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Androgen signaling restricts glutaminolysis to drive sex-specific Th17 metabolism in allergic airway inflammation
Nowrin U. Chowdhury, … , Jeffrey C. Rathmell, Dawn C. Newcomb
Nowrin U. Chowdhury, … , Jeffrey C. Rathmell, Dawn C. Newcomb
Published October 15, 2024
Citation Information: J Clin Invest. 2024;134(23):e177242. https://doi.org/10.1172/JCI177242.
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Research Article Immunology Pulmonology

Androgen signaling restricts glutaminolysis to drive sex-specific Th17 metabolism in allergic airway inflammation

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Abstract

Female individuals have an increased prevalence of many Th17 cell–mediated diseases, including asthma. Androgen signaling decreases Th17 cell–mediated airway inflammation, and Th17 cells rely on glutaminolysis. However, it remains unclear whether androgen receptor (AR) signaling modifies glutamine metabolism to suppress Th17 cell–mediated airway inflammation. We show that Th17 cells from male humans and mice had decreased glutaminolysis compared with female individuals, and that AR signaling attenuated Th17 cell mitochondrial respiration and glutaminolysis in mice. Using allergen-induced airway inflammation mouse models, we determined that females had a selective reliance upon glutaminolysis for Th17-mediated airway inflammation, and that AR signaling attenuated glutamine uptake in CD4+ T cells by reducing expression of glutamine transporters. In patients with asthma, circulating Th17 cells from men had minimal reliance upon glutamine uptake compared to Th17 cells from women. AR signaling thus attenuates glutaminolysis, demonstrating sex-specific metabolic regulation of Th17 cells with implications for Th17 or glutaminolysis targeted therapeutics.

Authors

Nowrin U. Chowdhury, Jacqueline-Yvonne Cephus, Emely Henriquez Pilier, Melissa M. Wolf, Matthew Z. Madden, Shelby N. Kuehnle, Kaitlin E. McKernan, Erin Q. Jennings, Emily N. Arner, Darren R. Heintzman, Channing Chi, Ayaka Sugiura, Matthew T. Stier, Kelsey Voss, Xiang Ye, Kennedi Scales, Evan S. Krystofiak, Vivek D. Gandhi, Robert D. Guzy, Katherine N. Cahill, Anne I. Sperling, R. Stokes Peebles Jr., Jeffrey C. Rathmell, Dawn C. Newcomb

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Figure 8

Males with severe asthma have decreased dependence on glutamine uptake in circulating CD4+ T cell subsets compared with females with severe asthma.

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Males with severe asthma have decreased dependence on glutamine uptake i...
(A) Model of SCENITH protocol on frozen PBMCs restimulated overnight with anti-CD3/CD28/CD2. (B–D) Glucose dependence, mitochondrial dependence, and glutamine uptake dependence in males and females measured using SCENITH inhibitors (2-deoxyglucose, oligomycin, and V9302, respectively) in (B) CD4+ TEMs (defined as Live, CD3+, CD4+, CD8–, CD45RA–, and CCR7–), (C) CCR4+ CD4+ TEMs, and (D) TEM 17 cells (defined as B and CCR4+, CCR6+). Data show mean ± SEM, *P < 0.05, **P < 0.01, or P value as shown; Mann-Whitney U test. See Supplemental Figure 13 and Supplemental Table 4.

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