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DEAD-box ATPases 是相分离细胞器的全局调节因子。

DEAD-box ATPases are global regulators of phase-separated organelles.

机构信息

Institute of Biochemistry, ETH Zurich, Zurich, Switzerland.

Department of Cell Biology, University of Texas Southwestern Medical Center, Dallas, TX, USA.

出版信息

Nature. 2019 Sep;573(7772):144-148. doi: 10.1038/s41586-019-1502-y. Epub 2019 Aug 21.

Abstract

The ability of proteins and nucleic acids to undergo liquid-liquid phase separation has recently emerged as an important molecular principle of how cells rapidly and reversibly compartmentalize their components into membrane-less organelles such as the nucleolus, processing bodies or stress granules. How the assembly and turnover of these organelles are controlled, and how these biological condensates selectively recruit or release components are poorly understood. Here we show that members of the large and highly abundant family of RNA-dependent DEAD-box ATPases (DDXs) are regulators of RNA-containing phase-separated organelles in prokaryotes and eukaryotes. Using in vitro reconstitution and in vivo experiments, we demonstrate that DDXs promote phase separation in their ATP-bound form, whereas ATP hydrolysis induces compartment turnover and release of RNA. This mechanism of membrane-less organelle regulation reveals a principle of cellular organization that is conserved from bacteria to humans. Furthermore, we show that DDXs control RNA flux into and out of phase-separated organelles, and thus propose that a cellular network of dynamic, DDX-controlled compartments establishes biochemical reaction centres that provide cells with spatial and temporal control of various RNA-processing steps, which could regulate the composition and fate of ribonucleoprotein particles.

摘要

蛋白质和核酸进行液-液相分离的能力最近成为了一个重要的分子原理,它解释了细胞如何快速且可逆地将其成分分隔到无膜细胞器中,如核仁、处理体或应激颗粒。这些细胞器的组装和周转是如何控制的,以及这些生物凝聚物如何选择性地招募或释放成分,这些都知之甚少。在这里,我们表明,RNA 依赖性 DEAD -box ATP 酶(DDX)的大型且高度丰富的家族成员是原核生物和真核生物中含 RNA 的相分离细胞器的调节剂。通过体外重组和体内实验,我们证明 DDXs 在其 ATP 结合形式下促进相分离,而 ATP 水解诱导隔室周转和 RNA 的释放。这种无膜细胞器调节的机制揭示了一种从细菌到人类都保守的细胞组织原则。此外,我们表明 DDXs 控制 RNA 进入和离开相分离细胞器的通量,因此我们提出了一个动态的、由 DDX 控制的隔室的细胞网络,它为细胞提供了对各种 RNA 处理步骤的时空控制,这可以调节核糖核蛋白颗粒的组成和命运。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/669e/7617057/e7ce416f0f90/EMS83777-f005.jpg

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