Tumor protein 53-induced nuclear protein 1 expression is repressed by miR-155, and its restoration inhibits pancreatic tumor development

Gironella, Meritxell; Seux, Mylène; Xie, Min; Cano, Carla E.; Tomasini, Richard; Gommeaux, Julien; García, Stéphane; Nowak, Jonathan A.; Yeung, Man Lung; Jeang, Kuan‐Teh; Chaix, Amandine; Fazli, Ladan; Motoo, Yoshiharu; Wang, Qing; Rocchi, Palma; Russo, Antonio; Gleave, Martin; Dagorn, Jean–Charles; Iovanna, Juan; Carrier, Alice; Pébusque, Marie‐Josèphe; Dusetti, Nelson

doi:10.1073/pnas.0703942104

Cited by 496 publications

(390 citation statements)

References 42 publications

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“…Oncogenic properties of miR-155 are attributed to its anti-apoptotic function through a blockade of caspase-3 activity or suppressing proapoptotic genes such as TP53BP1 (Gironella et al, 2007;Ovcharenko et al, 2007), and promote cell proliferation by downregulating the SOCS1 gene (Jiang et al, 2010), or activate AKT signaling via down-regulation of tumor suppressors including PTEN, PDCD4 and SHIP1 (Yamanaka et al, 2009). Besides, miR-155 is regulated by the transforming growth factor-beta (TGF-β)/Smad4 pathway and plays a role in cell invasion by targeting RhoA (Kong et al, 2008).…”

Section: Has Prognostic Value In Patients With Nsclcs and Digestive Smentioning

confidence: 99%

MicroRNA-155 Expression has Prognostic Value in Patients with Non-small Cell Lung Cancer and Digestive System Carcinomas

Xu¹,

Zhu²,

Zhang³

et al. 2013

Asian Pacific Journal of Cancer Prevention

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Section: Has Prognostic Value In Patients With Nsclcs and Digestive Smentioning

confidence: 99%

MicroRNA-155 Expression has Prognostic Value in Patients with Non-small Cell Lung Cancer and Digestive System Carcinomas

Xu¹,

Zhu²,

Zhang³

et al. 2013

Asian Pacific Journal of Cancer Prevention

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“…It has been reported that TP53INP1 is a cancer suppressor, which is associated with an oncogenic microRNA miR-155 [22,23]. And repressing TP53INP1 significantly enhanced the ability of the CD133 À cells to initiate spheroid formation [24], but whether silencing TP53INP1 could increase the population of CD133 + cells is unknown.…”

Section: Down-regulation Of Tp53inp1 Promotes the Acquisition Of Csc-mentioning

confidence: 99%

MiR‐155 targets TP53INP1 to regulate liver cancer stem cell acquisition and self‐renewal

Liu

Kong

et al. 2015

FEBS Letters

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a b s t r a c tIn liver cancer, miR-155 up-regulation can regulate cancer-cell invasion. However, whether miR-155 expression is associated with liver cancer stem cells (CSCs) remains unknown. Here, we show that miR-155 expression is up-regulated in tumor spheres. Knock-down of miR-155 resulted in suppression of tumor sphere formation, through a decrease in the proportion of CD90 + and CD133 + CSCs and in the expression of Oct4, whereas miR-155 overexpression had the opposite effect. TP53INP1 was determined to be involved in the CSCs-like properties that were regulated by miR-155. Thus, miR-155 may play an important role in promoting the generation of stem cell-like cells and their selfrenewal by targeting the gene TP53INP1.

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“…7,8 Our laboratory demonstrated that TP53INP1 is a tumor suppressor on the basis of the following observations: (i) TP53INP1 deficient mice present with an increased susceptibility to tumor development; (ii) TP53INP1 is lost at very early stages of pancreatic carcinogenesis through a mechanism involving the oncogenic miR-155 microRNA and (iii) when TP53INP1 expression is restored in pancreatic cells, it suppresses xenograft growth by increasing apoptotic cell death through a caspase-dependent mechanism. 3,9,10 More recently, in an attempt to decipher the molecular mechanism by which TP53INP1 induces cell death, we found that it interacts with a family of proteins involved in autophagy. Such interaction had already been reported for the TP53INP1 paralog TP53INP2 (also known as DOR) that shows 30% of amino-acid identity with TP53INP1.…”

