Genome-wide screening reveals metabolic regulation of stop-codon readthrough by cyclic AMP

Author:

Lyu Zhihui1,Villanueva Patricia1,O’Malley Liam1,Murphy Parker1,Augenstreich Jacques1,Briken Volker1,Singh Abhyudai2,Ling Jiqiang1ORCID

Affiliation:

1. Department of Cell Biology and Molecular Genetics, The University of Maryland, College Park , MD , USA

2. Department of Electrical and Computer Engineering and Biomedical Engineering, University of Delaware , Newark , DE , USA

Abstract

Abstract Translational fidelity is critical for microbial fitness, survival and stress responses. Much remains unknown about the genetic and environmental control of translational fidelity and its single-cell heterogeneity. In this study, we used a high-throughput fluorescence-based assay to screen a knock-out library of Escherichia coli and identified over 20 genes critical for stop-codon readthrough. Most of these identified genes were not previously known to affect translational fidelity. Intriguingly, we show that several genes controlling metabolism, including cyaA and crp, enhance stop-codon readthrough. CyaA catalyzes the synthesis of cyclic adenosine monophosphate (cAMP). Combining RNA sequencing, metabolomics and biochemical analyses, we show that deleting cyaA impairs amino acid catabolism and production of ATP, thus repressing the transcription of rRNAs and tRNAs to decrease readthrough. Single-cell analyses further show that cAMP is a major driver of heterogeneity in stop-codon readthrough and rRNA expression. Our results highlight that carbon metabolism is tightly coupled with stop-codon readthrough.

Funder

National Institute of General Medical Sciences

Publisher

Oxford University Press (OUP)

Subject

Genetics

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