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Pparα knockout in mice increases the Th17 development by facilitating the IKKα/RORγt and IKKα/Foxp3 complexes

Ping Wei, Wei Kou, Juan Fu, Zuojia Chen, Fan Pan

2023Communications Biology10 citationsDOIOpen Access PDF

Abstract

T cells (Tregs) are balanced through numerous molecular regulators, particularly metabolic factors, and their alteration causes immune dysregulation. Herein, we report that peroxisome proliferator of activated receptor-alpha (Pparα), a lipid metabolism regulator, suppresses Th17 differentiation. We demonstrated that Pparα ablation improves Th17 and pro-Th17 factor HIF-1α by enhancing the expression and nuclear localization of NFκB-activator IκB kinase-alpha (IKKα). Unexpectedly, we found that IKKα directly interacts with RORγt and enhances the expression of Il17a gene. Meanwhile, IKKα also interacts with Foxp3, leading to the post-translational regulation of Foxp3 by elevating its proteasomal degradation, and influencing Th17 development. Pparα deficiency leads to enhanced Th17 development in vivo and is associated with enhanced pathology in a murine experimental autoimmune encephalomyelitis (EAE) model. Overall, our data indicate that Pparα may serve as a potential therapeutic target for autoimmune and inflammatory diseases.

Topics & Concepts

RAR-related orphan receptor gammaFOXP3Experimental autoimmune encephalomyelitisInterleukin 17IκB kinaseCell biologyPeroxisome proliferator-activated receptorNuclear receptorImmune systemNF-κBTranscription factorCancer researchChemistryBiologySignal transductionReceptorImmunologyBiochemistryGeneNF-κB Signaling PathwaysImmune Cell Function and InteractionPeroxisome Proliferator-Activated Receptors
Pparα knockout in mice increases the Th17 development by facilitating the IKKα/RORγt and IKKα/Foxp3 complexes | Litcius