Nc886 is epigenetically repressed in prostate cancer and acts as a tumor suppressor through the inhibition of cell growth

Fort, Rafael Sebastián; Mathó, Cecilia; Geraldo, Murilo Vieira; Ottati, María Carolina; Yamashita, Alex Shimura; Saito, Kelly Cristina; Leite, Kátia R. M.; Rey-Méndez, Manuel; Maedo, Noemí; Méndez, Laura Rivera; Garat, Beatríz; Kimura, Edna Teruko; Sotelo‐Silveira, José; Duhagon, Marı́a Ana

doi:10.1186/s12885-018-4049-7

Cited by 35 publications

(68 citation statements)

References 42 publications

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“…nc886 was initially thought to be a tumor suppressor, because epigenetic silencing in cancer is a hallmark of tumor suppressor genes. To support this notion, ectopic expression of nc886 was shown to inhibit cell proliferation (Fort et al, ; Lee, Park, et al, ). However, we do not think that this can be attributed to PKR suppression, because PKR mostly stays inactive in normal tissues.…”

Section: Conclusion and Future Perspectivesmentioning

confidence: 99%

“…nc886 has a strong CpG island at the promoter region and its expression is silenced in a subset of malignant cells by DNA hypermethylation at the CpG island (Park et al, ). nc886 silencing occurs frequently in a number of malignancies (Ahn et al, ; Cao et al, ; Fort et al, ; Lee, Lee, et al, ; Lee, Park, et al, ; Park et al, ; Treppendahl et al, ), presumably because nc886 is an imprinted gene (Carpenter et al, ; Paliwal et al, ; Romanelli et al, ). Unlike typical imprinted genes which show monoallelic methylation in 100% of individuals, nc886 is estimated to be methylated in the maternal allele in approximately 75% of individuals (Treppendahl et al, ).…”

Section: Cellular Rnas That Controls Pkrmentioning

confidence: 99%

“…For all those reasons, we surmise that nc886 is vastly superior to other PKR repressors. nc886 silencing has been observed in diverse cancers including AML (Treppendahl et al, ), small cell lung cancer (Cao et al, ), gastric cancer (Lee, Park, et al, ), esophageal cell squamous carcinoma (Lee, Lee, et al, ), breast cancer (Park et al, ), and prostate cancer (Fort et al, ). Except nc886, there is one report about P58 whose expression was shown to be lower in more malignant breast cancer cells as compared to nontransformed breast cells (Kim et al, ).…”

Section: Pkr Regulation In Cancermentioning

confidence: 99%

“…Thus, the cellular outcome upon nc886 up‐regulation should be distinguished from nc886 silencing that activates PKR to trigger tumor surveillance role. In fact, ectopic expression of nc886 leads to delayed cell cycle progression, which seems to be independent of PKR (Fort et al, ). By contrast, PKR activation is a key event when nc886 knockdown causes apoptosis (Kunkeaw et al, ; Lee, Lee, et al, ).…”

Section: Conclusion and Future Perspectivesmentioning

confidence: 99%

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Protein kinase R and its cellular regulators in cancer: An active player or a surveillant?

2019

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Protein kinase R (PKR), originally known as an antiviral protein, senses various stresses as well as pathogen‐driven double‐stranded RNAs. Thereby activated PKR provokes diverse downstream events, including eIF2α phosphorylation and nuclear factor kappa‐light‐chain‐enhancer of activated B cells activation. Consequently, PKR induces apoptosis and inflammation, both of which are highly important in cancer as much as its original antiviral role. Therefore, cellular proteins and RNAs should tightly control PKR activity. PKR and its regulators are often dysregulated in cancer and it is undoubted that such dysregulation contributes to tumorigenesis. However, PKR's precise role in cancer is still in debate, due to incomprehensible and even contradictory data. In this review, we introduce important cellular PKR regulators and discuss about their roles in cancer. Among them, we pay particular attention to nc886, a PKR repressor noncoding RNA that has been identified relatively recently, because its expression pattern in cancer can explain interesting yet obscure oncologic aspects of PKR. Based on nc886 and its regulation of PKR, we have proposed a tumor surveillance model, which reconciles contradictory data about PKR in cancer. This article is categorized under: Regulatory RNAs/RNAi/Riboswitches > Regulatory RNAs RNA Interactions with Proteins and Other Molecules > Protein–RNA Interactions: Functional Implications

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Section: Conclusion and Future Perspectivesmentioning

confidence: 99%

Section: Cellular Rnas That Controls Pkrmentioning

confidence: 99%

Section: Pkr Regulation In Cancermentioning

confidence: 99%

Section: Conclusion and Future Perspectivesmentioning

confidence: 99%

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Protein kinase R and its cellular regulators in cancer: An active player or a surveillant?

