河马信号通路
生物
效应器
细胞生物学
转录因子
调解人
信号转导
癌变
再生(生物学)
雅普1
加压器
遗传学
抑制因子
癌症
基因
作者
Jing Cai,Kyungsuk Choi,Hongde Li,Katiuska Daniela Pulgar Prieto,Yonggang Zheng,Duojia Pan
出处
期刊:Genes & Development
[Cold Spring Harbor Laboratory]
日期:2022-11-01
卷期号:36 (21-24): 1119-1128
被引量:14
标识
DOI:10.1101/gad.350127.122
摘要
The Hippo-YAP signaling pathway plays a critical role in development, homeostasis, regeneration, and tumorigenesis by converging on YAP, a coactivator for the TEAD family DNA-binding transcription factors, to regulate downstream transcription programs. Given its pivotal role as the nuclear effector of the Hippo pathway, YAP is indispensable in multiple developmental and tissue contexts. Here we report that the essentiality of YAP in liver and lung development can be genetically bypassed by simultaneous inactivation of the TEAD corepressor VGLL4. This striking antagonistic epistasis suggests that the major physiological function of YAP is to antagonize VGLL4. We further show that the YAP-VGLL4 antagonism plays a widespread role in regulating Hippo pathway output beyond normal development, as inactivation of Vgll4 dramatically enhanced intrahepatic cholangiocarcinoma formation in Nf2-deficient livers and ameliorated CCl4-induced damage in normal livers. Interestingly, Vgll4 expression is temporally regulated in development and regeneration and, in certain contexts, provides a better indication of overall Hippo pathway output than YAP phosphorylation. Together, these findings highlight the central importance of VGLL4-mediated transcriptional repression in Hippo pathway regulation and inform potential strategies to modulate Hippo signaling in cancer and regenerative medicine.
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