Metabolic requirements of CD160 expressing memory‐like NK cells in Gram‐negative bacterial infection

Author:

Preechanukul Anucha12,Saiprom Natnaree1,Rochaikun Kitilak1,Moonmueangsan Boonthanom1,Phunpang Rungnapa1,Ottiwet Orawan3,Kongphrai Yuphin3,Wapee Soonthon3,Janon Rachan4,Dunachie Susanna5678,Kronsteiner Barbara67,Chantratita Narisara15

Affiliation:

1. Department of Microbiology and Immunology, Faculty of Tropical Medicine Mahidol University Bangkok Thailand

2. Division of Infection and Immunity University College London London UK

3. Department of Medical Technology and Clinical Pathology Mukdahan Hospital Mukdahan Thailand

4. Department of Medicine Mukdahan Hospital Mukdahan Thailand

5. Mahidol‐Oxford Tropical Medicine Research Unit Mahidol University Bangkok Thailand

6. Peter Medawar Building for Pathogen Research, Nuffield Department of Clinical Medicine University of Oxford Oxford UK

7. Nuffield Department of Clinical Medicine, NDM Centre for Global Health Research University of Oxford Oxford UK

8. Oxford University Hospitals NHS Foundation Trust Oxford UK

Abstract

AbstractObjectiveUnique metabolic requirements accompany the development and functional fates of immune cells. How cellular metabolism is important in natural killer (NK) cells and their memory‐like differentiation in bacterial infections remains elusive.MethodsHere, we utilise our established NK cell memory assay to investigate the metabolic requirement for memory‐like NK cell formation and function in response to the Gram‐negative intracellular bacteria Burkholderia pseudomallei (BP), the causative agent of melioidosis.ResultsWe demonstrate that CD160+ memory‐like NK cells upon BP stimulation upregulate glucose and amino acid transporters in a cohort of recovered melioidosis patients which is maintained at least 3‐month post‐hospital admission. Using an in vitro assay, human BP‐specific CD160+ memory‐like NK cells show metabolic priming including increased expression of glucose and amino acid transporters with elevated glucose uptake, increased mTOR activation and mitochondrial membrane potential upon BP re‐stimulation. Antigen‐specific and cytokine‐induced IFN‐γ production of this memory‐like NK cell subset are highly dependent on oxidative phosphorylation (OXPHOS) with some dependency on glycolysis, whereas the formation of CD160+ memory‐like NK cells in vitro is dependent on fatty acid oxidation and OXPHOS and further increased by metformin.ConclusionThis study reveals the link between metabolism and cellular function of memory‐like NK cells, which can be exploited for vaccine design and for monitoring protection against Gram‐negative bacterial infection.

Funder

Wellcome Trust

Publisher

Wiley

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