作者
Alessandra Mancino, Alberto Termanini, Iros Barozzi, Serena Ghisletti, Renato Ostuni, Elena Prosperini, Keiko Ozato, Gioacchino Natoli
发表日期
2015/2/15
期刊
Genes & development
卷号
29
期号
4
页码范围
394-408
出版商
Cold Spring Harbor Lab
简介
The transcription factor (TF) interferon regulatory factor 8 (IRF8) controls both developmental and inflammatory stimulus-inducible genes in macrophages, but the mechanisms underlying these two different functions are largely unknown. One possibility is that these different roles are linked to the ability of IRF8 to bind alternative DNA sequences. We found that IRF8 is recruited to distinct sets of DNA consensus sequences before and after lipopolysaccharide (LPS) stimulation. In resting cells, IRF8 was mainly bound to composite sites together with the master regulator of myeloid development PU.1. Basal IRF8–PU.1 binding maintained the expression of a broad panel of genes essential for macrophage functions (such as microbial recognition and response to purines) and contributed to basal expression of many LPS-inducible genes. After LPS stimulation, increased expression of IRF8, other IRFs, and AP-1 family …
引用总数
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