Suppressed miR-424 expression via upregulation of target gene Chk1 contributes to the progression of cervical cancer

Xu, Jianrong; Li, Y; Wang, F; Wang, X; Cheng, Bei; Ye, F; Xie, Xing; Zhou, Caiyun; Lü, Weiguo

doi:10.1038/onc.2012.121

Cited by 199 publications

(180 citation statements)

References 43 publications

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“…[22][23][24][25][26] In contrast to the well-known utility of Chk1 inhibitors in sensitizing tumors to chemotherapy agents, 23,27,28 Chk1 overexpression or downexpression also occurs in some types of tumors, including breast cancer, ovarian cancer, cervical cancer, and neuroblastoma. 22,[29][30][31][32][33] In our study, we found Chk1 mRNA and protein levels were upregulated in colorectal cancer tissues compared with paired normal tissues, and positively correlated with CCNB1 expression. We hypothesized that CCNB1 might serve as a Chk1-induced oncogene in colorectal cancer.…”

Section: Discussionsupporting

confidence: 49%

Chk1-induced CCNB1 overexpression promotes cell proliferation and tumor growth in human colorectal cancer

Fang

Liang

et al. 2014

Cancer Biology & Therapy

136

115

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Section: Discussionsupporting

confidence: 49%

Chk1-induced CCNB1 overexpression promotes cell proliferation and tumor growth in human colorectal cancer

Fang

Liang

et al. 2014

Cancer Biology & Therapy

136

115

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“…Of the four most effective miRNAs identified, let-7c and miR200b belong to the let-7 and miRNA-200s families, respectively, of which the tumour-suppressor roles in TICs have been well appreciated 8,23,46 , while miR-222 and miR-424 were first identified as TIC-suppressing miRNAs despite a tumoursuppressor role of both miRNAs has been identified in a number of cancers other than HCC [47][48][49][50] . Paradoxically, miR-222 was previously regarded as oncogene in some reports because it could enhance some tumour cell growth by targeting CDK inhibitor p27 in vitro, and was found to be upregulated in HCC and some other types of cancers 42,51,52 ; however, its tumourpromoting role was rarely validated in vivo.…”

Section: Discussionmentioning

confidence: 99%

PBX3 is targeted by multiple miRNAs and is essential for liver tumour-initiating cells

Han

Zhao

et al. 2015

Nat Commun

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Tumour-initiating cells (TICs) are advocated to constitute the sustaining force to maintain and renew fully established malignancy; however, the molecular mechanisms responsible for these properties are elusive. We previously demonstrated that voltage-gated calcium channel a2d1 subunit marks hepatocellular carcinoma (HCC) TICs. Here we confirm directly that a2d1 is a HCC TIC surface marker, and identify let-7c, miR-200b, miR-222 and miR-424 as suppressors of a2d1 þ HCC TICs. Interestingly, all the four miRNAs synergistically target PBX3, which is sufficient and necessary for the acquisition and maintenance of TIC properties. Moreover, PBX3 drives an essential transcriptional programme, activating the expression of genes critical for HCC TIC stemness including CACNA2D1, EpCAM, SOX2 and NOTCH3. In addition, the expression of CACNA2D1 and PBX3 mRNA is predictive of poor prognosis for HCC patients. Collectively, our study identifies an essential signalling pathway that controls the switch of HCC TIC phenotypes.

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“…Although the current view in the field is that ATM and ATR signaling inhibits tumor progression rather than promoting cancer (Bartkova et al, 2006;Gorgoulis et al, 2005;Halazonetis et al, 2008), there has been a number of recent reports of overexpression of ATM or ATR, or of activation of the downstream pathways in different cancers (Albiges et al, 2014;Bhatia et al, 2013;Hoglund et al, 2011;Mahajan et al, 2012;Sarmento et al, 2015;Tho et al, 2012;Vadnais et al, 2012;Verlinden et al, 2007;Xu et al, 2013) (see poster). Of note, the addition of an extra allele of Chk1 has even been found to promote Ras-or E1A-mediated transformation more efficiently in comparison to such transformation of wild-type littermates (Lopez-Contreras et al, 2012), suggesting that the ATR-Chk1 axis has a pro-malignant transformation role.…”

Section: Box 1 Relevance Of Atm and Atr Signaling In Cancermentioning

confidence: 99%

ATM and ATR signaling at a glance

Awasthi

Foiani

Kumar

2015

Journal of Cell Science

232

228

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There was an error published in J. Cell Sci. 128, 4255-4262.An incorrect citation and reference was given for the last sentence in Box 2. The correct citation and reference are: A recent review provides a detailed update on ATM and ATR inhibitors, and their potential as drug targets (Weber and Ryan, 2015).Weber, A.M. and Ryan, A.J. (2015). ATM and ATR as therapeutic targets in cancer. Pharmacol Ther. 149, 124-138.The authors apologise to the readers for any confusion that this error might have caused. Although the role of both ATM and ATR in DNA repair, cell cycle regulation and apoptosis have been well studied, both still remain in the focus of current research activities owing to their role in cancer. Recent advances in the field suggest that these proteins have an additional function in maintaining cellular homeostasis under both stressed and non-stressed conditions. In this Cell Science at a Glance article and the accompanying poster, we present an overview of recent advances in ATR and ATM research with emphasis on that into the modes of ATM and ATR activation, the different signaling pathways they participate in -including those that do not involve DNA damage -and highlight their relevance in cancer. 1285

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Suppressed miR-424 expression via upregulation of target gene Chk1 contributes to the progression of cervical cancer

Cited by 199 publications

References 43 publications

Chk1-induced CCNB1 overexpression promotes cell proliferation and tumor growth in human colorectal cancer

Chk1-induced CCNB1 overexpression promotes cell proliferation and tumor growth in human colorectal cancer

PBX3 is targeted by multiple miRNAs and is essential for liver tumour-initiating cells

ATM and ATR signaling at a glance

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