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miRNA 簇 C19MC 在甲状旁腺肿瘤中失调。

The microRNA cluster C19MC is deregulated in parathyroid tumours.

机构信息

Division of Pathology, Fondazione IRCCS Cà Granda Ospedale Maggiore Policlinico, Milan, Italy.

出版信息

J Mol Endocrinol. 2012 Jul 26;49(2):115-24. doi: 10.1530/JME-11-0189. Print 2012 Oct.

DOI:10.1530/JME-11-0189
PMID:22767050
Abstract

A subset of over-expressed microRNAs (miRNAs) identified in parathyroid carcinomas (Ca) compared to normal glands belongs to C19MC, a cluster on chromosome 19q13.4 involved in stem cell biology and tumourigenesis. In this study, the expression of C19MC-MIR371-3 clusters and the molecular mechanisms presiding their modulation were investigated in a series of six normal parathyroids, 24 adenomas (Ad), 15 Ca and five matched metastases. The general expression levels of C19MC or MIR371-3 clusters in Ad lesions did not differ from normal glands, while they distinguished Ad from Ca at unsupervised hierarchical cluster analysis (P=0.0008). MIR517C showed the most significant difference in expression between Ca and Ad (P=0.0003) and it positively correlated with serum calcium, parathormone and tumour weight. In regard to the molecular mechanism determining C19MC cluster activation, we could detect C19MC copy number (CN) gain in ten Ca (67%) extending distal to the MIR371-3 cluster in almost all samples. Conversely, only four Ad (16%) showed C19MC amplification, with one case presenting distal genomic aberration to MIR371-3. Globally, CN variations of 19q13.4 loci were significantly associated with MIR517C up-regulation (P=0.006). Opposite to normal glands where C19MC promoter was methylated, hypomethylation occurred in 15 out of 30 analysed tumours. Though the epigenetic status did not correlate with C19MC miRNA expression levels, loss of C19MC promoter methylation was significantly associated with Ca and metastatic disease (P=0.01). In conclusion, C19MC cluster aberrations are a characteristic of Ca with respect to Ad. Altogether, these evidences point towards a role for 19q13.4 miRNA clusters as oncogenes in parathyroid tumourigenesis.

摘要

在甲状旁腺癌(Ca)与正常腺体相比,一组过表达的 microRNAs(miRNAs)属于 19q13.4 染色体上的 C19MC,这是一个涉及干细胞生物学和肿瘤发生的簇。在这项研究中,研究了一系列 6 个正常甲状旁腺、24 个腺瘤(Ad)、15 个 Ca 和 5 个匹配转移瘤中 C19MC-MIR371-3 簇的表达及其调节的分子机制。在无监督层次聚类分析中,Ad 病变中的 C19MC 或 MIR371-3 簇的总体表达水平与正常腺体没有差异,但它们将 Ad 与 Ca 区分开来(P=0.0008)。MIR517C 在 Ca 与 Ad 之间的表达差异最大(P=0.0003),且与血清钙、甲状旁腺激素和肿瘤重量呈正相关。关于决定 C19MC 簇激活的分子机制,我们可以检测到 10 个 Ca(67%)中的 C19MC 拷贝数(CN)增益,几乎所有样本都延伸到 MIR371-3 簇之外。相反,只有 4 个 Ad(16%)显示出 C19MC 扩增,其中一个病例在 MIR371-3 处出现远端基因组异常。总体而言,19q13.4 位点的 CN 变化与 MIR517C 的上调显著相关(P=0.006)。与正常腺体中 C19MC 启动子甲基化相反,在 30 个分析的肿瘤中有 15 个发生了低甲基化。虽然表观遗传状态与 C19MC miRNA 表达水平没有相关性,但 C19MC 启动子甲基化的缺失与 Ca 和转移性疾病显著相关(P=0.01)。总之,C19MC 簇异常是 Ca 相对于 Ad 的特征。总之,这些证据表明 19q13.4 miRNA 簇在甲状旁腺肿瘤发生中作为癌基因发挥作用。

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