MicroRNA in Glioblastoma: An Overview

Banelli, Barbara; Forlani, Alessandra; Allemanni, Giorgio; Morabito, Anna; Pistillo, Maria Pia; Romani, Massimo

doi:10.1155/2017/7639084

Cited by 125 publications

(121 citation statements)

References 210 publications

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“…Recent studies have highlighted the pivotal roles of miRNAs in regulating GBM development and their potential as targets for cancer therapy . In order to reveal the regulatory mechanism of HMGB3 in GBM, we first sought to determine whether any relevant miRNAs regulate HMGB3.…”

Section: Resultsmentioning

confidence: 99%

“…Recent studies have highlighted the pivotal roles of miRNAs in regulating GBM development and their potential as targets for cancer therapy. 26 In order to reveal the regulatory mechanism of HMGB3 in GBM, we first sought to determine whether any relevant miRNAs regulate HMGB3. Using the miRNA target prediction algorithm TargetScan (www.targetscan.org), we determined that HMGB3 was a predicted target of miR-200b-3p and miR-200c-3p ( Figure 5A).…”

Section: Hmgb3 Is Targeted By Mir-200b-3p and Mir-200c-3pmentioning

confidence: 99%

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HMGB3 promotes the proliferation and metastasis of glioblastoma and is negatively regulated by miR‐200b‐3p and miR‐200c‐3p

Liu

Wang

2018

Cell Biochemistry & Function

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High mobility group box 3 (HMGB3) is strongly involved in oncogenesis in a variety of cancers. In the present study, we have explored the role of HMGB3 in glioblastoma multiforme (GBM) tumorigenesis and have identified the microRNAs (miRNAs) miR-200b-3p and miR-200c-3p as negative regulators of HMGB3 expression. We began by determining that endogenous HMGB3 expression levels were significantly elevated in GBM tissues and in 3 GBM cell lines. To study the function of HMGB3 in GBM, we transfected a small-interfering RNA (siRNA) against HMGB3 into GBM cell lines U251 and LN229. MTT and tumour sphere assays demonstrated that HMGB3 knockdown significantly inhibited cell proliferation. Wound healing and transwell assays determined that HMGB3 knockdown substantially suppressed GBM cell migration and invasion. We evaluated the effects of HMGB3 knockdown on MAPK phosphorylation and target gene expression, finding that HMGB3 knockdown significantly reduced MAPK phosphorylation (p-ERK (1/2), p-p38, and p-JNK). We then used the biologic prediction algorithm TargetScan to identify the 3' untranslated region (3'-UTR) of HMGB3 as a target of miR-200b-3p and miR-200c-3p. Luciferase, qRT-PCR, and western blot assays confirmed that miR-200b-3p and miR-200c-3p bind and inhibit HMGB3 expression. Finally, Pearson correlation analyses demonstrated a negative correlation between relative HMGB3 mRNA and miR-200b/c-3p expression levels in GBM tissue samples. Overall, the present study strongly suggests that HMGB3 promotes GBM oncogenesis through the MAPK signalling pathway while miR-200b-3p and miR-200c-3p inhibit its expression.

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Section: Resultsmentioning

confidence: 99%

Section: Hmgb3 Is Targeted By Mir-200b-3p and Mir-200c-3pmentioning

confidence: 99%

HMGB3 promotes the proliferation and metastasis of glioblastoma and is negatively regulated by miR‐200b‐3p and miR‐200c‐3p

Liu

Wang

2018

Cell Biochemistry & Function

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“…miRNAs are small non-protein-encoding RNAs which have been shown to be involved in cancer progression (Lu et al, 2005). Previous studies have shown that miRNAs can regulate glioma progression (Banelli et al, 2017;Shea et al, 2016), which makes miRNA a possible target for drug development in glioma. In the meanwhile, miRNAs and lncRNAs can also involve in the lncRNA-miRNA regulatory network to regulate cancer progression (Liz & Esteller, 2016 regulate renal carcinoma (Chiyomaru et al, 2013).…”

Section: Discussionmentioning

confidence: 99%

Long noncoding RNA gastric cancer‐associated transcript 3 plays oncogenic roles in glioma through sponging miR‐3127‐5p

