Eulalio Ana, Behm-Ansmant Isabelle, Schweizer Daniel, Izaurralde Elisa
Max Planck Institute for Developmental Biology, Spemannstrasse 35, D-72076 Tübingen, Germany.
Mol Cell Biol. 2007 Jun;27(11):3970-81. doi: 10.1128/MCB.00128-07. Epub 2007 Apr 2.
P bodies are cytoplasmic domains that contain proteins involved in diverse posttranscriptional processes, such as mRNA degradation, nonsense-mediated mRNA decay (NMD), translational repression, and RNA-mediated gene silencing. The localization of these proteins and their targets in P bodies raises the question of whether their spatial concentration in discrete cytoplasmic domains is required for posttranscriptional gene regulation. We show that processes such as mRNA decay, NMD, and RNA-mediated gene silencing are functional in cells lacking detectable microscopic P bodies. Although P bodies are not required for silencing, blocking small interfering RNA or microRNA silencing pathways at any step prevents P-body formation, indicating that P bodies arise as a consequence of silencing. Consistently, we show that releasing mRNAs from polysomes is insufficient to trigger P-body assembly: polysome-free mRNAs must enter silencing and/or decapping pathways to nucleate P bodies. Thus, even though P-body components play crucial roles in mRNA silencing and decay, aggregation into P bodies is not required for function but is instead a consequence of their activity.
P小体是细胞质结构域,包含参与多种转录后过程的蛋白质,如mRNA降解、无义介导的mRNA衰变(NMD)、翻译抑制和RNA介导的基因沉默。这些蛋白质及其靶标在P小体中的定位引发了一个问题,即它们在离散细胞质结构域中的空间聚集对于转录后基因调控是否必要。我们发现,诸如mRNA衰变、NMD和RNA介导的基因沉默等过程在缺乏可检测到的微观P小体的细胞中仍能发挥作用。虽然沉默并不需要P小体,但在任何步骤阻断小干扰RNA或微小RNA沉默途径都会阻止P小体形成,这表明P小体是沉默的结果。一致地,我们表明从多核糖体释放mRNA不足以触发P小体组装:无多核糖体的mRNA必须进入沉默和/或去帽途径才能形成P小体核心。因此,尽管P小体成分在mRNA沉默和衰变中起关键作用,但聚集形成P小体并非功能所必需,而是其活性的结果。
