Interleukin 21 Drives a Hypermetabolic State and CD4+ T-Cell-Associated Pathogenicity in Chronic Intestinal Inflammation

Adebowale O Bamidele; Shravan K Mishra; Guilherme Piovezani Ramos; Petra Hirsova; Emily E Klatt; Leena M Abdelrahman; Mary R Sagstetter; Heidi M Davidson; Patrick J Fehrenbach; Lucía Valenzuela-Pérez; Hyun Se Kim Lee; Song Zhang; Abner Aguirre Lopez; Ahmed T Kurdi; Maria S Westphal; Michelle M Gonzalez; Joseph M Gaballa; Robyn Laura Kosinsky; Hee Eun Lee; Thomas C Smyrk; Glenn Bantug; Naomi M Gades; William A Faubion Jr

doi:10.1053/j.gastro.2024.01.026

Interleukin 21 Drives a Hypermetabolic State and CD4⁺ T-Cell-Associated Pathogenicity in Chronic Intestinal Inflammation

Gastroenterology. 2024 May;166(5):826-841.e19. doi: 10.1053/j.gastro.2024.01.026. Epub 2024 Jan 23.

Authors

Adebowale O Bamidele¹, Shravan K Mishra², Guilherme Piovezani Ramos³, Petra Hirsova³, Emily E Klatt⁴, Leena M Abdelrahman², Mary R Sagstetter³, Heidi M Davidson³, Patrick J Fehrenbach², Lucía Valenzuela-Pérez³, Hyun Se Kim Lee³, Song Zhang⁵, Abner Aguirre Lopez², Ahmed T Kurdi³, Maria S Westphal³, Michelle M Gonzalez³, Joseph M Gaballa³, Robyn Laura Kosinsky³, Hee Eun Lee⁶, Thomas C Smyrk⁶, Glenn Bantug⁷, Naomi M Gades⁸, William A Faubion Jr³

Affiliations

¹ Immunometabolism and Mucosal Immunity Laboratory, Division of Gastroenterology and Hepatology, Mayo Clinic, Rochester, Minnesota; Department of Immunology, Mayo Clinic, Rochester, Minnesota. Electronic address: Bamidele.Adebowale@mayo.edu.
² Immunometabolism and Mucosal Immunity Laboratory, Division of Gastroenterology and Hepatology, Mayo Clinic, Rochester, Minnesota.
³ Division of Gastroenterology and Hepatology, Mayo Clinic, Rochester, Minnesota.
⁴ Department of Immunology, Mayo Clinic, Rochester, Minnesota.
⁵ Mayo Clinic Metabolomics Core, Mayo Clinic, Rochester, Minnesota; Department of Cardiovascular Medicine, Mayo Clinic, Rochester, Minnesota.
⁶ Department of Laboratory Medicine and Pathology, Mayo Clinic, Rochester, Minnesota.
⁷ Immunobiology Laboratory, Department of Biomedicine, University Hospital of Basel, Basel, Switzerland.
⁸ Department of Comparative Medicine, Mayo Clinic, Scottsdale, Arizona.

PMID: 38266738
PMCID: PMC11034723 (available on 2025-05-01)
DOI: 10.1053/j.gastro.2024.01.026

Abstract

Background & aims: Incapacitated regulatory T cells (Tregs) contribute to immune-mediated diseases. Inflammatory Tregs are evident during human inflammatory bowel disease; however, mechanisms driving the development of these cells and their function are not well understood. Therefore, we investigated the role of cellular metabolism in Tregs relevant to gut homeostasis.

Methods: Using human Tregs, we performed mitochondrial ultrastructural studies via electron microscopy and confocal imaging, biochemical and protein analyses using proximity ligation assay, immunoblotting, mass cytometry and fluorescence-activated cell sorting, metabolomics, gene expression analysis, and real-time metabolic profiling utilizing the Seahorse XF analyzer. We used a Crohn's disease single-cell RNA sequencing dataset to infer the therapeutic relevance of targeting metabolic pathways in inflammatory Tregs. We examined the superior functionality of genetically modified Tregs in CD4⁺ T-cell-induced murine colitis models.

Results: Mitochondria-endoplasmic reticulum appositions, known to mediate pyruvate entry into mitochondria via voltage-dependent anion channel 1 (VDAC1), are abundant in Tregs. VDAC1 inhibition perturbed pyruvate metabolism, eliciting sensitization to other inflammatory signals reversible by membrane-permeable methyl pyruvate supplementation. Notably, interleukin (IL) 21 diminished mitochondria-endoplasmic reticulum appositions, resulting in enhanced enzymatic function of glycogen synthase kinase 3 β, a putative negative regulator of VDAC1, and a hypermetabolic state that amplified Treg inflammatory response. Methyl pyruvate and glycogen synthase kinase 3 β pharmacologic inhibitor (LY2090314) reversed IL21-induced metabolic rewiring and inflammatory state. Moreover, IL21-induced metabolic genes in Tregs in vitro were enriched in human Crohn's disease intestinal Tregs. Adoptively transferred Il21r^-/- Tregs efficiently rescued murine colitis in contrast to wild-type Tregs.

Conclusions: IL21 triggers metabolic dysfunction associated with Treg inflammatory response. Inhibiting IL21-induced metabolism in Tregs may mitigate CD4⁺ T-cell-driven chronic intestinal inflammation.

Keywords: Inflammatory Bowel Disease; Interleukins; Mitochondria-ER Appositions; Pyruvate; Regulatory T Cells.

Publication types

Research Support, Non-U.S. Gov't
Research Support, N.I.H., Extramural

MeSH terms

Animals
CD4-Positive T-Lymphocytes / immunology
CD4-Positive T-Lymphocytes / metabolism
Chronic Disease
Colitis* / immunology
Colitis* / metabolism
Colitis* / pathology
Crohn Disease / immunology
Crohn Disease / metabolism
Crohn Disease / pathology
Humans
Interleukins / metabolism
Interleukins / pharmacology
Mice
Mice, Inbred C57BL
Mitochondria* / metabolism
T-Lymphocytes, Regulatory / immunology
Voltage-Dependent Anion Channel 1 / genetics
Voltage-Dependent Anion Channel 1 / metabolism

Substances

Interleukins
Voltage-Dependent Anion Channel 1

Abstract

Publication types

MeSH terms

Substances

Grants and funding