The Glucose Transporter 5 Enhances CAR-T Cell Metabolic Function and Anti-tumour Durability.
Bakir ValentićAndre KellyAlexander A ShestovZhiyang GanFeng ShenAdam ChatoffAlison JaccardClaudia V CrispimJohn SchollerSimon HeekeNathaniel W SnyderSaba GhassemiNicholas JonesSaar I GillRoderick O'ConnorPublished in: Research square (2024)
Activated T cells undergo a metabolic shift to aerobic glycolysis to support the energetic demands of proliferation, differentiation, and cytolytic function. Transmembrane glucose flux is facilitated by glucose transporters (GLUT) that play a vital role in T cell metabolic reprogramming and anti-tumour function. GLUT isoforms are regulated at the level of expression and subcellular distribution. GLUTs also display preferential selectivity for carbohydrate macronutrients including glucose, galactose, and fructose. GLUT5, which selectively transports fructose over glucose, has never been explored as a genetic engineering strategy to enhance CAR-T cells in fructose-rich tumour environments. Fructose levels are significantly elevated in the bone marrow and the plasma of acute myeloid leukaemia (AML) patients. Here, we demonstrate that the expression of wild-type GLUT5 restores T cell metabolic fitness in glucose-free, high fructose conditions. We find that fructose supports maximal glycolytic capacity and ATP replenishment rates in GLUT5-expressing T cells. Using steady state tracer technology, we show that 13 C 6 fructose supports glycolytic reprogramming and TCA anaplerosis in CAR-T cells undergoing log phase expansion. In cytotoxicity assays, GLUT5 rescues T cell cytolytic function in glucose-free medium. The fructose/GLUT5 metabolic axis also supports maximal migratory velocity, which provides mechanistic insight into why GLUT5-expressing CAR-Ts have superior effector function as they undergo "hit-and-run" serial killing. These findings translate to superior anti-tumour function in a xenograft model of AML. In fact, we found that GLUT5 enhances CAR-T cell anti-tumour function in vivo without any need for fructose intervention. Accordingly, we hypothesize that GLUT5 is sufficient to enhance CAR-T resilience by increasing the cells' competitiveness for glucose at physiologic metabolite levels. Our findings have immediate translational relevance by providing the first evidence that GLUT5 confers a competitive edge in a fructose-enriched milieu, and is a novel approach to overcome glucose depletion in hostile tumour microenvironments (TMEs).
Keyphrases
- blood glucose
- bone marrow
- acute myeloid leukemia
- poor prognosis
- randomized controlled trial
- computed tomography
- wild type
- climate change
- physical activity
- type diabetes
- stem cells
- intensive care unit
- regulatory t cells
- skeletal muscle
- adipose tissue
- metabolic syndrome
- newly diagnosed
- immune response
- body composition
- insulin resistance
- gene expression
- positron emission tomography
- extracorporeal membrane oxygenation
- ejection fraction
- transcription factor
- heart rate
- acute lymphoblastic leukemia
- patient reported
- cell cycle arrest