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miR‐15a‐5p miR‐15b‐5p and miR‐16‐5p inhibit tumor progression by directly targeting MYCN in neuroblastoma

机译：miR-15a-5pmiR-15b-5p和miR-16-5p通过直接靶向成神经细胞瘤中的MYCN抑制肿瘤进展

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Neuroblastoma (NB) is the most common extracranial solid malignancy in children. Despite current aggressive treatment regimens, the prognosis for high‐risk NB patients remains poor, with the survival of less than 40%. Amplification/stabilization of MYCN oncogene, in NB is associated with a high risk of recurrence. Thus, there is an urgent need for novel therapeutics. The deregulated expression of microRNA (miR) is reported in NB; nonetheless, its effect on regulation is poorly understood. First, we identified that miR‐15a‐5p, miR‐15b‐5p, and miR‐16‐5p (hereafter miR‐15a, miR‐15b or miR‐16) were down‐regulated in patient‐derived xenografts (PDX) with high expression. MiR targeting sequences on MYCN mRNA were predicted using online databases such as TargetScan and miR database. The R2 database, containing 105 NB patients, showed an inverse correlation between MYCN mRNA and deleted in lymphocytic leukemia ( ) 2, a host gene of miR‐15. Moreover, overexpression of miR‐15a, miR‐15b or miR‐16 significantly reduced the levels of MYCN mRNA and N‐Myc protein. Conversely, inhibiting miR dramatically enhanced MYCN mRNA and N‐Myc protein levels, as well as increasing mRNA half‐life in NB cells. By performing immunoprecipitation assays of argonaute‐2 (Ago2), a core component of the RNA‐induced silencing complex, we showed that miR‐15a, miR‐15b and miR‐16 interact with MYCN mRNA. Luciferase reporter assays showed that miR‐15a, miR‐15b and miR‐16 bind with 3’UTR of MYCN mRNA, resulting in suppression. Moreover, induced expression of miR‐15a, miR‐15b and miR‐16 significantly reduced the proliferation, migration, and invasion of NB cells. Finally, transplanting miR‐15a‐, miR‐15b‐ and miR‐16‐expressing NB cells into NSG mice repressed tumor formation and expression. These data suggest that miR‐15a, miR‐15b and miR‐16 exert a tumor‐suppressive function in NB by targeting . Therefore, these miRs could be considered as potential targets for NB treatment.

机译：神经母细胞瘤（NB）是儿童中最常见的颅外实体恶性肿瘤。尽管目前有积极的治疗方案，但高危NB患者的预后仍然很差，存活率不到40％。 NB中MYCN致癌基因的扩增/稳定与高复发风险相关。因此，迫切需要新的疗法。 NB中报道了microRNA（miR）的表达失调；然而，人们对它对监管的影响知之甚少。首先，我们确定在患者源性异种移植（PDX）中，miR-15a-5p，miR-15b-5p和miR-16-5p（以下称miR-15a，miR-15b或miR-16）被下调。高表达。使用在线数据库（例如TargetScan和miR数据库）预测了MYCN mRNA上的MiR靶向序列。 R2数据库包含105个NB患者，显示MYCN mRNA与miR-15的宿主基因淋巴细胞白血病（）2中的缺失呈负相关。此外，miR-15a，miR-15b或miR-16的过表达显着降低了MYCN mRNA和N-Myc蛋白的水平。相反，抑制miR可以显着提高MYCN mRNA和N-Myc蛋白水平，并增加NB细胞的mRNA半衰期。通过对argonaute-2（Ago2）（RNA诱导的沉默复合体的核心组成部分）进行免疫沉淀测定，我们证明了miR-15a，miR-15b和miR-16与MYCN mRNA相互作用。萤光素酶报告基因检测表明，miR-15a，miR-15b和miR-16与MYCN mRNA的3′UTR结合，从而导致抑制。此外，miR-15a，miR-15b和miR-16的诱导表达显着降低了NB细胞的增殖，迁移和侵袭。最后，将表达miR-15a‐，miR‐15b‐和miR‐16的NB细胞移植到NSG小鼠中可抑制肿瘤的形成和表达。这些数据表明，miR-15a，miR-15b和miR-16通过靶向作用在NB中发挥肿瘤抑制功能。因此，这些miRs可被视为NB治疗的潜在靶标。

