Inhibition of glucose uptake increase serial-killing capacity of Natural Killer cells

Author:

Picard Lea Katharina1,Niemann Jens Alexander1,Littwitz-Salomon Elisabeth2,Waldmann Herbert3,Watzl Carsten1ORCID

Affiliation:

1. Leibniz-Institut für Arbeitsforschung an der TU Dortmund: Leibniz-Institut fur Arbeitsforschung an der TU Dortmund

2. University of Duisburg-Essen - Campus Essen: Universitat Duisburg-Essen - Campus Essen

3. Max-Planck-Institute of Molecular Physiology: Max-Planck-Institut fur molekulare Physiologie

Abstract

Abstract Tumor cells rely heavily on glycolysis to meet their high metabolic demands. While this results in nutrient deprivation within the tumor microenvironment and has negative effects on infiltrating immune cells such as Natural Killer (NK) cells, it also creates a potential target for cancer therapies. Here we use Glupin, an inhibitor of glucose transporters, to study the effect of limited glucose uptake on NK cells and their anti-tumor functions. Glupin treatment effectively inhibited glucose uptake and restricted glycolysis in NK cells. However, acute treatment had no negative effect on NK cell cytotoxicity or cytokine production. Long-term restriction of glucose uptake by Glupin treatment only delayed NK cell proliferation as they could switch to glutaminolysis as alternative energy source. While IFN-g production was partially impaired, long-term Glupin treatment had no negative effect on degranulation. Interestingly, the serial killing activity of NK cells was even enhanced, possibly due to changes in NAD metabolism. This demonstrates that NK cell cytotoxicity is remarkably robust and insensitive to metabolic disturbances and makes cellular metabolism an attractive target for immune-mediated tumor therapies.

Publisher

Research Square Platform LLC

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