Theoretical Biology and Biophysics, Theoretical Division, Los Alamos National Laboratory, Los Alamos, New Mexico 87545, USA.
Nucleic Acids Res. 2012 Jun;40(11):5034-51. doi: 10.1093/nar/gks071. Epub 2012 Feb 22.
While functional roles of several long non-coding RNAs (lncRNAs) have been determined, the molecular mechanisms are not well understood. Here, we report the first experimentally derived secondary structure of a human lncRNA, the steroid receptor RNA activator (SRA), 0.87 kB in size. The SRA RNA is a non-coding RNA that coactivates several human sex hormone receptors and is strongly associated with breast cancer. Coding isoforms of SRA are also expressed to produce proteins, making the SRA gene a unique bifunctional system. Our experimental findings (SHAPE, in-line, DMS and RNase V1 probing) reveal that this lncRNA has a complex structural organization, consisting of four domains, with a variety of secondary structure elements. We examine the coevolution of the SRA gene at the RNA structure and protein structure levels using comparative sequence analysis across vertebrates. Rapid evolutionary stabilization of RNA structure, combined with frame-disrupting mutations in conserved regions, suggests that evolutionary pressure preserves the RNA structural core rather than its translational product. We perform similar experiments on alternatively spliced SRA isoforms to assess their structural features.
虽然已经确定了几个长非编码 RNA(lncRNA)的功能作用,但分子机制尚不清楚。在这里,我们报告了第一个人类 lncRNA——甾体激素受体 RNA 激活物(SRA)的实验推导的二级结构,其大小为 0.87 kB。SRA RNA 是一种非编码 RNA,可共激活几种人类性激素受体,与乳腺癌密切相关。SRA 的编码同工型也被表达以产生蛋白质,使 SRA 基因成为一个独特的双功能系统。我们的实验结果(SHAPE、在线、DMS 和 RNase V1 探测)表明,这种 lncRNA 具有复杂的结构组织,由四个结构域组成,具有多种二级结构元件。我们使用脊椎动物的比较序列分析来检查 SRA 基因在 RNA 结构和蛋白质结构水平上的共进化。RNA 结构的快速进化稳定,加上保守区域的框架中断突变,表明进化压力保留了 RNA 结构的核心,而不是其翻译产物。我们对不同剪接的 SRA 同工型进行类似的实验,以评估它们的结构特征。
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