VGLL4 targets a TCF4–TEAD4 complex to coregulate Wnt and Hippo signalling in colorectal cancer

Shi, Jianzhong; Li, Chuanchuan; Hao, Qian; Miao, Haofei; Zhang, Lei; Lin, Li; Zhou, Zhaocai

doi:10.1038/ncomms14058

Cited by 121 publications

(120 citation statements)

References 37 publications

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“…Consistent with this, genome-wide surveys of TCF or β-cat binding in vertebrates reveal the presence of several TF binding site motifs besides the TCF site consensus 1, 30, 39, 77, 78 . Other TFs have been reported to co-localize with TCFs 36, 38, 39, 79, 80 , and in the cases of Cdx2 79 , Sp5/8 81 , and TEAD TFs 82 , a co-dependency with TCFs or β-cat for chromatin association has been reported. In addition, TCF binding to chromatin is highly cell type specific 36 and is dynamic over time in the same cell type 38, 39 .…”

Section: Tcfs and Wnt Target Locationmentioning

confidence: 98%

Wnt target genes and where to find them

Ramakrishnan

Cadigan

2017

F1000Res

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Wnt/β-catenin signaling is highly conserved throughout metazoans, is required for numerous essential events in development, and serves as a stem cell niche signal in many contexts. Misregulation of the pathway is linked to several human pathologies, most notably cancer. Wnt stimulation results in stabilization and nuclear import of β-catenin, which then acts as a transcriptional co-activator. Transcription factors of the T-cell family (TCF) are the best-characterized nuclear binding partners of β-catenin and mediators of Wnt gene regulation. This review provides an update on what is known about the transcriptional activation of Wnt target genes, highlighting recent work that modifies the conventional model. Wnt/β-catenin signaling regulates genes in a highly context-dependent manner, and the role of other signaling pathways and TCF co-factors in this process will be discussed. Understanding Wnt gene regulation has served to elucidate many biological roles of the pathway, and we will use examples from stem cell biology, metabolism, and evolution to illustrate some of the rich Wnt biology that has been uncovered.

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Section: Tcfs and Wnt Target Locationmentioning

confidence: 98%

Wnt target genes and where to find them

Ramakrishnan

Cadigan

2017

F1000Res

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“…VGLL4 binding to TEAD4 inhibits TEAD4-TCF4 driven target gene expression as it does for TEAD-YAP/TAZ target gene expression, but does not compete with TCF4 for TEAD binding. Instead, VGLL4 inhibition of TEAD4-TCF4 transcriptional activity is due to formation of a TEAD4/TCF4/VGLL4 ternary complex [41]. The p160 family of steroid receptor coactivators was also identified to interact with TEAD.…”

Section: Regulation Of Tead By Coactivatorsmentioning

confidence: 99%

Regulation of the Hippo Pathway Transcription Factor TEAD

Lin

Park

Guan

2017

Trends in Biochemical Sciences

260

206

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The TEAD transcription factor family is best known for transcriptional output of the Hippo signaling pathway and has been implicated in processes such as development, cell growth and proliferation, tissue homeostasis, and regeneration. Our understanding of the functional importance of TEADs has increased dramatically since its initial discovery three decades ago. The majority of our knowledge of TEADs is in the context of Hippo signaling as nuclear DNA binding proteins passively activated by YAP and TAZ, transcription coactivators downstream of the Hippo pathway. However, recent studies suggest that TEAD itself is actively regulated. Here, we highlight evidence demonstrating Hippo-independent regulation of TEADs and the potential impacts these studies may have on new cancer therapeutics.

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“…Complexes of YAP1/TEAD and betacatenin/TCF have been detected and a subset of Wnt/ beta-catenin target genes may rely on nuclear YAP1/ TEAD complexes for full induction in response to Wnt ligands (18). These data suggest that in addition to the complex interactions between Wnt and Hippo signaling components in the cytoplasm, both pathways can cooperate in the nucleus to execute gene expression programs that affect proliferation, organ size, tissue repair, and tumor growth.…”

Section: Cell-cell Adhesionmentioning

confidence: 91%

“…These data highlight how interactions between pathways can result in, at first glance, paradoxical findings: e.g., the signaling of pro-tumorigenic pathways Wnt and YAP1 can have opposing effects on tumor growth (18). Furthermore, in some experimental systems a majority of beta-catenin regulated genes are dependent on WWTR1 (TAZ) (20).…”

Section: Cell-cell Adhesionmentioning

confidence: 99%

“…Furthermore, in some experimental systems a majority of beta-catenin regulated genes are dependent on WWTR1 (TAZ) (20). Although this reliance on Wnt target genes appears to be dependent on cytoplasmic interactions between betacatenin and WWTR1 (TAZ), co-regulation of a subset of Wnt target genes can also be achieved by the cooperation of beta-catenin/TCF and YAP1/WWTR1/TEAD transcriptional complexes (18). On the other hand, Park et al observed in their experiments that activation of noncanonical Wnt signaling-i.e., Wnt signaling independent of beta-catenin-resulted in increased levels of WWTR1 and YAP1, increased expression of YAP1 target genes, increased TEAD-dependent migration and differentiation, and expression of Wnt signaling inhibitors, all of which leads to reduced canonical Wnt signaling (21).…”

Section: Cell-cell Adhesionmentioning

confidence: 99%

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