| Literature DB >> 28122243 |
Xiong-Jun Wang1, Yunbo Qiao2, Minzhe M Xiao3, Lingbo Wang4, Jun Chen5, Wenjian Lv4, Li Xu6, Yan Li6, Yumei Wang3, Ming-Dian Tan3, Chao Huang3, Jinsong Li4, Ting C Zhao7, Zhaoyuan Hou8, Naihe Jing9, Y Eugene Chin10.
Abstract
LIF promotes self-renewal of mouse embryonic stem cells (mESCs), and in its absence, the cells differentiate. LIF binds to the LIF receptor (LIFR) and activates the JAK-STAT3 pathway, but it remains unknown how the receptor complex triggers differentiation or self-renewal. Here, we report that the LIFR cytoplasmic domain contains a self-renewal domain within the juxtamembrane region and a differentiation domain within the C-terminal region. The differentiation domain contains four SPXX repeats that are phosphorylated by MAPK to restrict STAT3 activation; the self-renewal domain is characterized by a 3K motif that is acetylated by p300. In mESCs, acetyl-LIFR undergoes homodimerization, leading to STAT3 hypo- or hyper-activation depending on the presence or absence of gp130. LIFR-activated STAT3 restricts differentiation via cytokine induction. Thus, LIFR acetylation and serine phosphorylation differentially promote stem cell self-renewal and differentiation.Entities:
Keywords: LIF; LIFR; MAPK; STAT3; acetylation; differentiation; embryonic stem cells; phosphorylation; self-renewal; signaling
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Year: 2017 PMID: 28122243 DOI: 10.1016/j.celrep.2016.12.081
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423