Hypermethylation of potential tumor suppressor miR-34b/c is correlated with late clinical stage in patients with soft tissue sarcomas

Xie Yuwen; Zong Peizhi; Wang Weiwei; Liu Dong; Li Bingcheng; Wang Yuanyuan; Hu Jianming; Ren Yan; Qi Yan; Cui Xiaobin; Chen Yunzhao; Liu Chunxia; Li Feng

首页> 外文期刊>Experimental & Molecular Pathology >Hypermethylation of potential tumor suppressor miR-34b/c is correlated with late clinical stage in patients with soft tissue sarcomas

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Hypermethylation of potential tumor suppressor miR-34b/c is correlated with late clinical stage in patients with soft tissue sarcomas

机译：潜在的肿瘤抑制因子miR-34b / c的高甲基化与软组织肉瘤患者的临床晚期相关

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Soft tissue sarcomas (STSs) are comparatively rare malignant tumors with poor prognosis. STSs predominantly arise from mesenchymal differentiation. MicroRNA-34b/c, the transcriptional targets of tumor suppressor p53, possesses tumor suppressing property. Hypermethylation of miR-34b/c has been associated with tumorigenesis and the progression of various cancers. To determine whether aberrant miR-34b/c methylation occurs in STSs, we quantitatively evaluated the methylation level of miR-34b/c in 57 STS samples and 20 cases of peripheral blood from healthy volunteers serving as normal controls by using matrix-assisted laser desorption ionization time-of-flight mass spectrometry. We found that miRNA34b/c is more frequently methylated in STSs (0.157 +/- 0.028) than in normal controls (0.098 +/- 0.012, p = 0.038). Furthermore, the methylation levels of CpG_1.2.3, CpG_4.5.6.7, and CpG_11.12.13 of miR-34b/c were significantly higher in the STS group than in the normal control group (p < 0.001). No significant differences in the methylation levels within miR-34b/c were observed between specific reciprocal translocations in STSs and nonspecific reciprocal translocations in STSs (0.146 +/- 0.039 vs. 0.168 +/- 0.035, p > 0.05). The methylation levels of miR-34b/c in STSs were associated with clinical stage. The methylation levels of CpG_1.2.3, CpG_4.5.6.7, CpG_9.10, CpG_11.12.13, and CpG_14 in tumor-stage III/IV tissues were significantly higher than those in tumor-stage I/II tissues. Our findings indicated that DNA hypermethylation of the miR-34b/c is a relatively common event in STSs and is significantly correlated with late clinical stage in patients with STSs. Hypermethylation of the miR-34b/c may be pivotal in the oncogenesis and progression of STSs and may be a potential prognostic factor for STSs. (C) 2015 The Authors. Published by Elsevier Inc. This is an open access article under the CC BY-NC-ND license.

机译：软组织肉瘤（STS）是比较少见的恶性肿瘤，预后较差。 STS主要来自间充质分化。抑癌基因p53的转录靶标MicroRNA-34b / c具有抑癌作用。 miR-34b / c的超甲基化与肿瘤发生和各种癌症的进展有关。为了确定STS中是否发生异常的miR-34b / c甲基化，我们通过基质辅助激光解吸定量评估了57名STS样品和20例健康志愿者作为正常对照的外周血中的miR-34b / c甲基化水平电离飞行时间质谱。我们发现，与正常对照（0.098 +/- 0.012，p = 0.038）相比，STS中的miRNA34b / c甲基化程度更高（0.157 +/- 0.028）。此外，STS组中miR-34b / c的CpG_1.2.3，CpG_4.5.6.7和CpG_11.12.13的甲基化水平显着高于正常对照组（p <0.001）。在STS的特异性互易位和STS的非特异性互易位之间，未观察到miR-34b / c内甲基化水平的显着差异（0.146 +/- 0.039与0.168 +/- 0.035，p> 0.05）。 STS中miR-34b / c的甲基化水平与临床分期有关。 III / IV期肿瘤组织中CpG_1.2.3，CpG_4.5.6.7，CpG_9.10，CpG_11.12.13和CpG_14的甲基化水平显着高于肿瘤I / II组织中的甲基化水平。我们的发现表明，miR-34b / c的DNA超甲基化在STS中是相对常见的事件，并且与STS患者的临床晚期阶段显着相关。 miR-34b / c的超甲基化可能在STS的发生和发展中起关键作用，并且可能是STS的潜在预后因素。（C）2015作者。由Elsevier Inc.发行。这是CC BY-NC-ND许可下的开放获取文章。

