Zusammenfassung der Projektergebnisse

Our results clearly demonstrate that T cell effector functions can be preserved in the presence of metabolic inhibitors. Proliferation turned out to be more sensitive, however, even under administration of potent glycolytic inhibitors only a reduction was observed but not a complete blockade. The administration of diclofenac or lumiracoxib, blocking MCT1 and MCT4 and at the same time COX activity, thereby reducing the secretion of the immunosuppressive metabolite prostaglandine E2, turned out to be a promising strategy in the context of immunotherapeutic approaches, underlined by our first in vivo mouse experiments. With regard to glutamine metabolism, there seems to be a window for certain pathway inhibitors, whereas the application of glutamine analogues or pan-glutamine inhibitors most likely results in severe immunosuppression. Further evaluation is warranted to exclude adverse side effects. From the results obtained in this project we conclude, that the detailed analysis of the link between metabolism and CD8+ T cell function and the impact of anti-metabolic drugs reveal possible favourable combinations of anti-metabolic drugs and immunotherapeutic approaches (such as checkpoint inhibitors), which appear to strengthen the anti-tumor immune response and should be tested within clinical trials.

Projektbezogene Publikationen (Auswahl)

• (2014) Immunologic and metabolic characteristics of HPV-negative and HPV-positive head and neck squamous cell carcinomas are strikingly different. Virchows Arch. Sep;465(3):299-312
  Krupar R, Robold K, Gaag D, Spanier G, Kreutz M, Renner K, Hellerbrand C, Hofstaedter F, Bosserhoff AK
  (Siehe online unter https://doi.org/10.1007/s00428-014-1630-6)
• (2015) Metabolic plasticity of human T cells: Preserved cytokine production under glucose deprivation or mitochondrial restriction, but 2-deoxyglucose affects effector functions. Eur J Immunol. Sep;45(9):2504-16
  Renner K, Geiselhöringer AL, Fante M, Bruss C, Färber S, Schönhammer G, Peter K, Singer K, Andreesen R, Hoffmann P, Oefner P, Herr W, Kreutz M
  (Siehe online unter https://doi.org/10.1002/eji.201545473)
• (2016) LDHA-Associated Lactic Acid Production Blunts Tumor Immunosurveillance by T and NK Cells, Cell Metabolism Nov 8;24(5):657-671
  Brand A., Singer K, Koehl G.E., Kolitzus M., Schoenhammer G., Thiel A., Matos C., Bruss C., Klobuch S., Peter K., Kastenberger M., Bogdan C., Schleicher U., Mackensen A., Ullrich E., Fichtner-Feigl S., Kesselring R., Mack M., Ritter U., Schmid M., Blank C., Dettmer K., Oefner PJ, Hoffmann P., Herr W., Walenta S., Geissler EK., Pouyssegur J., Villunger A., Steven A., Seliger B., Schreml S., Haferkamp S., Kohl E., Karrer S., Berneburg M., Mueller-Klieser M., Renner K., Kreutz M.
  (Siehe online unter https://doi.org/10.1016/j.cmet.2016.08.011)
• (2017) Stattic and metformin inhibit brain tumor initiating cells by reducing STAT3-phosphorylation.Oncotarget Jan 31;8(5):8250-8263
  Leidgens V, Proske J, Rauer L, Moeckel S, Renner K, Bogdahn U, Riemenschneider JM, Proescholdt M, Vollmann-Zwerenz A, Hau P and Seliger C
  (Siehe online unter https://doi.org/10.18632/oncotarget.14159)
• (2018) Combined metabolic targeting with metformin and the NSAIDs diflunisal and diclofenac induces apoptosis in acute myeloid leukemia cells. Frontiers in Pharmacology Nov 2;9:1258
  Renner K., Seilbeck A., Kauer N., Ugele I., Siska P.J., Brummer C., Bruss C., Decking S., Fante M., Schmid A., Hammon K., Singer K., Klobuch S., Thomas S., Gottfried E., Peter K., Kreutz M.
  (Siehe online unter https://doi.org/10.3389/fphar.2018.01258)
• (2018) Combined Modulation of Tumor Metabolism by Metformin and Diclofenac in Glioma. Int J Mol Sci. Aug 31;19(9)
  Gerthofer V, Kreutz M, Renner K, Jachnik B, Dettmer K, Oefner P, Riemenschneider MJ, Proescholdt M, Vollmann-Zwerenz A, Hau P, Seliger C
  (Siehe online unter https://doi.org/10.3390/ijms19092586)
• (2018) D-2-hydroxyglutarate interferes with HIF-1α stability skewing T-cell metabolism towards oxidative phosphorylation and impairing Th17 polarization. Oncoimmunology 7(7):e1445454
  Böttcher M, Renner K, Berger R, Mentz K, Thomas S, Cardenas-Conejo ZE, Dettmer K, Oefner PJ, Mackensen A, Kreutz M, Mougiakakos D
  (Siehe online unter https://doi.org/10.1080/2162402X.2018.1445454)
• (2018) Double genetic disruption of lactate dehydrogenases A and B is required to ablate the "Warburg effect" restricting tumor growth to oxidative metabolism. J BiolChem. Oct 12;293(41):15947-15961
  Ždralević M, Brand A, Di Ianni L, Dettmer K, Reinders J, Singer K, Peter K, Schnell A, Bruss C, Decking SM, Koehl G, Felipe-Abrio B, Durivault J, Bayer P, Evangelista M, O'Brien T, Oefner PJ, Renner K, Pouysségur J, Kreutz M
  (Siehe online unter https://doi.org/10.1074/jbc.RA118.004180)
• (2018) Metabolic targeting synergizes with MAPK inhibition and delays drug resistance in melanoma., Cancer Lett. Nov 24; 442:453-463
  Brummer C, Faerber S, Bruss C, Blank C, Lacroix R, Haferkamp S, Herr W, Kreutz M, Renner K
  (Siehe online unter https://doi.org/10.1016/j.canlet.2018.11.018)
• (2018) Tumor immunoevasion via acidosis dependent induction of regulatory tumor-associated macrophages. Nature Immunology Dec;19(12):1319-1329
  Bohn T., Rapp S., Luther N., Klein M., Bruehl T., Kojima N Lopez P:A., Hahlbrock J., Muth S., Endo S., Pektor S., Brand A., Renner K., Popp V., Gerlach K., Vogel D., Lueckel C., Arnold-Schild D., Pouyssegur J., Kreutz M., Huber M., Koenig J., Weigmann B., Probst H., Stebut E., Becker C., Schild H., Schmitt E., Bopp T.
  (Siehe online unter https://doi.org/10.1038/s41590-018-0226-8)