Discovery of 20 novel ribosomal leader candidates in bacteria and archaea

Abstract Background RNAs perform many functions in addition to supplying coding templates, such as binding proteins. RNA-protein interactions are important in multiple processes in all domains of life, and the discovery of additional protein-binding RNAs expands the scope for studying such interacti...

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Main Authors: Iris Eckert, Zasha Weinberg
Format: Article
Language:English
Published: BMC 2020-05-01
Series:BMC Microbiology
Subjects:
Online Access:http://link.springer.com/article/10.1186/s12866-020-01823-6
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spelling doaj-cedcc98e5c3340cebe6b902fb8aa5c942020-11-25T03:02:14ZengBMCBMC Microbiology1471-21802020-05-0120111210.1186/s12866-020-01823-6Discovery of 20 novel ribosomal leader candidates in bacteria and archaeaIris Eckert0Zasha Weinberg1Bioinformatics Group, Department of Computer Science and Interdisciplinary Centre for Bioinformatics, Leipzig UniversityBioinformatics Group, Department of Computer Science and Interdisciplinary Centre for Bioinformatics, Leipzig UniversityAbstract Background RNAs perform many functions in addition to supplying coding templates, such as binding proteins. RNA-protein interactions are important in multiple processes in all domains of life, and the discovery of additional protein-binding RNAs expands the scope for studying such interactions. To find such RNAs, we exploited a form of ribosomal regulation. Ribosome biosynthesis must be tightly regulated to ensure that concentrations of rRNAs and ribosomal proteins (r-proteins) match. One regulatory mechanism is a ribosomal leader (r-leader), which is a domain in the 5′ UTR of an mRNA whose genes encode r-proteins. When the concentration of one of these r-proteins is high, the protein binds the r-leader in its own mRNA, reducing gene expression and thus protein concentrations. To date, 35 types of r-leaders have been validated or predicted. Results By analyzing additional conserved RNA structures on a multi-genome scale, we identified 20 novel r-leader structures. Surprisingly, these included new r-leaders in the highly studied organisms Escherichia coli and Bacillus subtilis. Our results reveal several cases where multiple unrelated RNA structures likely bind the same r-protein ligand, and uncover previously unknown r-protein ligands. Each r-leader consistently occurs upstream of r-protein genes, suggesting a regulatory function. That the predicted r-leaders function as RNAs is supported by evolutionary correlations in the nucleotide sequences that are characteristic of a conserved RNA secondary structure. The r-leader predictions are also consistent with the locations of experimentally determined transcription start sites. Conclusions This work increases the number of known or predicted r-leader structures by more than 50%, providing additional opportunities to study structural and evolutionary aspects of RNA-protein interactions. These results provide a starting point for detailed experimental studies.http://link.springer.com/article/10.1186/s12866-020-01823-6Comparative genomicsRibosomal leaderBioinformaticsRNA-protein interactioncis-regulatory RNA
collection DOAJ
language English
format Article
sources DOAJ
author Iris Eckert
Zasha Weinberg
spellingShingle Iris Eckert
Zasha Weinberg
Discovery of 20 novel ribosomal leader candidates in bacteria and archaea
BMC Microbiology
Comparative genomics
Ribosomal leader
Bioinformatics
RNA-protein interaction
cis-regulatory RNA
author_facet Iris Eckert
Zasha Weinberg
author_sort Iris Eckert
title Discovery of 20 novel ribosomal leader candidates in bacteria and archaea
title_short Discovery of 20 novel ribosomal leader candidates in bacteria and archaea
title_full Discovery of 20 novel ribosomal leader candidates in bacteria and archaea
title_fullStr Discovery of 20 novel ribosomal leader candidates in bacteria and archaea
title_full_unstemmed Discovery of 20 novel ribosomal leader candidates in bacteria and archaea
title_sort discovery of 20 novel ribosomal leader candidates in bacteria and archaea
publisher BMC
series BMC Microbiology
issn 1471-2180
publishDate 2020-05-01
description Abstract Background RNAs perform many functions in addition to supplying coding templates, such as binding proteins. RNA-protein interactions are important in multiple processes in all domains of life, and the discovery of additional protein-binding RNAs expands the scope for studying such interactions. To find such RNAs, we exploited a form of ribosomal regulation. Ribosome biosynthesis must be tightly regulated to ensure that concentrations of rRNAs and ribosomal proteins (r-proteins) match. One regulatory mechanism is a ribosomal leader (r-leader), which is a domain in the 5′ UTR of an mRNA whose genes encode r-proteins. When the concentration of one of these r-proteins is high, the protein binds the r-leader in its own mRNA, reducing gene expression and thus protein concentrations. To date, 35 types of r-leaders have been validated or predicted. Results By analyzing additional conserved RNA structures on a multi-genome scale, we identified 20 novel r-leader structures. Surprisingly, these included new r-leaders in the highly studied organisms Escherichia coli and Bacillus subtilis. Our results reveal several cases where multiple unrelated RNA structures likely bind the same r-protein ligand, and uncover previously unknown r-protein ligands. Each r-leader consistently occurs upstream of r-protein genes, suggesting a regulatory function. That the predicted r-leaders function as RNAs is supported by evolutionary correlations in the nucleotide sequences that are characteristic of a conserved RNA secondary structure. The r-leader predictions are also consistent with the locations of experimentally determined transcription start sites. Conclusions This work increases the number of known or predicted r-leader structures by more than 50%, providing additional opportunities to study structural and evolutionary aspects of RNA-protein interactions. These results provide a starting point for detailed experimental studies.
topic Comparative genomics
Ribosomal leader
Bioinformatics
RNA-protein interaction
cis-regulatory RNA
url http://link.springer.com/article/10.1186/s12866-020-01823-6
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