<i>MicroRNA-148a</i> Suppresses Tumor Cell Invasion and Metastasis by Downregulating <i>ROCK1</i> in Gastric Cancer

Zheng, Biqiang; Liang, Linhui; Wang, Chunmeng; Huang, Shenglin; Cao, Xi; Zha, Rujing; Liu, Li; Jia, Deshui; Tian, Qiang; Wu, Jianghong; Ye, Yanwei; Wang, Qifeng; Long, Ziwen; Zhou, Ye; Du, Chunyan; He, Xianghuo; Shi, Yingqiang

doi:10.1158/1078-0432.ccr-11-1714

Cited by 249 publications

(212 citation statements)

References 38 publications

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“…These papilloma data thus link NF-κβ with increased DNA mutations/chromosomal instability 25,39 following p53 loss and associated p21 inhibition 47 [below]; and indirectly link ROCK2-mediated NF-κβ to stromal remodelling 25 thus accounting for effects previously observed on expression of ECM molecules such as tenascin C. 48,49 One consequence of p53 loss leading to an altered matrix may involve downregulated microRNAs, 34 such as miR-200 which regulates cell-cell adhesion molecules 35 and effected ROCK signalling in gastric cancer. 36 Of note, p53-mediated miR-200 expression depended upon AKT levels, 37 consistent with p53 loss driving malignant conversion in trigenic HK1.ras/fos/Pten flx carcinogenesis. 20 Early NF-κβ expression coupled to p53 down regulation in K14.ROCK er /HK1.ras 1205 papillomas 25,26 would account for increased proliferation, possibly via the NF-κβ responsive element regulating cyclin D 43 and, in sync with ROCK2/ras signalling, 12 add to the increasing pool of cycling cells susceptible to DNA damage/chromosomal re-arrangements.…”

Section: Discussionmentioning

confidence: 79%

“…loss and the lack of DNA repair would give rise to additional mutations in highly proliferative cells giving a susceptibility to malignant conversion. 32,33 Indeed, as outlined below, these K14.ROCK er /HK1.ras 1205 data suggest a mechanism involving p53 loss which links ROCK2-associated NF-κβ deregulation to the matrix remodelling that drives progression [34][35][36][37] when coupled to GSK3β/β-catenin/WNT signalling effects. 5 20,23,41 All wdSCCs exhibited persistent basal-layer p21 expression, which exactly paralleled K14.ROCK er /pMypt1 expression suggesting that increased p21 is a common response to ras/ROCK er /ROCK2 activities.…”

Section: Rock2 Activation Co-operates With Ras Ha To Elicit Malignantmentioning

confidence: 94%

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ROCK2/rasHa co-operation induces malignant conversion via p53 loss, elevated NF-κB and tenascin C-associated rigidity, but p21 inhibits ROCK2/NF-κB-mediated progression

et al. 2016

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ROCK2/rasHa cooperation induce malignant conversion via p53 loss, elevated NF-κβ and tenascin C-associated rigidity but p21 inhibits ROCK2/NF-κβ-mediated progression. Oncogene, 36, pp. 2529Oncogene, 36, pp. -2542Oncogene, 36, pp. . (doi:10.1038Oncogene, 36, pp. /onc.2016 This is the author's final accepted version.There may be differences between this version and the published version. You are advised to consult the publisher's version if you wish to cite from it.http://eprints.gla.ac.uk/129163/ Malignancy depended on ROCK er /p-Mypt1 expression, as cessation of 4HT-treatment induced disorganised tissue architecture and p21-associated differentiation in wdSCCs; yet tenascin C retention in connective tissue ECM suggests the rigidity laid down for conversion persists. Novel papilloma outgrowths appeared expressing intense, basal-layer p21 which confined endogenous ROCK2/p-Mypt1/NF-κβ to supra-basal layers, and was paralleled by restored basal-layer p53. In later SCCs, 4HT-cessation became irrelevant as endogenous ROCK2 expression increased, driving progression via p21 loss, elevated NF-κβ expression and tenascin C-associated rigidity; with p-Mypt1 inactivation/actinomyosin-mediated contractility to facilitate invasion. However, p21-associated inhibition of early-stage malignant progression and the intense expression in papilloma outgrowths, identifies a novel, significant antagonism between p21 and ras Ha /ROCK2/NF-κβ signalling in skin 3 carcinogenesis. Collectively these data show that ROCK2 activation induces malignancy in ras Ha -initiated/promoted papillomas in the context of p53 loss and novel NF-κβ expression; whilst increased tissue rigidity and cell motility/contractility help mediate tumour progression.4

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Section: Discussionmentioning

confidence: 79%

Section: Rock2 Activation Co-operates With Ras Ha To Elicit Malignantmentioning

confidence: 94%

ROCK2/rasHa co-operation induces malignant conversion via p53 loss, elevated NF-κB and tenascin C-associated rigidity, but p21 inhibits ROCK2/NF-κB-mediated progression

et al. 2016

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“…36 Generally, miR-148a functions as a tumor suppressor in cancer cells. [33][34][35][36] However, in most studies, miR-148a was detected in specimens of tissues or cell lines. There is limited research involving exosomes containing miR-148a.…”

Section: Discussionmentioning

confidence: 99%

Characterization of exosomal RNAs derived from human gastric cancer cells by deep sequencing

Ren

Zhou

et al. 2017

Tumour Biol.

