%0 Journal Article
%T A CTCF-binding site in the Mdm1-Il22-Ifng locus shapes cytokine expression profiles and plays a critical role in early Th1 cell fate specification.
%A Liu C
%A Nagashima H
%A Fernando N
%A Bass V
%A Gopalakrishnan J
%A Signorella S
%A Montgomery W
%A Lim AI
%A Harrison O
%A Reich L
%A Yao C
%A Sun HW
%A Brooks SR
%A Jiang K
%A Nagarajan V
%A Zhao Y
%A Jung S
%A Phillips R
%A Mikami Y
%A Lareau CA
%A Kanno Y
%A Jankovic D
%A Aryee MJ
%A Pękowska A
%A Belkaid Y
%A O'Shea J
%A Shih HY
%J Immunity
%V 57
%N 5
%D 2024 May 14
%M 38697116
%F 43.474
%R 10.1016/j.immuni.2024.04.007
%X Cytokine expression during T cell differentiation is a highly regulated process that involves long-range promoter-enhancer and CTCF-CTCF contacts at cytokine loci. Here, we investigated the impact of dynamic chromatin loop formation within the topologically associating domain (TAD) in regulating the expression of interferon gamma (IFN-γ) and interleukin-22 (IL-22); these cytokine loci are closely located in the genome and are associated with complex enhancer landscapes, which are selectively active in type 1 and type 3 lymphocytes. In situ Hi-C analyses revealed inducible TADs that insulated Ifng and Il22 enhancers during Th1 cell differentiation. Targeted deletion of a 17 bp boundary motif of these TADs imbalanced Th1- and Th17-associated immunity, both in vitro and in vivo, upon Toxoplasma gondii infection. In contrast, this boundary element was dispensable for cytokine regulation in natural killer cells. Our findings suggest that precise cytokine regulation relies on lineage- and developmental stage-specific interactions of 3D chromatin architectures and enhancer landscapes.