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Phosphatase PRL-3 is a direct regulatory target of TGFbeta in colon cancer metastasis.


ABSTRACT: Metastasis causes most deaths from cancer yet mechanistic understanding and therapeutic options remain limited. Overexpression of the phosphatase PRL-3 (phosphatase of regenerating liver) is associated with metastasis of colon cancer. Here, we show that PRL-3 is a direct target of signaling by TGF?, which is broadly implicated in progression and metastasis. We found that suppression of PRL-3 expression by TGF? was mediated by Smad-dependent inhibition of PRL-3 transcription at the level of promoter activity. PRL-3 activation stimulated PI3K/AKT signaling that caused resistance to stress-induced apoptosis. PRL-3 overexpression promoted metastatic colonization in an orthotopic mouse model of colon cancer, whereas PRL-3 knockdown reduced metastatic potential. Altered metastatic phenotypes were not derivative of primary tumor development or local invasion but could be attributed to PRL-3-mediated cell survival. Our findings suggest that inhibiting PRL-3 expression might be an important mechanism through which TGF? suppresses metastasis in colon cancer. In addition, our findings suggest that loss of TGF? signaling, which occurs commonly during colon cancer progression, is sufficient to activate a PRL-3-mediated cell survival pathway that can selectively promote metastasis. Therefore, a major implication of our findings is that PRL-3 antagonists may offer significant value for antimetastatic therapy in patients with colon cancer.

SUBMITTER: Jiang Y 

PROVIDER: S-EPMC3064433 | biostudies-literature | 2011 Jan

REPOSITORIES: biostudies-literature

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Phosphatase PRL-3 is a direct regulatory target of TGFbeta in colon cancer metastasis.

Jiang Yanjun Y   Liu Xiao-Qiong XQ   Rajput Ashwani A   Geng Liying L   Ongchin Melanie M   Zeng Qi Q   Taylor Gregory S GS   Wang Jing J  

Cancer research 20101116 1


Metastasis causes most deaths from cancer yet mechanistic understanding and therapeutic options remain limited. Overexpression of the phosphatase PRL-3 (phosphatase of regenerating liver) is associated with metastasis of colon cancer. Here, we show that PRL-3 is a direct target of signaling by TGFβ, which is broadly implicated in progression and metastasis. We found that suppression of PRL-3 expression by TGFβ was mediated by Smad-dependent inhibition of PRL-3 transcription at the level of promo  ...[more]

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