The role of MerTK in promoting cell migration is enhanced by the oncogenic Ras/IL‐33 signaling axis

The role of MerTK in promoting cell migration is enhanced by the oncogenic Ras/IL‐33 signaling axis

Ras genes are frequently mutated in many cancer types; however, there are currently no conclusively effective anticancer drugs against Ras‐induced cancer. Therefore, the downstream effectors of Ras signaling need to be identified for the development of promising novel therapeutic approaches. We prev...

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Veröffentlicht in:The FEBS journal 2022-04, Vol.289 (7), p.1950-1967
Hauptverfasser: Ohta, Satoshi, Tago, Kenji, Kuchimaru, Takahiro, Funakoshi‐Tago, Megumi, Horie, Hisanaga, Aoki‐Ohmura, Chihiro, Matsugi, Jitsuhiro, Yanagisawa, Ken
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Anticancer properties
Antineoplastic drugs
Antitumor agents
c-Mer Tyrosine Kinase - genetics
c-Mer Tyrosine Kinase - metabolism
Cancer
Cell adhesion & migration
Cell migration
Cell Movement
colorectal cancer
Colorectal carcinoma
Genes, ras
Humans
IL‐33
Interleukin-33 - genetics
Interleukins
Kinases
Malignancy
MerTK
Mice
Mutation
Oncogenes
Phosphorylation
Protein-tyrosine kinase receptors
Ras
Signaling
Transformed cells
Tyrosine
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Zusammenfassung:Ras genes are frequently mutated in many cancer types; however, there are currently no conclusively effective anticancer drugs against Ras‐induced cancer. Therefore, the downstream effectors of Ras signaling need to be identified for the development of promising novel therapeutic approaches. We previously reported that oncogenic Ras induced the expression of NF‐HEV/IL‐33, a member of the interleukin‐1 family, and showed that intracellular IL‐33 was required for oncogenic Ras‐induced cellular transformation. In the present study, we demonstrated that the c‐Mer proto‐oncogene tyrosine kinase (MerTK), a receptor tyrosine kinase, played essential roles in oncogenic Ras/IL‐33 signaling. The expression of MerTK was enhanced in transformed NIH‐3T3 cells by the expression of oncogenic Ras, H‐Ras (G12V), in an IL‐33‐dependent manner. In human colorectal cancer tissues, MerTK expression also correlated with IL‐33 expression. The knockdown of IL‐33 or MerTK effectively attenuated the migration of NIH‐3T3 cells transformed by H‐Ras (G12V) and A549, LoVo, and HCT116 cells harboring an oncogenic K‐Ras mutation. Furthermore, the suppression of Ras‐induced cell migration by the knockdown of IL‐33 was rescued by the enforced expression of MerTK. The present results also revealed that MerTK was effectively phosphorylated in NIH‐3T3 cells transformed by Ras (G12V). Ras signaling was essential for the tyrosine phosphorylation of MerTK, and the kinase activity of MerTK was indispensable for accelerating cell migration. Collectively, the present results reveal a novel role for MerTK in cancer malignancy, which may be utilized to develop novel therapeutic strategies that target Ras‐transformed cells. Oncogenic Ras alters intracellular signals to transform cells and cause cancer. Here, we described a novel oncogenic Ras signaling where the expression of MerTK is induced by oncogenic Ras in an IL‐33‐dependent manner. MerTK is strongly phosphorylated by oncogenic Ras. Subsequently, IL‐33, MerTK, and the kinase activity of MerTK are indispensable for oncogenic Ras‐induced cell migration.
ISSN:1742-464X
1742-4658
DOI:10.1111/febs.16271