Distinct super-enhancer elements differentially controlIl2ragene expression in a cell-type specific fashion

Author:

Spolski Rosanne,Li Peng,Chandra Vivek,Shin Boyoung,Liu Chengyu,Oh Jangsuk,Ren Min,Enomoto Yutaka,West Erin E.,Christensen Stephen,Wan Edwin C.K.,Ge Meili,Lin Jian-Xin,Vijayanand Pandurangan,Rothenberg Ellen V.,Leonard Warren J.

Abstract

SummaryThe IL-2 receptor α-chain (IL-2Rα/CD25) is constitutively expressed on DN2/DN3 thymocytes and Treg cells but induced by IL-2 on mature T and NK cells.Il2raexpression is regulated by a super-enhancer extensively bound by STAT5 in mature T cells. Here, we demonstrate that STAT5 cooperates with Notch to induce/maintainIl2ra/CD25 expression in DN2/DN3 cells. Moreover, we systematically investigated CD25 regulation using a series of mice with deletions spanning STAT5 binding elements. Deleting the upstream super-enhancer region mainly affected constitutive CD25 expression on DN2/DN3 thymocytes and Tregs, whereas deleting an intronic region primarily decreased IL-2-induced CD25 on peripheral T and NK cells. Thus, distinct elements preferentially control constitutive versus inducible expression in a cell-type-specific manner, with the MED1 coactivator co-localizing with specific STAT5 binding sites. Moreover, the intronic region was a dominant element whose deletion altered the structure throughout the super-enhancer in mature T cells. These results demonstrate differential functions for distinct super-enhancer elements, thereby indicating ways to manipulate CD25 expression in a cell-type specific fashion.

Publisher

Cold Spring Harbor Laboratory

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