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Misshapen Disruption Cooperates with RasV12 to Drive Tumorigenesis.


ABSTRACT: Although RAS family genes play essential roles in tumorigenesis, effective treatments targeting RAS-related tumors are lacking, partly because of an incomplete understanding of the complex signaling crosstalk within RAS-related tumors. Here, we performed a large-scale genetic screen in Drosophila eye imaginal discs and identified Misshapen (Msn) as a tumor suppressor that synergizes with oncogenic Ras (RasV12) to induce c-Jun N-terminal kinase (JNK) activation and Hippo inactivation, then subsequently leads to tumor overgrowth and invasion. Moreover, ectopic Msn expression activates Hippo signaling pathway and suppresses Hippo signaling disruption-induced overgrowth. Importantly, we further found that Msn acts downstream of protocadherin Fat (Ft) to regulate Hippo signaling. Finally, we identified msn as a Yki/Sd target gene that regulates Hippo pathway in a negative feedback manner. Together, our findings identified Msn as a tumor suppressor and provide a novel insight into RAS-related tumorigenesis that may be relevant to human cancer biology.

SUBMITTER: Kong D 

PROVIDER: S-EPMC8070713 | biostudies-literature | 2021 Apr

REPOSITORIES: biostudies-literature

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Misshapen Disruption Cooperates with <i>Ras<sup>V12</sup></i> to Drive Tumorigenesis.

Kong Du D   Lu Jin-Yu JY   Li Xiaoqin X   Zhao Sihua S   Xu Wenyan W   Fang Jinan J   Wang Xing X   Ma Xianjue X  

Cells 20210414 4


Although <i>RAS</i> family genes play essential roles in tumorigenesis, effective treatments targeting <i>RAS</i>-related tumors are lacking, partly because of an incomplete understanding of the complex signaling crosstalk within <i>RAS</i>-related tumors. Here, we performed a large-scale genetic screen in <i>Drosophila</i> eye imaginal discs and identified <i>Misshapen</i> (<i>Msn</i>) as a tumor suppressor that synergizes with oncogenic <i>Ras</i> (<i>Ras<sup>V12</sup></i>) to induce c-Jun N-t  ...[more]

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