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人类癌症中微小RNA的序列变异:预测二级结构的改变不影响加工过程。

Sequence variations of microRNAs in human cancer: alterations in predicted secondary structure do not affect processing.

作者信息

Diederichs Sven, Haber Daniel A

机构信息

Massachusetts General Hospital Cancer Center, Harvard Medical School, Charlestown, Massachusetts 02129, USA.

出版信息

Cancer Res. 2006 Jun 15;66(12):6097-104. doi: 10.1158/0008-5472.CAN-06-0537.

DOI:10.1158/0008-5472.CAN-06-0537
PMID:16778182
Abstract

Expression levels of microRNAs (miRNAs) are globally reduced in cancer compared with matched normal tissues, and miRNA function has recently been implicated in tumorigenesis. To test whether epigenetic silencing contributes to miRNA suppression in tumors, lung cancer cells were treated with inhibitors of DNA methylation or histone deacetylation. No significant alteration in miRNA expression was detected using microarray profiling. To search for tumor-associated mutations that could affect processing and expression of mature miRNAs, a panel of 91 cancer-derived cell lines was analyzed for sequence variations in 15 miRNAs implicated in tumorigenesis by virtue of their known target transcripts (let-7 family targeting oncogenic Ras) or their localization to sites of frequent chromosomal instability (miR-143, miR-145, miR-26a-1, and miR-21). No mutations were detected within any of the short mature miRNA sequences. In addition to previously reported polymorphisms, 1 sequence variant in a precursor miRNA and 15 variants in primary miRNA (pri-miRNA) transcripts were identified. Despite pri-miRNAs having dramatic changes in the predicted secondary folding structure flanking putative cleavage sites, processing and miRNA maturation were not affected in vivo. Thus, genetic variants in miRNA precursors are common in cancer cells but are unlikely to have physiologic significance.

摘要

与匹配的正常组织相比,癌症中微小RNA(miRNA)的表达水平整体降低,并且miRNA功能最近被认为与肿瘤发生有关。为了测试表观遗传沉默是否导致肿瘤中miRNA的抑制,用DNA甲基化抑制剂或组蛋白去乙酰化抑制剂处理肺癌细胞。使用微阵列分析未检测到miRNA表达的显著变化。为了寻找可能影响成熟miRNA加工和表达的肿瘤相关突变,分析了一组91个癌症来源的细胞系,以寻找15个miRNA的序列变异,这些miRNA因其已知的靶转录本(靶向致癌Ras的let-7家族)或其定位于频繁染色体不稳定位点(miR-143、miR-145、miR-26a-1和miR-21)而与肿瘤发生有关。在任何短的成熟miRNA序列中均未检测到突变。除了先前报道的多态性外,还鉴定了前体miRNA中的1个序列变异和初级miRNA(pri-miRNA)转录本中的15个变异。尽管pri-miRNA在假定切割位点侧翼的预测二级折叠结构中有显著变化,但在体内加工和miRNA成熟并未受到影响。因此,miRNA前体中的遗传变异在癌细胞中很常见,但不太可能具有生理意义。

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