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JUN — MYLIP
Text-mined interactions from Literome
Talotta et al., Oncogene 2009
(Cell Transformation, Neoplastic) :
Here, we show that the miRNA
miR-21 , which represents the most frequently upregulated oncomir in solid tumors, is
induced by
AP-1 in response to RAS
Tili et al., Carcinogenesis 2010
:
We further establish that the downregulation of AP-1 activity by resveratrol is
miR-663 dependent and that the effects of resveratrol on both
AP-1 activity and JunB levels are dose
dependent
Dai et al., Hum Reprod 2011
(Pre-Eclampsia) :
DNA precipitation assays and luciferase reporter analysis were used to evaluate the
regulation of
miR-155 by
AP-1 and NF-?B ... Both
JunB/FosB and p65 were
increased in placenta from women with severe pre-eclampsia versus a normal pregnancy, with elevated expression of
miR-155 ( P < 0.05 )
Zhou et al., Proc Natl Acad Sci U S A 2011
(Inflammation) :
Overexpression of PPARa significantly attenuated the
AP-1 mediated
miR-21 expression ... These results demonstrate a unique mechanism by which OSS induces
AP-1 dependent
miR-21 expression, which directly targets PPARa to inhibit its expression, thereby allowing activation of AP-1 and the promotion of monocyte adhesion
Acunzo et al., Oncogene 2012
(Carcinoma, Non-Small-Cell Lung...) :
Here, we further investigated this pathway and showed that miR-130a, expressed at low level in lung cancer cell lines, by targeting MET was able to reduce TRAIL resistance in NSCLC cells through the
c-Jun mediated downregulation of
miR-221 and miR-222
Arora et al., PloS one 2011
(Lung Neoplasms) :
When
c-Jun N-terminal kinase activity was inhibited using SP600125, expression of
miR-26b was
induced following ?-irradiation in H1299 cells
Zhou et al., PloS one 2012
:
In addition, we found that miR-222 might regulate the phosphorylation of cAMP response element binding protein ( CREB ) through PTEN, and
c-Jun activation might
enhance the
miR-222 expression
Song et al., PloS one 2012
:
Stretch upregulates miR-21 expression at least in part at the transcription level and
AP-1 is
essential for stretch induced
miR-21 expression
Shen et al., PloS one 2013
(Cell Transformation, Neoplastic) :
Down-regulation of
miR-21 and up-regulations of Pdcd44 or Spry1
blocked the arsenite induced activations of
JNK/c-Jun or ERK/NF-?B, indicating that knockdown of miR-21 inhibits feedback of ERK activation and JNK activation via increases of Pdcd4 and Spry1 protein levels, respectively
Cheng et al., J Biol Chem 2013
(Alzheimer Disease) :
Moreover, we also showed that
activator protein-1 regulates the transcription of miR-144 and the up-regulation of
miR-144 at least partially
induces the suppression of the ADAM10 protein in the presence of Aß
Sonkoly et al., Oncogenesis 2012
:
We identify
c-JUN , a key effector of the HH pathway, as a novel direct
target for
miR-203 in vivo
Yu et al., Cell death & disease 2013
(Cell Transformation, Neoplastic...) :
Further, we discovered that attenuated CTGF mediated upregulation of
miR-18b was
dependent on the increased binding of transcription factors Jun
proto-oncogene (C-Jun) and v-Myc myelocytomatosis viral oncogene homolog ( C-Myc ) to miR-18b promoter region via phosphoinositide 3-kinase (PI3K)/AKT pathway ... Our studies are the first to demonstrate that reduced CTGF as an unfavorable prognosis factor mediates the
activation of
miR-18b , an oncomir directly suppresses CTGF expression, by
PI3K/AKT/C-Jun and C-Myc and promotes cell growth of NPC
Onyeagucha et al., Exp Cell Res 2013
(Colonic Neoplasms) :
Altogether, these data demonstrate that the expression of
miR-155 is regulated by S100P and is
dependent on RAGE activation and stimulation of
AP-1
Yang et al., PloS one 2013
(Carcinoma, Hepatocellular...) :
In turn, TGFß decreases miR-127 expression by enhancing
c-Jun mediated inhibition of
miR-127 promoter activity
Kang et al., Mol Biol Rep 2013
:
miR-21 could significantly
promote adipocyte differentiation, increase adiponectin mRNA and protein expression, while decrease
AP-1 protein level