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<scp>MYO10</scp> contributes to the malignant phenotypes of colorectal cancer via <scp>RACK1</scp> by activating integrin/Src/<scp>FAK</scp> signaling

Haibin Ou, Lili Wang, Ziyao Xi, Hui Shen, Yaofei Jiang, Fuxiang Zhou, Yu Liu, Yunfeng Zhou

2022Cancer Science19 citationsDOIOpen Access PDF

Abstract

Liver metastases still remain a major cause of colorectal cancer (CRC) patient death. MYO10 is upregulated in several tumor types; however, its significance and the underlying mechanism in CRC are not entirely clear. Here, we found that MYO10 was highly expressed in CRC tumor tissues, especially in liver metastasis tissues. MYO10 knockout reduced CRC cell proliferation, invasion, and migration in vitro and CRC metastasis in vivo. We identified RACK1 by LC-MS/MS and demonstrated that MYO10 interacts with and stabilizes RACK1. Mechanistically, MYO10 promotes CRC cell progression and metastasis via ubiquitination-mediated RACK1 degradation and integrin/Src/FAK signaling activation. Therefore, the MYO10/RACK1/integrin/Src/FAK axis may play an important role in CRC progression and metastasis.

Topics & Concepts

MetastasisProto-oncogene tyrosine-protein kinase SrcCancer researchIntegrinDownregulation and upregulationColorectal cancerFocal adhesionSignal transductionCancerUbiquitinCell migrationCell biologyBiologyMedicineCellInternal medicineGeneticsBiochemistryGeneCell Adhesion Molecules ResearchPeptidase Inhibition and AnalysisUbiquitin and proteasome pathways
<scp>MYO10</scp> contributes to the malignant phenotypes of colorectal cancer via <scp>RACK1</scp> by activating integrin/Src/<scp>FAK</scp> signaling | Litcius