Pan

Zhao

2018

Journal Cellular Physiology

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Evidence is emerging that long noncoding RNAs (lncRNAs) play vital roles in tumorigenesis. LncRNA gastric cancer‐associated transcript 3 (GACAT3) is reported to participate in the development of breast cancer, colorectal cancer, nonsmall cell lung cancer, and gastric cancer. However, whether it is implicated in glioma has not been elucidated. Here, we found that GACAT3 level was aberrantly elevated in glioma tissues and cell lines. Higher GACAT3 expression predicted lower survival rate. Knockdown of GACAT3 suppressed the proliferation, colony formation, migration, and invasion but promoting apoptosis in glioma cells. Next, we determined that GACAT3 contributes to glioma progression through inhibiting microRNA (miR)‐3127‐5p. Subsequently, ELAVL1 was identified as a direct target of miR‐3127‐5p by bioinformatics analysis and luciferase reporter assay. Moreover, we confirmed that GACAT3 promoted ELAVL1 expression through sponging miR‐3127‐5p, leading to glioma progression. Taken together, our study elucidated that GACAT3/miR‐3127‐5p/ELAVL1 signaling regulates glioma development and might be a promising therapeutic target.

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“…MiRNAs are small, noncoding RNAs that regulate gene expression preferentially by binding to the 3′‐untranslated region (3′‐UTR) of mRNAs in a sequence specific manner, thereby leading to inhibition of translation and/or enhanced mRNA degradation . Altered miRNA expression, including down‐regulation of tumour suppressive and up‐regulation of tumour promoting miRNAs, have been identified in many cancers , including gliomas . Among the first miRNAs implicated as tumour suppressors was miR‐16‐5p , which belongs to a family of evolutionary conserved miRNAs that share a common seed sequence.…”

Section: Introductionmentioning

confidence: 99%

MiR‐16‐5p is frequently down‐regulated in astrocytic gliomas and modulates glioma cell proliferation, apoptosis and response to cytotoxic therapy

Krell

Wolter

Stojcheva

et al. 2019

Neuropathology Appl Neurobio

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Aims Aberrant expression of microRNAs (miRNAs) is frequent in various cancers including gliomas. We aimed to characterize the role of miR‐16‐5p as a candidate tumour suppressor miRNA in gliomas. Methods Real‐time PCR‐based approaches were used for miRNA and mRNA expression profiling of glioma and non‐neoplastic brain tissues as well as glioma cell lines. Protein levels were determined by Western blotting. In vitro analyses were performed following overexpression of miR‐16‐5p, trichostatin A (TSA) treatment, and siRNA‐mediated knock‐down of HDAC3 in glioma cells. Effects of miR‐16‐5p on glioma cell viability, apoptosis and response to irradiation and temozolomide (TMZ) were assessed. Results Expression of miR‐16‐5p was reduced relative to control brain tissue in isocitrate dehydrogenase (IDH)‐mutant astrocytomas of World Health Organization (WHO) grades II, III and IV, and a subset of IDH‐wildtype glioblastomas WHO grade IV. MiR‐16‐5p expression was lower in IDH‐mutant than in IDH‐wildtype gliomas, and down‐regulated in IDH‐wildtype glioma lines. MiR‐16‐5p overexpression reduced expression of important cell cycle and apoptosis regulators in glioma cells, including CDK6, CDC25A, CCND3, CCNE1, WEE1, CHEK1, BCL2 and MCL1. In line, CDK6, WEE1, CHEK1, BCL2 and MCL1 transcript levels were increased in WHO grade III or IV gliomas. TSA treatment and HDAC3 knockdown in glioma cells induced miR‐16‐5p up‐regulation and reduced expression of its targets. Moreover, miR‐16‐5p overexpression inhibited proliferation and induced apoptosis in various glioma cell lines and increased sensitivity of A172 glioma cells to irradiation and TMZ. Conclusion Reduced expression of miR‐16‐5p contributes to glioma cell proliferation, survival and resistance to cytotoxic therapy.

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MicroRNA in Glioblastoma: An Overview

Cited by 125 publications

References 210 publications

HMGB3 promotes the proliferation and metastasis of glioblastoma and is negatively regulated by miR‐200b‐3p and miR‐200c‐3p

HMGB3 promotes the proliferation and metastasis of glioblastoma and is negatively regulated by miR‐200b‐3p and miR‐200c‐3p

Long noncoding RNA gastric cancer‐associated transcript 3 plays oncogenic roles in glioma through sponging miR‐3127‐5p

MiR‐16‐5p is frequently down‐regulated in astrocytic gliomas and modulates glioma cell proliferation, apoptosis and response to cytotoxic therapy

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