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eIF4F complex dynamics are important for the activation of the integrated stress response

Kyusik Q. Kim, Ankanahalli N. Nanjaraj Urs, Victor Lasehinde, Alison C. Greenlaw, Benjamin H. Hudson, Hani Zaher

2024Molecular Cell10 citationsDOIOpen Access PDF

Abstract

In response to stress, eukaryotes activate the integrated stress response (ISR) via phosphorylation of eIF2α to promote the translation of pro-survival effector genes, such as GCN4 in yeast. Complementing the ISR is the target of rapamycin (TOR) pathway, which regulates eIF4E function. Here, we probe translational control in the absence of eIF4E in Saccharomyces cerevisiae. Intriguingly, we find that loss of eIF4E leads to de-repression of GCN4 translation. In addition, we find that de-repression of GCN4 translation is accompanied by neither eIF2α phosphorylation nor reduction in initiator ternary complex (TC). Our data suggest that when eIF4E levels are depleted, GCN4 translation is de-repressed via a unique mechanism that may involve faster scanning by the small ribosome subunit due to increased local concentration of eIF4A. Overall, our findings suggest that relative levels of eIF4F components are key to ribosome dynamics and may play important roles in translational control of gene expression.

Topics & Concepts

EIF4EBiologyTranslation (biology)Initiation factorEukaryotic translationCell biologyeIF2Eukaryotic initiation factorIntegrated stress responseEffectorPsychological repressioneIF4ATranslational regulationRibosomePhosphorylationProtein biosynthesisEukaryotic Small Ribosomal SubunitMessenger RNAGeneticsGene expressionGeneRNARNA and protein synthesis mechanismsPolyamine Metabolism and ApplicationsFungal and yeast genetics research