Interaction of the La-related protein Slf1 with colliding ribosomes maintains translation of oxidative-stress responsive mRNAs

Author:

Jennings Martin D1,Srivastava Priya1,Kershaw Christopher J1,Talavera David2,Grant Christopher M1ORCID,Pavitt Graham D1ORCID

Affiliation:

1. Division of Molecular and Cellular Function, School of Biological Sciences, The University of Manchester , Manchester, M13 9PT, UK

2. Division of Cardiovascular Sciences, School of Medical Sciences, The University of Manchester , Manchester, M13 9PT, UK

Abstract

Abstract In response to oxidative stress cells reprogram gene expression to enhance levels of antioxidant enzymes and promote survival. In Saccharomyces cerevisiae the polysome-interacting La-related proteins (LARPs) Slf1 and Sro9 aid adaptation of protein synthesis during stress by undetermined means. To gain insight in their mechanisms of action in stress responses, we determined LARP mRNA binding positions in stressed and unstressed cells. Both proteins bind within coding regions of stress-regulated antioxidant enzyme and other highly translated mRNAs in both optimal and stressed conditions. LARP interaction sites are framed and enriched with ribosome footprints suggesting ribosome–LARP–mRNA complexes are identified. Although stress-induced translation of antioxidant enzyme mRNAs is attenuated in slf1Δ, these mRNAs remain on polysomes. Focusing further on Slf1, we find it binds to both monosomes and disomes following RNase treatment. slf1Δ reduces disome enrichment during stress and alters programmed ribosome frameshifting rates. We propose that Slf1 is a ribosome-associated translational modulator that stabilises stalled/collided ribosomes, prevents ribosome frameshifting and so promotes translation of a set of highly-translated mRNAs that together facilitate cell survival and adaptation to stress.

Funder

UK Biotechnology and Biological Research Council

University of Manchester

Publisher

Oxford University Press (OUP)

Subject

Genetics

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