Foxp3 Depends on Ikaros for Control of Regulatory T Cell Gene Expression and Function

Overview

Journal Elife

Specialty Biology

Date 2024 Apr 24

PMID 38655862

Authors

Rajan M Thomas

Matthew C Pahl

Liqing Wang

Struan F A Grant

Wayne W Hancock

Andrew D Wells

Affiliations

Soon will be listed here.

Abstract

Ikaros is a transcriptional factor required for conventional T cell development, differentiation, and anergy. While the related factors Helios and Eos have defined roles in regulatory T cells (Treg), a role for Ikaros has not been established. To determine the function of Ikaros in the Treg lineage, we generated mice with Treg-specific deletion of the Ikaros gene (). We find that Ikaros cooperates with Foxp3 to establish a major portion of the Treg epigenome and transcriptome. Ikaros-deficient Treg exhibit Th1-like gene expression with abnormal production of IL-2, IFNg, TNFa, and factors involved in Wnt and Notch signaling. While -Treg-cko mice do not develop spontaneous autoimmunity, Ikaros-deficient Treg are unable to control conventional T cell-mediated immune pathology in response to TCR and inflammatory stimuli in models of IBD and organ transplantation. These studies establish Ikaros as a core factor required in Treg for tolerance and the control of inflammatory immune responses.

Citing Articles

Cis-Regulatory Element and Transcription Factor Circuitry Required for Cell-Type Specific Expression of FOXP3.

Umhoefer J, Arce M, Whalen S, Dajani R, Goudy L, Kasinathan S bioRxiv. 2024; .

PMID: 39282425 PMC: 11398386. DOI: 10.1101/2024.08.30.610436.

Foxp3 depends on Ikaros for control of regulatory T cell gene expression and function.

Thomas R, Pahl M, Wang L, Grant S, Hancock W, Wells A Elife. 2024; 12.

PMID: 38655862 PMC: 11042806. DOI: 10.7554/eLife.91392.

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