Dezhen Peng scite author profile

Tumor metastasis is the most cause of high mortality for cancer patients. Identification of novel factors that modulate tumor cell migration is of great significance for therapeutic strategies. Here, we find that the ubiquitin-specific protease 8 (Usp8) promotes tumor cell migration through activating the c-Jun N-terminal kinase (JNK) pathway. Genetic epistasis analyses uncover Usp8 acts upstream of Tak1 to control the JNK pathway. Consistently, biochemical results reveal that Usp8 binds Tak1 to remove ubiquitin modification from Tak1, leading to its stabilization. In addition, human USP8 also triggers tumor cell migration and activates the JNK pathway. Finally, we show that knockdown of USP8 in human breast cancer cells suppresses cell migration. Taken together, our findings demonstrate that a conserved Usp8-Tak1-JNK axis promotes tumor cell migration, and providing USP8 as a potential therapeutic target for cancer treatment.

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Inhibition of the transcription factor ZNF281 by SUFU to suppress tumor cell migration

Deng

Peng

Xiao

et al. 2022

Cell Death Differ

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Non-invasive detection and localization of genitourinary cancers using urinary sediment DNA methylomes and copy number profiles

Xu¹,

Ge²,

Guan³

et al. 2020

European Urology Open Science

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Targetable genetic alterations screen by broad, hybrid capture-based next generation sequencing in driver-negative advanced malignant tumor facilitated personalized therapy.

Zhang

Hou

Mao

et al. 2015

JCO

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Dezhen Peng

Preclinical efficacy against acute myeloid leukaemia of SH1573, a novel mutant IDH2 inhibitor approved for clinical trials in China

Usp8 promotes tumor cell migration through activating the JNK pathway

Inhibition of the transcription factor ZNF281 by SUFU to suppress tumor cell migration

Non-invasive detection and localization of genitourinary cancers using urinary sediment DNA methylomes and copy number profiles

Targetable genetic alterations screen by broad, hybrid capture-based next generation sequencing in driver-negative advanced malignant tumor facilitated personalized therapy.

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