MARK2/MARK3 kinases are catalytic co-dependencies of YAP/TAZ in human cancer.
Olaf KlingbeilDamianos SkopelitisClaudia TonelliToyoki YoshimotoAktan AlpsoyMaria C PanepintoFrancesca MinicozziJoseph R MerrillAmanda M CafieroDisha AggarwalSuzanne RussoTaehoon HaOsama E DemerdashTse-Luen WeeDavid L SpectorScott K LyonsDavid A TuvesonPaolo CifaniChristopher R VakocPublished in: Cancer discovery (2024)
The Hippo signaling pathway is commonly dysregulated in human cancer, which leads to a powerful tumor dependency on the YAP/TAZ transcriptional coactivators. Here, we used paralog co-targeting CRISPR screens to identify the kinases MARK2/3 as absolute catalytic requirements for YAP/TAZ function in diverse carcinoma and sarcoma contexts. Underlying this observation is direct MARK2/3-dependent phosphorylation of NF2 and YAP/TAZ, which effectively reverses the tumor suppressive activity of the Hippo module kinases LATS1/2. To simulate targeting of MARK2/3, we adapted the CagA protein from H. pylori as a catalytic inhibitor of MARK2/3, which we show can regress established tumors in vivo. Together, these findings reveal MARK2/3 as powerful co-dependencies of YAP/TAZ in human cancer; targets that may allow for pharmacology that restores Hippo pathway-mediated tumor suppression.
Keyphrases
- endothelial cells
- papillary thyroid
- signaling pathway
- squamous cell
- genome wide
- induced pluripotent stem cells
- pluripotent stem cells
- helicobacter pylori
- gene expression
- pi k akt
- epithelial mesenchymal transition
- oxidative stress
- transcription factor
- crispr cas
- dna methylation
- squamous cell carcinoma
- drug delivery
- lps induced
- toll like receptor
- induced apoptosis
- young adults
- binding protein
- protein kinase