A molecular network of conserved factors keeps ribosomes dormant in the egg

核糖体 生物 细胞生物学 计算生物学 遗传学 核糖核酸 基因
作者
Friederike Leesch,Laura Lorenzo‐Orts,Carina Pribitzer,Irina Grishkovskaya,Josef Roehsner,Anastasia Chugunova,Manuel Matzinger,Elisabeth Roitinger,Katarina Belačić,Susanne Kandolf,Tzi-Yang Lin,Karl Mechtler,Anton Meinhart,David Haselbach,Andrea Pauli
出处
期刊:Nature [Springer Nature]
卷期号:613 (7945): 712-720 被引量:12
标识
DOI:10.1038/s41586-022-05623-y
摘要

Ribosomes are produced in large quantities during oogenesis and are stored in the egg. However, the egg and early embryo are translationally repressed1–4. Here, using mass spectrometry and cryo-electron microscopy analyses of ribosomes isolated from zebrafish (Danio rerio) and Xenopus laevis eggs and embryos, we provide molecular evidence that ribosomes transition from a dormant state to an active state during the first hours of embryogenesis. Dormant ribosomes are associated with four conserved factors that form two modules, consisting of Habp4–eEF2 and death associated protein 1b (Dap1b) or Dap in complex with eIF5a. Both modules occupy functionally important sites and act together to stabilize ribosomes and repress translation. Dap1b (also known as Dapl1 in mammals) is a newly discovered translational inhibitor that stably inserts into the polypeptide exit tunnel. Addition of recombinant zebrafish Dap1b protein is sufficient to block translation and reconstitute the dormant egg ribosome state in a mammalian translation extract in vitro. Thus, a developmentally programmed, conserved ribosome state has a key role in ribosome storage and translational repression in the egg. Mass spectrometry and structural studies demonstrate the specific changes in protein composition that accompany the transition of ribosomes in zebrafish and Xenopus eggs from a dormant to an active state during early embryogenesis.
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