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期刊名称 Molecular Oncology
作者
Srinivas Chava; C. Patrick Reynolds; Anup S. Pathania; Santhi Gorantla; Larisa Y. Poluektova; Don W. Coulter; Subash C. Gupta; Manoj K. Pandey; Kishore B. Challagundla;
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年(卷),期 2020(14),1
年度 2020
页码 -1
总页数 17
原文格式 PDF
正文语种
中图分类肿瘤学;
关键词
Ago2; microRNA; MYCN; neuroblastoma; patient‐derived xenografts;

机译：Ago2;microRNA;MYCN;神经母细胞瘤;患者来源的异种移植;

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1. miR‐15a‐5p, miR‐15b‐5p, and miR‐16‐5p inhibit tumor progression by directly targeting MYCN in neuroblastoma [J] . Srinivas Chava, C. Patrick Reynolds, Anup S. Pathania, Molecular oncology. . 2020,第1期

机译：miR-15a-5p，miR-15b-5p和miR-16-5p通过直接靶向神经母细胞瘤中的mycn来抑制肿瘤进展
2. miR‐15a‐5p and miR‐21‐5p contribute to chemoresistance in cytogenetically normal acute myeloid leukaemia by targeting PDCD4, ARL2 and BTG2 [J] . Virginie Vandewalle, Ahmed Essaghir, Emeline Bollaert, Journal of cellular and molecular medicine. . 2021,第1期

机译：miR-15a-5p和miR-21-5p通过靶向pdcd4，arl2和btg2，有助于化学常规急性骨髓性白血病的化学抑制剂
3. MiR‐139‐5p, miR‐940 and miR‐193a‐5p inhibit the growth of hepatocellular carcinoma by targeting SPOCK1 [J] . Peng Li, Zhiwei Xiao, Jiajun Luo, Journal of cellular and molecular medicine. . 2019,第4期

机译：通过靶向SPOCK1，MiR-139-5p，miR-940和miR-193a-5p抑制肝细胞癌的生长
4. Induced miR-30e-5p expression represses YAP1 cooperatively with miR- 15a to promote fat metabolism [C] . Zhi Chen, Jun Luo, Hui Wang, The 3rd Asian-Australasian dairy goat conference . 2016

机译：诱导的miR-30e-5p表达与miR-15a协同抑制YAP1以促进脂肪代谢
5. Dual strands of the miR-223 duplex (miR-223-5p and miR-223-3p) inhibit cancer cell aggressiveness : targeted genes are involved in bladder cancer pathogenesis [D] . SUGAWARA, Sho 2019

机译：miR-223双链体的双链（miR-223-5p和miR-223-3p）抑制癌细胞侵袭性：靶向基因参与膀胱癌的发病机理
6. miR‐15a‐5p and miR‐21‐5p contribute to chemoresistance in cytogenetically normal acute myeloid leukaemia by targeting PDCD4 ARL2 and BTG2 [O] . Virginie Vandewalle, Ahmed Essaghir, Emeline Bollaert, 2021

机译：miR-15a-5p和miR-21-5p通过靶向pdcd4arl2和btg2有助于化学常规急性髓细胞白血病的化学抑制
7. miR‐15a‐5p, miR‐15b‐5p, and miR‐16‐5p inhibit tumor progression by directly targeting MYCN in neuroblastoma [O] . Srinivas Chava, C. Patrick Reynolds, Anup S. Pathania, 2019

机译：miR-15a-5p，miR-15b-5p和miR-16-5p通过直接靶向神经母细胞瘤中的mycn来抑制肿瘤进展
8. Further analysis of the microgravity environment on Mir Space Station during Mir-16 [R] . Ryaboukha, Stanislav, Hrovat, Ken, Miskowitz, Milton, 1996

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miR‐15a‐5p miR‐15b‐5p and miR‐16‐5p inhibit tumor progression by directly targeting MYCN in neuroblastoma

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