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CIP4 targeted to recruit GTP-Cdc42 involving in invadopodia formation via NF-κB signaling pathway promotes invasion and metastasis of CRC

Zhiyan Hu, Jiaxian Zhu, Yidan Ma, Ting Long, Ling-Fang Gao, Yan Zhong, Xiaoyan Wang, Zuguo Li

2022Molecular Therapy — Oncolytics17 citationsDOIOpen Access PDF

Abstract

, while the overexpression of CIP4 promoted invadopodia formation and matrix degradation ability. We then identified GTP-Cdc42 as a directly interactive protein of CIP4, which was upregulated and recruited by CIP4. Furthermore, activated NF-κB signaling pathway was found in CIP4 overexpression of CRC cells contributing to invadopodia formation, while the inhibition of either CIP4 or Cdc42 led to the suppression of the NF-κB pathway and resulted in a decreased quantity of invadopodia. Our findings suggested that CIP4 targets to recruit GTP-Cdc42 and directly combines with it to accelerate invadopodia formation and function by activating NF-κB signaling pathway, thus promoting CRC infiltration and metastasis.

Topics & Concepts

InvadopodiaCDC42Cell biologyCancer researchChemistrySignal transductionMetastasisBiologyCancerGeneticsCellular Mechanics and InteractionsCell Adhesion Molecules ResearchSignaling Pathways in Disease