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《Experimental & Molecular Pathology》 |2015年第3期|共9页
作者
Xie Yuwen; Zong Peizhi; Wang Weiwei; Liu Dong; Li Bingcheng; Wang Yuanyuan; Hu Jianming; Ren Yan; Qi Yan; Cui Xiaobin; Chen Yunzhao; Liu Chunxia; Li Feng;
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正文语种 eng
中图分类病理学;
关键词
MircroRNA-34b/c; Soft tissue sarcomas; Translocation; Methylation; Tumorigenesis;

机译：MircroRNA-34b / c;软组织肉瘤;易位;甲基化;成瘤;
入库时间 2022-08-18 11:02:29

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1. Hypermethylation of potential tumor suppressor miR-34b/c is correlated with late clinical stage in patients with soft tissue sarcomas [J] . Xie Yuwen, Zong Peizhi, Wang Weiwei, Experimental & Molecular Pathology . 2015,第3期

机译：潜在的肿瘤抑制因子miR-34b / c的高甲基化与软组织肉瘤患者的临床晚期相关
2. Advanced Rai Stage in Patients with Chronic Lymphocytic Leukaemia Correlates with Simultaneous Hypermethylation of Plural Tumour Suppressor Genes [J] . K. FORSTEROVá, H. VOTAVOVá, J. SCHWARZ, Folia biologica . 2010,第4期

机译：慢性淋巴细胞白血病患者的晚期Rai分期与多个肿瘤抑制基因的同时超甲基化相关
3. The status quo of treatment and clinical outcomes for patients over 80 years of age with high-grade soft tissue sarcoma: report from the soft tissue tumor registry in Japan [J] . Okamoto Masanori, Kito Munehisa, Yoshimura Yasuo, Japanese journal of clinical oncology. . 2018,第10期

机译：高档软组织肉瘤80岁以上患者治疗和临床结果的现状：日本软组织肿瘤登记处的报告
4. Histological Characteristics of Soft Tissue Sarcomas Correlated to Electrical Resistance [C] . A.L. Tosi, L.G. Campana, F. Dughiero World Congress on Electroporation and Pulsed Electric Fields in Biology, Medicine and Food Environmental Technologies . 2016

机译：软组织肉瘤的组织学特征与电阻相关
5. Walleye retroviral cyclins phosphorylate pRb tumor suppressor and the walleye dermal sarcoma retrovirus cyclin and G2/M cyclins repress transcription of p14ARF tumor suppressor through interaction with TBX2, possibly contributing to tumorigenesis. [D] . Kim, Sang-Woo. 2004

机译：角膜白斑逆转录病毒细胞周期蛋白使pRb肿瘤抑制蛋白磷酸化，而角膜皮肉瘤逆转录病毒细胞周期蛋白和G2 / M细胞周期蛋白通过与TBX2相互作用抑制p14ARF肿瘤抑制因子的转录，可能有助于肿瘤发生。
6. Hypermethylation of miR-34b/c is associated with early clinical stages and tumor differentiation in Kazakh patients with esophageal squamous cell carcinoma [O] . Qian Wang, Dong Liu, Kaige Wang, 2019

机译：哈萨克族食管鳞癌患者中miR-34b / c的甲基化与早期临床阶段和肿瘤分化有关
7. Hypermethylation of potential tumor suppressor miR-34b/c is correlated with late clinical stage in patients with soft tissue sarcomas [O] . Xie Yuwen, Zong Peizhi, Wang Weiwei, 2015

机译：潜在的抑癌基因miR-34b / c的甲基化与软组织肉瘤患者的临床晚期相关

Hypermethylation of potential tumor suppressor miR-34b/c is correlated with late clinical stage in patients with soft tissue sarcomas

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