Biophysics Graduate Group, University of California, Berkeley, 742 Stanley Hall, Berkeley, CA 94720, USA.
J Mol Biol. 2013 Oct 9;425(19):3639-48. doi: 10.1016/j.jmb.2012.08.024. Epub 2012 Sep 4.
Gene transcription is regulated in response to environmental changes and developmental cues. In mammalian cells subjected to stress conditions such as heat shock, transcription of most protein-coding genes decreases, while the transcription of heat shock protein genes increases. Repression involves direct binding to RNA polymerase II (Pol II) of certain noncoding RNAs (ncRNAs) that are upregulated upon heat shock. Another class of ncRNAs is also upregulated and binds to Pol II but does not inhibit transcription. Incorporation of repressive ncRNAs into pre-initiation complexes prevents transcription initiation, while non-repressive ncRNAs are displaced from Pol II by TFIIF. Here, we present cryo-electron microscopy reconstructions of human Pol II in complex with six different ncRNAs from mouse and human. Our structures show that both repressive and non-repressive ncRNAs bind to a conserved binding site within the cleft of Pol II. The site, which is also shared with a previously characterized yeast aptamer, is close to the active center and, thus, in an ideal position to regulate transcription. Importantly, additional RNA elements extend flexibly beyond the docking site. We propose that the differences concerning the repressive activity of the ncRNAs analyzed must be due to the distinct character of these more unstructured, flexible segments of the RNA that emanate from the cleft.
基因转录是响应环境变化和发育线索而调节的。在哺乳动物细胞受到热休克等应激条件时,大多数蛋白质编码基因的转录减少,而热休克蛋白基因的转录增加。抑制涉及某些非编码 RNA(ncRNA)与 RNA 聚合酶 II(Pol II)的直接结合,这些 ncRNA 在热休克时上调。另一类 ncRNA 也上调并与 Pol II 结合,但不抑制转录。抑制性 ncRNA 掺入起始前复合物会阻止转录起始,而非抑制性 ncRNA 则被 TFIIF 从 Pol II 上置换。在这里,我们展示了与人 Pol II 复合的来自小鼠和人的六种不同 ncRNA 的冷冻电镜重建结构。我们的结构表明,抑制性和非抑制性 ncRNA 都结合到 Pol II 裂隙内的保守结合位点上。该位点也与先前表征的酵母适体共享,靠近活性中心,因此处于调节转录的理想位置。重要的是,附加的 RNA 元件在对接位点之外灵活地延伸。我们提出,所分析的 ncRNA 的抑制活性的差异必须归因于从裂隙中伸出的这些更无规则、更灵活的 RNA 片段的独特性质。
