Pentose phosphate pathway inhibition metabolically reprograms CD8+ T cells and disrupts CNS autoimmunity
Ethan M. Grund, Benjamin D.S. Clarkson, Susanna Pucci, Maria S. Westphal, Carolina Muniz Partida, Sara A. Muhammad, Charles L. Howe
Ethan M. Grund, Benjamin D.S. Clarkson, Susanna Pucci, Maria S. Westphal, Carolina Muniz Partida, Sara A. Muhammad, Charles L. Howe
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Research Article Immunology Neuroscience

Pentose phosphate pathway inhibition metabolically reprograms CD8+ T cells and disrupts CNS autoimmunity

Abstract

Multiple sclerosis is characterized by CNS infiltration of autoreactive immune cells that drive both acute inflammatory demyelination and chronic progressive axonal and neuronal injury. Expanding evidence implicates CD8+ antineural T cells in the neurodegeneration that underlies irreversible clinical progression in multiple sclerosis, yet therapies specifically targeting this cell population are limited. CD8+ T cells from patients with MS exhibit increased engagement of the pentose phosphate pathway. Pharmacologic inhibition of the pentose phosphate pathway reduced glycolysis, glucose uptake, NADPH production, ATP production, proliferation, and proinflammatory cytokine secretion in CD8+ T cells activated by ligation of CD3 and CD28. Pentose phosphate pathway inhibition also prevented CD8+ T cell–mediated antigen-specific neuronal injury in vitro and in both an adoptive transfer–based cuprizone model of demyelination and in mice with experimental autoimmune encephalomyelitis. Notably, transcriptional profiling of CNS-infiltrating CD8+ T cells in patients with MS indicated increased pentose phosphate pathway engagement, suggesting that this pathway is involved in CD8+ T cell–mediated injury of axons and neurons in the demyelinated CNS. Inhibiting the pentose phosphate pathway disrupts CD8+ T cell metabolic reprogramming and effector functions, suggesting that such inhibition may serve as a therapeutic strategy to prevent neurodegeneration in patients with progressive MS.

Authors

Ethan M. Grund, Benjamin D.S. Clarkson, Susanna Pucci, Maria S. Westphal, Carolina Muniz Partida, Sara A. Muhammad, Charles L. Howe

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Figure 10

Systemic treatment with 6AN attenuates functional deficits in EAE.

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Systemic treatment with 6AN attenuates functional deficits in EAE. (A) B...
(A) Body weights of mice treated by daily i.p. injection of different 6AN doses. Red, 10 mg/kg; yellow, 5 mg/kg; blue, 2.5 mg/kg; turquoise, 1.25 mg/kg; N = 4 mice per condition; each symbol represents 1 animal; zero indicates animal removed from study due to euthanasia criteria or death. (B) Daily disability scores in mice following induction of MOG EAE. Red, EAE mice treated with vehicle (N, 25); yellow, EAE mice treated every other day with 6AN (5 mg/kg) (N, 30) starting at day 11; green triangles, treatment day; symbols show median ± 95% CI. (C) Peak EAE score and AUC for the data shown in B; vehicle-treated (red) or 6AN-treated (yellow). N = 25 vehicle-treated and N = 30 6AN-treated mice for peak disease score; N = 25 vehicle-treated and N = 25 6AN-treated mice for AUC (animals removed based on euthanasia criteria or death not included). Each symbol represents 1 animal. Two-way ANOVA with a mixed-effects model and Šidák’s pairwise comparison was used for repeated measures analysis; Mann-Whitney U test was used for comparison of VEH and 6AN groups; *P < 0.05, **P < 0.01, ***P < 0.001, ****P < 0.0001. Data are shown as mean ± 95% CI.