microRNAs in Cancer Cell Response to Ionizing Radiation

Czochor, Jennifer R.; Glazer, Peter M.

doi:10.1089/ars.2013.5718

Cited by 84 publications

(82 citation statements)

References 170 publications

(242 reference statements)

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“…Several signaling pathways, including PI3K/AKT, mitogen-activated protein kinase and ATM/CHK2/p53, have been linked to the tumor radioresistance. 22,23 In the present study we have demonstrated that IKKα-mediated miR-196a biogenesis regulates the sensitivity of NPC cells to radiotherapy. Dephosphorylation of p-IKKαT23 downregulates miR-196a expression and promotes the resistance of NPC cells to radiation treatment.…”

Section: Discussionmentioning

confidence: 52%

IKKα-mediated biogenesis of miR-196a through interaction with Drosha regulates the sensitivity of cancer cells to radiotherapy

et al. 2016

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Radioresistance is a major obstacle in successful clinical cancer radiotherapy, and the underlying mechanisms are not clear. Here we show that IKKα-mediated miR-196a biogenesis via interaction with Drosha regulates the sensitivity of nasopharyngeal carcinoma (NPC) cells to radiotherapy. Phosphorylation of IKKα at T23 site (p-IKKαT23) promotes the binding of IKKα to Drosha that accelerates the processing of miR-196a primary transcripts, leading to increased expressions of both precursor and mature miR-196a. Dephosphorylation of p-IKKαT23 downregulates miR-196a expression and promotes the resistance of NPC cells to radiation treatment. The miR-196a mimic suppresses while its inhibitor promotes the resistance of NPC to radiation treatment. Importantly, the expression of p-IKKαT23 is positively related to the expression of miR-196a in human NPC tissues, and expression of p-IKKαT23 and miR-196a is inversely correlated with NPC clinical radioresistance. Thus, our studies establish a novel mechanistic link between the inactivation of IKKαT23-Drosha-miR-196a pathway and NPC radioresistance, and de-inactivation of IKKαT23-Drosha-miR-196a pathway would be an efficient way to restore the sensitivity of radioresistant NPC to radiotherapy.

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Section: Discussionmentioning

confidence: 52%

IKKα-mediated biogenesis of miR-196a through interaction with Drosha regulates the sensitivity of cancer cells to radiotherapy

et al. 2016

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“…More than 1000 miRNAs have been identified in humans and are predicted to modulate the expression of at least 60% of protein-coding genes at the transcriptional level [11][12][13]. By repressing target genes, miRNAs play key roles in various biological events in tumors, such as cell proliferation, differentiation, apoptosis and tumor invasion [14][15][16][17][18].…”

Section: Introductionmentioning

confidence: 99%

Expression Signature and Role of miR-30d-5p in Non-Small Cell Lung Cancer: a Comprehensive Study Based on in Silico Analysis of Public Databases and in Vitro Experiments

et al. 2018

Cell Physiol Biochem

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Background/Aims: The purpose of this study was to probe the clinico-pathological significance and the underlying mechanism of miR-30d-5p expression in non-small cell lung cancer (NSCLC). Methods: We initially examined the level of miR-30d-5p expression in NSCLC and non-cancer tissues using RT-qPCR. Then, a series of validation analyses including a meta-analysis of data from microarray chips in Gene Expression Omnibus (GEO), data mining of the cancer genome atlas (TCGA) and an integrated meta-analysis incorporating GEO microarray chips, TCGA data, in-house RT-qPCR and literature studies were performed to examine the clinico-pathological value of miR-30d-5p expression in NSCLC. In vitro experiments were further conducted to investigate the impact of miR-30d-5p on NSCLC cell growth. The molecular mechanism by which miR-30d-5p regulates the pathogenesis of NSCLC was probed through a bioinformatics analysis of its target genes. Moreover, dual luciferase reporter assay was conducted to verify the targeting regulatory relationship between miR-30d-5p and CCNE2. Results: Based on results from RT-qPCR, GEO meta-analysis, TCGA data mining and the integrated meta-analysis incorporating GEO microarray chips, TCGA data, in-house RT-qPCR and literature studies, miR-30d-5p expression was decreased in NSCLC tissues, and patients with NSCLC who presented with lower miR-30d-5p expression tended to display an advanced clinical progression. Significant pathways including the Mucin type O-glycan biosynthesis pathway, cell cycle pathway and cysteine and methionine metabolism pathway (all P< 0.05) revealed potential roles of the target genes of miR-30d-5p in the oncogenesis of NSCLC. Results from in vitro experiments indicated that miR-30d-5p could attenuate proliferation and viability of NSCLC cells. Among the 12 identified hub genes, nine genes including E2F3, CCNE2, SKP2, CDK6, TFDP1, LDHA, GOT2, DNMT3B and ST6GALNAC1 were validated by Pearson’s correlation test and the human protein atlas (HPA) database as targets of miR-30d-5p with higher probability. Specifically, dual luciferase reporter assay confirmed that CCNE2 was directly targeted by miR-30d-5p. Conclusion: In summary, miR-30d-5p expression is decreased in NSCLC, and it might play the role as tumor suppressor in NSCLC by regulating target genes.

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“…MiRNAs are involved in regulating at the post-transcriptional level the expression of important targets in the DDR pathway [14,15] . Indeed, miRNAs have been shown to efficiently modulate tumor radiosensitivity by blocking both the NHEJ and HR repair pathways involved in the DDR; they have proven to interfere with the major pathways activated by ionizing radiation, such as the PI3-K/Akt, NF-κB, MAPK and TGFβ signaling pathways [16] .…”

Section: Mirnas Influence Rt By Affecting Specific Cellular Pathwaysmentioning

confidence: 99%

Emerging role of microRNAs in breast cancer radiotherapy

Marvaso

Barone

Amodio

2015

RNA Dis

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Breast cancer represents the leading cause of death in women worldwide. Ionizing radiation is one of the most relevant therapeutic approaches for the treatment of this type of cancer. Unfortunately, either resistance of tumor cells to therapeutic doses of radiation or normal tissue tolerance have proven to limit the effectiveness of radiotherapy. In the last few years, several studies have highlighted an important link between radioresistance, cancer and microRNAs (miRNAs), an emerging class of endogenous non coding RNAs that control gene expression. MiRNAs influence carcinogenesis at multiple stages and effectively control tumor radiosensitivity as they affect levels of target genes regulating relavant radio-related signal transduction pathways. Since radiationand multidrug-resistances are the characteristic properties of numerous type of tumors, there is a huge interest in understanding the connection between miRNA expression in tumors and chemo-or radio-sensitivity. In the present review, we summarize the emerging evidence of miRNAs involvement in the radioresponse of breast tumors and discuss their potential role of radiosensitizers.

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microRNAs in Cancer Cell Response to Ionizing Radiation

Cited by 84 publications

References 170 publications

IKKα-mediated biogenesis of miR-196a through interaction with Drosha regulates the sensitivity of cancer cells to radiotherapy

IKKα-mediated biogenesis of miR-196a through interaction with Drosha regulates the sensitivity of cancer cells to radiotherapy

Expression Signature and Role of miR-30d-5p in Non-Small Cell Lung Cancer: a Comprehensive Study Based on in Silico Analysis of Public Databases and in Vitro Experiments

Emerging role of microRNAs in breast cancer radiotherapy

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