.3390/cancers13143464
    Type Journal Article
    Author Pons M
    Journal Cancers
    Pages 3464
    Link Publication
  • 2021
    Title Efficacy and Synergy of Small Molecule Inhibitors Targeting FLT3-ITD+ Acute Myeloid Leukemia
    DOI 10.3390/cancers13246181
    Type Journal Article
    Author Bregante J
    Journal Cancers
    Pages 6181
    Link Publication
  • 2021
    Title The Diverse Roles of ?d T Cells in Cancer: From Rapid Immunity to Aggressive Lymphoma
    DOI 10.3390/cancers13246212
    Type Journal Article
    Author Schönefeldt S
    Journal Cancers
    Pages 6212
    Link Publication
  • 2020
    Title STAT5 is required for lipid breakdown and beta-adrenergic responsiveness of brown adipose tissue
    DOI 10.1016/j.molmet.2020.101026
    Type Journal Article
    Author Kaltenecker D
    Journal Molecular Metabolism
    Pages 101026
    Link Publication
  • 2020
    Title Targeting STAT3 and STAT5 in Cancer
    DOI 10.3390/cancers12082002
    Type Journal Article
    Author De Araujo E
    Journal Cancers
    Pages 2002
    Link Publication
  • 2019
    Title The stromal microenvironment provides an escape route from FLT3 inhibitors through the GAS6-AXL-STAT5 axis
    DOI 10.3324/haematol.2019.225862
    Type Journal Article
    Author Orlova A
    Journal Haematologica
    Pages 1907-1909
    Link Publication
  • 2022
    Title JAK-STAT core cancer pathway: An integrative cancer interactome analysis
    DOI 10.1111/jcmm.17228
    Type Journal Article
    Author Erdogan F
    Journal Journal of Cellular and Molecular Medicine
    Pages 2049-2062
    Link Publication
  • 2021
    Title A Recurrent STAT5BN642H Driver Mutation in Feline Alimentary T Cell Lymphoma
    DOI 10.3390/cancers13205238
    Type Journal Article
    Author Kieslinger M
    Journal Cancers
    Pages 5238
    Link Publication
  • 2021
    Title Structural and mutational analysis of member-specific STAT functions
    DOI 10.1016/j.bbagen.2021.130058
    Type Journal Article
    Author Erdogan F
    Journal Biochimica et Biophysica Acta (BBA) - General Subjects
    Pages 130058
  • 2021
    Title A centric view of JAK/STAT5 in intestinal homeostasis, infection, and inflammation
    DOI 10.1016/j.cyto.2020.155392
    Type Journal Article
    Author Surbek M
    Journal Cytokine
    Pages 155392
    Link Publication
  • 2021
    Title Opioids drive breast cancer metastasis through the d-opioid receptor and oncogenic STAT3
    DOI 10.1016/j.neo.2020.12.011
    Type Journal Article
    Author Tripolt S
    Journal Neoplasia
    Pages 270-279
    Link Publication
  • 2021
    Title STAT3 activation in large granular lymphocyte leukemia is associated with cytokine signaling and DNA hypermethylation
    DOI 10.1038/s41375-021-01296-0
    Type Journal Article
    Author Kim D
    Journal Leukemia
    Pages 3430-3443
    Link Publication

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