mentioning

confidence: 99%

“…One of the p53 target genes is TP53INP1 (tumor protein 53-induced nuclear protein 1). [3][4][5][6] p53-dependent expression of TP53INP1 is triggered in response to several stress agents such as mutagens, ethanol, heat shock or conditions promoting reactive oxygen species formation (i.e., exposure to UV light or g-irradiation). 4,6 TP53INP1 interacts with kinases, HIPK2 and PKCd, which in turn phosphorylate p53 creating a positive feedback loop between p53 and TP53INP1.…”

mentioning

confidence: 99%

TP53INP1, a tumor suppressor, interacts with LC3 and ATG8-family proteins through the LC3-interacting region (LIR) and promotes autophagy-dependent cell death

et al. 2012

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TP53INP1 (tumor protein 53-induced nuclear protein 1) is a tumor suppressor, whose expression is downregulated in cancers from different organs. It was described as a p53 target gene involved in cell death, cell-cycle arrest and cellular migration. In this work, we show that TP53INP1 is also able to interact with ATG8-family proteins and to induce autophagy-dependent cell death. In agreement with this finding, we observe that TP53INP1, which is mainly nuclear, relocalizes in autophagosomes during autophagy where it is eventually degraded. TP53INP1-LC3 interaction occurs via a functional LC3-interacting region (LIR). Inactivating mutations of this sequence abolish TP53INP1-LC3 interaction, relocalize TP53INP1 in autophagosomes and decrease TP53INP1 ability to trigger cell death. Interestingly, TP53INP1 binds to ATG8-family proteins with higher affinity than p62, suggesting that it could partially displace p62 from autophagosomes, modifying thereby their composition. Moreover, silencing the expression of autophagy related genes (ATG5 or Beclin-1) or inhibiting caspase activity significantly decreases cell death induced by TP53INP1. These data indicate that cell death observed after TP53INP1-LC3 interaction depends on both autophagy and caspase activity. We conclude that TP53INP1 could act as a tumor suppressor by inducing cell death by caspasedependent autophagy. Increased resistance to cell death participates in pancreatic cancer progression. Cells unable to undergo self elimination accumulate mutations and epigenetic modifications that in turn induce uncontrolled replication. 1 Various concomitant mechanisms exist in normal cells to induce death and, as consequence, a number of known cell-death regulators are missing in cancer cells. One of the most studied is the tumor suppressor TP53, which is inactivated in 450% of pancreatic tumors. 2 p53 induces cell death by both direct permeabilization of the outer mitochondrial membrane or translocation to the nucleus where it activates the transcription of several target genes. One of the p53 target genes is TP53INP1 (tumor protein 53-induced nuclear protein 1). 3-6 p53-dependent expression of TP53INP1 is triggered in response to several stress agents such as mutagens, ethanol, heat shock or conditions promoting reactive oxygen species formation (i.e., exposure to UV light or g-irradiation). 4,6 TP53INP1 interacts with kinases, HIPK2 and PKCd, which in turn phosphorylate p53 creating a positive feedback loop between p53 and TP53INP1. 7,8 Our laboratory demonstrated that TP53INP1 is a tumor suppressor on the basis of the following observations: (i) TP53INP1 deficient mice present with an increased susceptibility to tumor development; (ii) TP53INP1 is lost at very early stages of pancreatic carcinogenesis through a mechanism involving the oncogenic miR-155 microRNA and (iii) when TP53INP1 expression is restored in pancreatic cells, it suppresses xenograft growth by increasing apoptotic cell death through a caspase-dependent mechanism. 3,9,10 More recently, in an attempt t...

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Tumor protein 53-induced nuclear protein 1 expression is repressed by miR-155, and its restoration inhibits pancreatic tumor development

Cited by 496 publications

References 42 publications

MicroRNA-155 Expression has Prognostic Value in Patients with Non-small Cell Lung Cancer and Digestive System Carcinomas

MicroRNA-155 Expression has Prognostic Value in Patients with Non-small Cell Lung Cancer and Digestive System Carcinomas

MiR‐155 targets TP53INP1 to regulate liver cancer stem cell acquisition and self‐renewal

TP53INP1, a tumor suppressor, interacts with LC3 and ATG8-family proteins through the LC3-interacting region (LIR) and promotes autophagy-dependent cell death

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