The Hippo pathway kinase Lats2 prevents DNA damage-induced apoptosis through inhibition of the tyrosine kinase c-Abl

Reuven, Nina; Adler, Julia; Meltser, V; Shaul, Yoav D.

doi:10.1038/cdd.2013.83

Cited by 64 publications

(61 citation statements)

References 58 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…In crowded cells, where the Hippo pathway is functional, activated Lats phosphorylates c-Abl to downregulate its kinase activity, 32 suggesting the domination of Hippo over the DNA damage pathway. Hippo pathway cross-talks with other signaling pathways to orchestrate cell-fate decisions was lately reinforced in studies outlining the connection of Hippo components with the PI(3)K-mTOR pathway, Wnt/β-catenin pathway, and mechanotransduction.…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

c-Abl antagonizes the YAP oncogenic function

et al. 2014

Self Cite

View full text Add to dashboard Cite

YES-associated protein (YAP) is a central transcription coactivator that functions as an oncogene in a number of experimental systems. However, under DNA damage, YAP activates pro-apoptotic genes in conjunction with p73. This program switching is mediated by c-Abl (Abelson murine leukemia viral oncogene) via phosphorylation of YAP at the Y357 residue (pY357). YAP as an oncogene coactivates the TEAD (transcriptional enhancer activator domain) family transcription factors. Here we asked whether c-Abl regulates the YAP-TEAD functional module. We found that DNA damage, through c-Abl activation, specifically depressed YAP-TEAD-induced transcription. Remarkably, c-Abl counteracts YAP-induced transformation by interfering with the YAP-TEAD transcriptional program. c-Abl induced TEAD1 phosphorylation, but the YAP-TEAD complex remained unaffected. In contrast, TEAD coactivation was compromised by phosphomimetic YAP Y357E mutation but not Y357F, as demonstrated at the level of reporter genes and endogenous TEAD target genes. Furthermore, YAP Y357E also severely compromised the role of YAP in cell transformation, migration, anchorage-independent growth, and epithelial-to-mesenchymal transition (EMT) in human mammary MCF10A cells. These results suggest that YAP pY357 lost TEAD transcription activation function. Our results demonstrate that YAP pY357 inactivates YAP oncogenic function and establish a role for YAP Y357 phosphorylation in cell-fate decision.

show abstract

Section: Discussionmentioning

confidence: 99%

“…pCDNA c-Abl Δ1-81 and pCDNA c-Abl Δ1-81 K290H (kinase dead) have been previously described. 32 PCDNA3-HA-TEAD1 was cloned from pPGS-3HA-TEAD1, kindly provided by KL Guan (Addgene, Cambridge, MA, USA; plasmid no. 33050).…”

Section: Methodsmentioning

confidence: 99%

c-Abl antagonizes the YAP oncogenic function

et al. 2014

Self Cite

View full text Add to dashboard Cite

show abstract

“…Finally, overexpression of mutant c-Abl constructs, which lack LATS2 phosphosite or harbor a point mutation in SH3 domain, overcame LATS2 inhibition and resulted in apoptosis in densely plated cells upon DNA damage. Taken together, these observations by Reuven et al 1 suggest that when DNA damage is induced in dense cells, activated LATS2 binds and inhibits c-Abl-mediating phosphorylation of p73Y99 and YAPY357, resulting in reduced apoptosis and cytoprotection (Figure 1). Importantly, under these conditions, LATS2 can also bind and phosphorylate YAP at S127, resulting in its cytoplasmic sequestration, thus YAP becomes unable to bind and coactivate p73 to enhance its apoptotic function.…”

mentioning

confidence: 63%

“…In this issue of CDD, Reuven et al 1 provide an elegant mechanism by which LATS2, a core component of the Hippo pathway, impedes DNA damage-induced apoptosis through inhibition of c-Abl. By dissecting signaling events upon g-irradiation of sparse and dense cell, the authors revealed a dialogue between Hippo signaling members and DNA damage response (DDR) proteins.…”

mentioning

confidence: 99%

See 1 more Smart Citation

Hippo signaling: to die or not to die

Aqeilan

2013

Cell Death Differ

View full text Add to dashboard Cite

Hyaluronan Degradation Promotes Cancer via Hippo‐YAP Signaling: An Intervention Point for Cancer Therapy

Ooki

Hatakeyama

2020

BioEssays

View full text Add to dashboard Cite

High‐molecular‐weight hyaluronan acts as a ligand of the tumor‐suppressive Hippo signal, whereas degradation of hyaluronan from a high‐molecular‐weight form to a low‐molecular‐weight forms by hyaluronidase 2 inhibits Hippo signal activation and thereby activates the pro‐oncogenic transcriptional coactivator yes‐associated protein (YAP), which creates a cancer‐predisposing microenvironment and drives neoplastic transformation of cells through both cell‐autonomous and non‐cell‐autonomous mechanisms. In fact, accumulation of low‐molecular‐weight hyaluronan in tissue stroma is observed in many types of cancers. Since inhibition of YAP activity suppresses tumor growth in vivo, pharmacological intervention of the Hippo‐YAP signal is an attractive approach for future drug development. In this review, pharmacological intervention of excessive hyaluronan degradation as a novel approach for inhibition of the Hippo‐YAP signal is also discussed. Development of hyaluronidase inhibitors may provide novel therapeutic strategies for human malignant tumors.

show abstract

The Hippo pathway kinase Lats2 prevents DNA damage-induced apoptosis through inhibition of the tyrosine kinase c-Abl

Cited by 64 publications

References 58 publications

c-Abl antagonizes the YAP oncogenic function

c-Abl antagonizes the YAP oncogenic function

Hippo signaling: to die or not to die

Hyaluronan Degradation Promotes Cancer via Hippo‐YAP Signaling: An Intervention Point for Cancer Therapy

Contact Info

Product

Resources

About