2019

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“…We have previously identified PKR as a molecular target of 5-FU in several colon and breast cancer cells lines, playing an important role in the cytotoxic effect of 5-FU at least, in part, through the induction of cell death by apoptosis [14]. Because PKR has also been implicated in the anti-tumour activity of chemotherapeutic drugs such as doxorubicin (DOX) and etoposide [15,16], and nc886 has been identified as an interesting tumour suppressor [17][18][19], we consider the analysis of PKR and the nc886 in patients as potential predictive biomarkers to be of clinical importance. For this reason, the aim of this work was to carry out an ambispective study in 197 metastatic colon cancer patients to evaluate the expression levels of PKR and its pre-microRNA-nc886 by qPCR in colon tumour samples and their respective healthy tissues and plasma, analysing its relation with the patient's clinical evolution.…”

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confidence: 99%

Uncovering Tumour Heterogeneity through PKR and nc886 Analysis in Metastatic Colon Cancer Patients Treated with 5-FU-Based Chemotherapy

Ortega-García

Mesa

Moya

et al. 2020

Cancers

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Colorectal cancer treatment has advanced over the past decade. The drug 5-fluorouracil is still used with a wide percentage of patients who do not respond. Therefore, a challenge is the identification of predictive biomarkers. The protein kinase R (PKR also called EIF2AK2) and its regulator, the non-coding pre-mir-nc886, have multiple effects on cells in response to numerous types of stress, including chemotherapy. In this work, we performed an ambispective study with 197 metastatic colon cancer patients with unresectable metastases to determine the relative expression levels of both nc886 and PKR by qPCR, as well as the location of PKR by immunohistochemistry in tumour samples and healthy tissues (plasma and colon epithelium). As primary end point, the expression levels were related to the objective response to first-line chemotherapy following the response evaluation criteria in solid tumours (RECIST) and, as the second end point, with survival at 18 and 36 months. Hierarchical agglomerative clustering was performed to accommodate the heterogeneity and complexity of oncological patients' data. High expression levels of nc886 were related to the response to treatment and allowed to identify clusters of patients. Although the PKR Cancers 2020, 12, 379 2 of 17 mRNA expression was not associated with chemotherapy response, the absence of PKR location in the nucleolus was correlated with first-line chemotherapy response. Moreover, a relationship between survival and the expression of both PKR and nc886 in healthy tissues was found. Therefore, this work evaluated the best way to analyse the potential biomarkers PKR and nc886 in order to establish clusters of patients depending on the cancer outcomes using algorithms for complex and heterogeneous data.

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Noncoding RNA 886 alleviates tumor cellular immunological rejection in host C57BL/C mice

Wang

Zhou

et al. 2020

Cancer Medicine

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Non‐coding RNA 886 (nc886/VTRNA2‐1) is a Pol III transcript and an atypical imprinted gene. Its exact function as a negative regulator of protein kinase R establishes its connection with innate immunity. Studies have shown that nc886 silencing is closely associated with prostate cancer progression. Previous work has constructed a cell model of stable nc886 overexpression (“mimic” or “nc886 + ”) in PC‐3M‐1E8 cell lines (1E8), which are highly bone‐metastatic human prostate cancer cells with low expression of nc886, and cells expressing the mimic were validated to have lower invasive and metastatic abilities than cells expressing the scramble transcript in vitro and in vivo. In this study, we directly injected mimic or scramble cells into the left ventricle of C57BL/C mice, an immunocompetent animal model, to elucidate the immune mechanisms of tumor‐host interactions. Interestingly, we found that tumor cells induced the inflammation of many important organs due to xenogeneic antigen rejection; this inflammation was ultimately repaired by tissue fibrosis after 28 days, except for in the spleen. The reason is that mimic cells, as heterogeneous antigens, are mostly directly recognized by macrophages or T cells in blood, and few mimic cells enter the spleen compared with scramble cells. The induction of splenic macrophage polarization to M2 macrophages by scramble cells is a critical factor in maintaining chronic splenic inflammation. In addition, we recognize that nc886 broadly decreases the expression of some human leukocyte antigen molecules and antigen transporters. This evidence reveals the interesting role of nc886 in regulating tumor cell antigens.

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Nc886 is epigenetically repressed in prostate cancer and acts as a tumor suppressor through the inhibition of cell growth

Cited by 35 publications

References 42 publications

Protein kinase R and its cellular regulators in cancer: An active player or a surveillant?

Protein kinase R and its cellular regulators in cancer: An active player or a surveillant?

Uncovering Tumour Heterogeneity through PKR and nc886 Analysis in Metastatic Colon Cancer Patients Treated with 5-FU-Based Chemotherapy

Noncoding RNA 886 alleviates tumor cellular immunological rejection in host C57BL/C mice

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