Single amino-acid mutation in a Drosoph ila melanogaster ribosomal protein: An insight in uL11 transcriptional activity

The ribosomal protein uL11 is located at the basis of the ribosome P-stalk and plays a paramount role in translational efficiency. In addition, no mutant for uL11 is available suggesting that this gene is haplo-insufficient as many other Ribosomal Protein Genes (RPGs). We have previously shown that...

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Autores principales: Grunchec, Héloïse, Deraze, Jérôme, Dardalhon-Cuménal, Delphine, Ribeiro, Valérie, Coléno-Costes, Anne, Dias, Karine, Bloyer, Sébastien, Mouchel-Vielh, Emmanuèle, Peronnet, Frédérique, Thomassin, Hélène
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2022
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9387862/
https://www.ncbi.nlm.nih.gov/pubmed/35981051
http://dx.doi.org/10.1371/journal.pone.0273198
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author Grunchec, Héloïse
Deraze, Jérôme
Dardalhon-Cuménal, Delphine
Ribeiro, Valérie
Coléno-Costes, Anne
Dias, Karine
Bloyer, Sébastien
Mouchel-Vielh, Emmanuèle
Peronnet, Frédérique
Thomassin, Hélène
author_facet Grunchec, Héloïse
Deraze, Jérôme
Dardalhon-Cuménal, Delphine
Ribeiro, Valérie
Coléno-Costes, Anne
Dias, Karine
Bloyer, Sébastien
Mouchel-Vielh, Emmanuèle
Peronnet, Frédérique
Thomassin, Hélène
author_sort Grunchec, Héloïse
collection PubMed
description The ribosomal protein uL11 is located at the basis of the ribosome P-stalk and plays a paramount role in translational efficiency. In addition, no mutant for uL11 is available suggesting that this gene is haplo-insufficient as many other Ribosomal Protein Genes (RPGs). We have previously shown that overexpression of Drosophila melanogaster uL11 enhances the transcription of many RPGs and Ribosomal Biogenesis genes (RiBis) suggesting that uL11 might globally regulate the level of translation through its transcriptional activity. Moreover, uL11 trimethylated on lysine 3 (uL11K3me3) interacts with the chromodomain of the Enhancer of Polycomb and Trithorax Corto, and both proteins co-localize with RNA Polymerase II at many sites on polytene chromosomes. These data have led to the hypothesis that the N-terminal end of uL11, and more particularly the trimethylation of lysine 3, supports the extra-ribosomal activity of uL11 in transcription. To address this question, we mutated the lysine 3 codon using a CRISPR/Cas9 strategy and obtained several lysine 3 mutants. We describe here the first mutants of D. melanogaster uL11. Unexpectedly, the uL11(K3A) mutant, in which the lysine 3 codon is replaced by an alanine, displays a genuine Minute phenotype known to be characteristic of RPG deletions (longer development, low fertility, high lethality, thin and short bristles) whereas the uL11(K3Y) mutant, in which the lysine 3 codon is replaced by a tyrosine, is unaffected. In agreement, the rate of translation decreases in uL11(K3A) but not in uL11(K3Y). Co-immunoprecipitation experiments show that the interaction between uL11 and the Corto chromodomain is impaired by both mutations. However, Histone Association Assays indicate that the mutant proteins still bind chromatin. RNA-seq analyses from wing imaginal discs show that Corto represses RPG expression whereas very few genes are deregulated in uL11 mutants. We propose that Corto, by repressing RPG expression, ensures that all ribosomal proteins are present at the correct stoichiometry, and that uL11 fine-tunes its transcriptional regulation of RPGs.
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spelling pubmed-93878622022-08-19 Single amino-acid mutation in a Drosoph ila melanogaster ribosomal protein: An insight in uL11 transcriptional activity Grunchec, Héloïse Deraze, Jérôme Dardalhon-Cuménal, Delphine Ribeiro, Valérie Coléno-Costes, Anne Dias, Karine Bloyer, Sébastien Mouchel-Vielh, Emmanuèle Peronnet, Frédérique Thomassin, Hélène PLoS One Research Article The ribosomal protein uL11 is located at the basis of the ribosome P-stalk and plays a paramount role in translational efficiency. In addition, no mutant for uL11 is available suggesting that this gene is haplo-insufficient as many other Ribosomal Protein Genes (RPGs). We have previously shown that overexpression of Drosophila melanogaster uL11 enhances the transcription of many RPGs and Ribosomal Biogenesis genes (RiBis) suggesting that uL11 might globally regulate the level of translation through its transcriptional activity. Moreover, uL11 trimethylated on lysine 3 (uL11K3me3) interacts with the chromodomain of the Enhancer of Polycomb and Trithorax Corto, and both proteins co-localize with RNA Polymerase II at many sites on polytene chromosomes. These data have led to the hypothesis that the N-terminal end of uL11, and more particularly the trimethylation of lysine 3, supports the extra-ribosomal activity of uL11 in transcription. To address this question, we mutated the lysine 3 codon using a CRISPR/Cas9 strategy and obtained several lysine 3 mutants. We describe here the first mutants of D. melanogaster uL11. Unexpectedly, the uL11(K3A) mutant, in which the lysine 3 codon is replaced by an alanine, displays a genuine Minute phenotype known to be characteristic of RPG deletions (longer development, low fertility, high lethality, thin and short bristles) whereas the uL11(K3Y) mutant, in which the lysine 3 codon is replaced by a tyrosine, is unaffected. In agreement, the rate of translation decreases in uL11(K3A) but not in uL11(K3Y). Co-immunoprecipitation experiments show that the interaction between uL11 and the Corto chromodomain is impaired by both mutations. However, Histone Association Assays indicate that the mutant proteins still bind chromatin. RNA-seq analyses from wing imaginal discs show that Corto represses RPG expression whereas very few genes are deregulated in uL11 mutants. We propose that Corto, by repressing RPG expression, ensures that all ribosomal proteins are present at the correct stoichiometry, and that uL11 fine-tunes its transcriptional regulation of RPGs. Public Library of Science 2022-08-18 /pmc/articles/PMC9387862/ /pubmed/35981051 http://dx.doi.org/10.1371/journal.pone.0273198 Text en © 2022 Grunchec et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Grunchec, Héloïse
Deraze, Jérôme
Dardalhon-Cuménal, Delphine
Ribeiro, Valérie
Coléno-Costes, Anne
Dias, Karine
Bloyer, Sébastien
Mouchel-Vielh, Emmanuèle
Peronnet, Frédérique
Thomassin, Hélène
Single amino-acid mutation in a Drosoph ila melanogaster ribosomal protein: An insight in uL11 transcriptional activity
title Single amino-acid mutation in a Drosoph ila melanogaster ribosomal protein: An insight in uL11 transcriptional activity
title_full Single amino-acid mutation in a Drosoph ila melanogaster ribosomal protein: An insight in uL11 transcriptional activity
title_fullStr Single amino-acid mutation in a Drosoph ila melanogaster ribosomal protein: An insight in uL11 transcriptional activity
title_full_unstemmed Single amino-acid mutation in a Drosoph ila melanogaster ribosomal protein: An insight in uL11 transcriptional activity
title_short Single amino-acid mutation in a Drosoph ila melanogaster ribosomal protein: An insight in uL11 transcriptional activity
title_sort single amino-acid mutation in a drosoph ila melanogaster ribosomal protein: an insight in ul11 transcriptional activity
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9387862/
https://www.ncbi.nlm.nih.gov/pubmed/35981051
http://dx.doi.org/10.1371/journal.pone.0273198
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