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Exosomes secreted from the cell to the extracellular environment play an important role in intercellular communication.Next-generation sequencing technology, which has achieved great development recently, allows us to detect more complete data and gain even deeper analyses of RNA transcriptomes. In our research, we extracted exosomes from different gastric cancer cell lines and immortalized normal gastric mucosal epithelial cell line and examined the amounts of exosomal proteins and RNAs. Our data showed that the secreted amount of cancer cell-derived exosomes, which contain proteins and RNAs, was much higher than that of normal cell-derived exosomes. Moreover, next-generation sequencing technology confirmed the presence of small non-coding RNAs in exosomes. Based on publicly available databases, we classified small non-coding RNAs. According to the microRNA profiles of exosomes, hsa-miR-21-5p and hsa-miR-30a-5p were two of the most abundant sequences among all libraries. The expression levels of the two microRNAs, miR-100 and miR-148a, in exosomes were validated through reverse transcription polymerase chain reaction. The reverse transcription polymerase chain reaction result, consistent with the trend of sequencing result, indicated a significant difference in exosomes between gastric cancer and gastric mucosal epithelial cell lines. We also predicted novel microRNA candidates but they need to be validated. This research provided an atlas of small noncoding RNA in exosomes and may make a little contribution to the understanding of exosomal RNA composition and finding parts of differential expression of RNAs in exosomes.

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“…For in vivo experimental metastasis assay, 0.4 Â 10 6 cancer cells (per mouse, n ¼ 6 for each group) were transplanted into peripheral circulation of 5-week-old male nude mice through the lateral tail vein (24). After 8 weeks, mice were dissected to determine the number of metastatic colonies within the lungs (24).…”

Section: In Vivo Growth and Metastasis Assaymentioning

confidence: 99%

“…After 8 weeks, mice were dissected to determine the number of metastatic colonies within the lungs (24).…”

Section: In Vivo Growth and Metastasis Assaymentioning

confidence: 99%

miRNA-145 Targets v-ets Erythroblastosis Virus E26 Oncogene Homolog 1 to Suppress the Invasion, Metastasis, and Angiogenesis of Gastric Cancer Cells

Zheng

et al. 2013

Molecular Cancer Research

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Recent evidence shows that v-ets erythroblastosis virus E26 oncogene homolog 1 (Ets1) is implicated in tumor development and progression. However, the clinical potentials and underlying mechanisms of Ets1 in gastric cancer progression and metastasis remain largely unknown. In this study, Ets1 immunostaining was identified in 56 of 84 (66.7%) gastric cancer tissues, which was correlated with tumor invasion and metastasis. In gastric cancer specimens and cell lines, miRNA-145 (miR-145) was downregulated and inversely correlated with Ets1 expression. Bioinformatics analysis and luciferase reporter assay revealed that miR-145 directly targeted the 3 0 -untranslated region (3 0 -UTR) of Ets1 mRNA. Overexpression or knockdown of miR-145 responsively altered both the mRNA and protein levels of Ets1 and its downstream genes, matrix metalloproteinase (MMP-1)-1 and -9, in gastric cancer cell lines SGC-7901 and MKN-45. Ectopic expression of miR-145 suppressed the invasion, metastasis, and angiogenesis of SGC-7901 and MKN-45 cells in vitro and in vivo. In addition, the effects of miR-145 on Ets1 expression, migration, invasion, and angiogenesis were rescued by restoration of Ets1 expression in these cells. Furthermore, anti-miR-145 inhibitor promoted the migration, invasion, and angiogenesis, whereas siRNAmediated Ets1 knockdown phenocopied the effects of miR-145 overexpression in gastric cancer cells. These results show that miR-145 suppresses Ets1 expression via the binding site in the 3 0 -UTR, thus inhibiting the invasion, metastasis, and angiogenesis of gastric cancer cells. Mol Cancer Res; 11(2); 182-93. Ó2012 AACR.

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MicroRNA-148a Suppresses Tumor Cell Invasion and Metastasis by Downregulating ROCK1 in Gastric Cancer

Cited by 249 publications

References 38 publications

ROCK2/rasHa co-operation induces malignant conversion via p53 loss, elevated NF-κB and tenascin C-associated rigidity, but p21 inhibits ROCK2/NF-κB-mediated progression

ROCK2/rasHa co-operation induces malignant conversion via p53 loss, elevated NF-κB and tenascin C-associated rigidity, but p21 inhibits ROCK2/NF-κB-mediated progression

Characterization of exosomal RNAs derived from human gastric cancer cells by deep sequencing

miRNA-145 Targets v-ets Erythroblastosis Virus E26 Oncogene Homolog 1 to Suppress the Invasion, Metastasis, and Angiogenesis of Gastric Cancer Cells

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