Ribosome stoichiometry: from form to function.

Emmott, Edward; Jovanović, Marko; Slavov, Nikolai

doi:10.7287/peerj.preprints.26991

Cited by 10 publications

(13 citation statements)

References 57 publications

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“…Of note, reversible adjustment of 26S proteasome assembly was also evident in other cell types, i.e., MEFs and primary human skin or lung fibroblasts, indicating a robust and conserved mechanism of metabolic fine-tuning of proteasome function. These findings add an important aspect of proteasome regulation and fit to the emerging concepts of fine-tuning of proteasome activity and also ribosome function according to cellular needs (Emmott et al, 2019;Meiners et al, 2014;Rousseau and Bertolotti, 2018;Wang et al, 2020).…”

Section: Discussionsupporting

confidence: 68%

Mitochondrial Regulation of the 26S Proteasome

et al. 2020

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Section: Discussionsupporting

confidence: 68%

Mitochondrial Regulation of the 26S Proteasome

et al. 2020

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“…At the same time recent work has provided ample evidence for subpopulations of ribosomes that differ in composition (Emmott et al, 2019;Ferretti and Karbstein, 2019;Genuth and Barna, 2018a, b;Sauert et al, 2015). While many of these are associated with disease states and arise from haploinsufficiency of ribosomal proteins (Bolze et al, 2013;Fortier et al, 2015;Kondrashov et al, 2011), others are found in wild type cells (Ferretti et al, 2017;Loveland et al, 2016;Shi et al, 2017;Slavov et al, 2015).…”

Section: Introductionmentioning

confidence: 99%

The chaperone Tsr2 regulates Rps26 release and reincorporation from mature ribosomes to enable a reversible, ribosome-mediated response to stress

Yang

Karbstein

2021

Preprint

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Although ribosome assembly is quality controlled to maintain protein homeostasis, different ribosome populations have been described. How these form, especially under stress conditions that impact energy levels and stop the energy-intensive production of ribosomes, remains unknown. Here we demonstrate how a physiologically relevant ribosome population arises during high Na+ and pH stress via dissociation of Rps26 from fully assembled ribosomes to enable a translational response to these stresses. The chaperone Tsr2 releases Rps26 in the presence of high Na or pH in vitro and is required for Rps26 release in vivo. Moreover, Tsr2 stores free Rps26 and promotes re-incorporation of the protein, thereby repairing the subunit after the stress subsides. Our data implicate a residue in Rps26 involved in Diamond Blackfan Anemia in mediating the effects of Na+. These data demonstrate how different ribosome populations can arise rapidly, without major energy input, and without bypass of quality control mechanisms.

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“…2B) and opens an entirely new avenue for drug development. On a side note, this concept is paralleled by an emerging fine-tuning of ribosome form and function (Emmott, Jovanovic, & Slavov, 2019;Xue & Barna, 2012) The aim of this review is to summarize the available evidence that supports a proteasome building block concept thereby providing a strong rationale for the defined targeting of distinct proteasome super-complexes in disease. We thereby hope to stimulate research on the regulation of the proteasome system under physiological and pathological conditions, which might ultimately lead to the development of tool compounds to study proteasome complexes in detail as well as of inno https://doi.org/10.1016/j.pharmthera.2020.107526 0163-7258/© 2020.…”

Section: Introductionmentioning

confidence: 99%