GATA2 and PU.1 Collaborate To Activate the Expression of the Mouse Gene, Encoding FcεRIβ, Through Distinct Mechanisms

Overview

Journal Mol Cell Biol

Specialty Cell Biology

Date 2019 Sep 11

PMID 31501274

Citations 8

Authors

Shinya Ohmori

Yasushi Ishijima

Suzuka Numata

Mai Takahashi

Masataka Sekita

Taichi Sato

Keisuke Chugun

Masayuki Yamamoto

Kinuko Ohneda

Affiliations

Soon will be listed here.

Abstract

GATA factors GATA1 and GATA2 and ETS factor PU.1 are known to function antagonistically during hematopoietic development. In mouse mast cells, however, these factors are coexpressed and activate the expression of the gene encoding the β chain of the high-affinity IgE receptor (FcεRI). The present study showed that these factors cooperatively regulate gene expression through distinct mechanisms. Although GATA2 and PU.1 contributed almost equally to gene expression, gene ablation experiments revealed that simultaneous knockdown of both factors showed neither a synergistic nor an additive effect. A chromatin immunoprecipitation analysis showed that they shared DNA binding to the +10.4-kbp region downstream of the gene with chromatin looping factor LDB1, whereas the proximal -60-bp region was exclusively bound by GATA2 in a mast cell-specific manner. Ablation of PU.1 significantly reduced the level of GATA2 binding to both the +10.4-kbp and -60-bp regions. Surprisingly, the deletion of the +10.4-kbp region by genome editing completely abolished the gene expression as well as the cell surface expression of FcεRI. These results suggest that PU.1 and LDB1 play central roles in the formation of active chromatin structure whereas GATA2 directly activates the promoter.

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