Reproducible analysis of sequencing-based RNA structure probing data with user-friendly tools

Lukasz Jan Kielpinski; Nikos Sidiropoulos; Jeppe Vinther

doi:10.1016/bs.mie.2015.01.014

Reproducible analysis of sequencing-based RNA structure probing data with user-friendly tools

Lukasz Jan Kielpinski, Nikos Sidiropoulos, Jeppe Vinther^*

^*Corresponding author af dette arbejde

Bioinformatik og RNA Biologi

7 Citationer (Scopus)

Abstract

RNA structure-probing data can improve the prediction of RNA secondary and tertiary structure and allow structural changes to be identified and investigated. In recent years, massive parallel sequencing has dramatically improved the throughput of RNA structure probing experiments, but at the same time also made analysis of the data challenging for scientists without formal training in computational biology. Here, we discuss different strategies for data analysis of massive parallel sequencing-based structure-probing data. To facilitate reproducible and standardized analysis of this type of data, we have made a collection of tools, which allow raw sequencing reads to be converted to normalized probing values using different published strategies. In addition, we also provide tools for visualization of the probing data in the UCSC Genome Browser and for converting RNA coordinates to genomic coordinates and vice versa. The collection is implemented as functions in the R statistical environment and as tools in the Galaxy platform, making them easily accessible for the scientific community. We demonstrate the usefulness of the collection by applying it to the analysis of sequencing-based hydroxyl radical probing data and comparing different normalization strategies.

Originalsprog	Engelsk
Titel	Structures of large RNA molecules and their complexes
Redaktører	Sarah A. Woodson, Frédéric H.T. Allain
Antal sider	28
Forlag	Elsevier
Publikationsdato	2015
Sider	153-180
Kapitel	6
ISBN (Elektronisk)	978-0-12-801934-4
DOI	https://doi.org/10.1016/bs.mie.2015.01.014
Status	Udgivet - 2015

Navn	Methods in Enzymology
Vol/bind	558
ISSN	0076-6879

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10.1016/bs.mie.2015.01.014

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Reproducible analysis of sequencing-based RNA structure probing data with user-friendly tools. / Kielpinski, Lukasz Jan; Sidiropoulos, Nikos ; Vinther, Jeppe.

Structures of large RNA molecules and their complexes. red. / Sarah A. Woodson; Frédéric H.T. Allain. Elsevier, 2015. s. 153-180 (Methods in Enzymology, Bind 558).

Publikation: Bidrag til bog/antologi/rapport › Bidrag til bog/antologi › Forskning › peer review

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abstract = "RNA structure-probing data can improve the prediction of RNA secondary and tertiary structure and allow structural changes to be identified and investigated. In recent years, massive parallel sequencing has dramatically improved the throughput of RNA structure probing experiments, but at the same time also made analysis of the data challenging for scientists without formal training in computational biology. Here, we discuss different strategies for data analysis of massive parallel sequencing-based structure-probing data. To facilitate reproducible and standardized analysis of this type of data, we have made a collection of tools, which allow raw sequencing reads to be converted to normalized probing values using different published strategies. In addition, we also provide tools for visualization of the probing data in the UCSC Genome Browser and for converting RNA coordinates to genomic coordinates and vice versa. The collection is implemented as functions in the R statistical environment and as tools in the Galaxy platform, making them easily accessible for the scientific community. We demonstrate the usefulness of the collection by applying it to the analysis of sequencing-based hydroxyl radical probing data and comparing different normalization strategies.",

author = "Kielpinski, {Lukasz Jan} and Nikos Sidiropoulos and Jeppe Vinther",

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N2 - RNA structure-probing data can improve the prediction of RNA secondary and tertiary structure and allow structural changes to be identified and investigated. In recent years, massive parallel sequencing has dramatically improved the throughput of RNA structure probing experiments, but at the same time also made analysis of the data challenging for scientists without formal training in computational biology. Here, we discuss different strategies for data analysis of massive parallel sequencing-based structure-probing data. To facilitate reproducible and standardized analysis of this type of data, we have made a collection of tools, which allow raw sequencing reads to be converted to normalized probing values using different published strategies. In addition, we also provide tools for visualization of the probing data in the UCSC Genome Browser and for converting RNA coordinates to genomic coordinates and vice versa. The collection is implemented as functions in the R statistical environment and as tools in the Galaxy platform, making them easily accessible for the scientific community. We demonstrate the usefulness of the collection by applying it to the analysis of sequencing-based hydroxyl radical probing data and comparing different normalization strategies.

AB - RNA structure-probing data can improve the prediction of RNA secondary and tertiary structure and allow structural changes to be identified and investigated. In recent years, massive parallel sequencing has dramatically improved the throughput of RNA structure probing experiments, but at the same time also made analysis of the data challenging for scientists without formal training in computational biology. Here, we discuss different strategies for data analysis of massive parallel sequencing-based structure-probing data. To facilitate reproducible and standardized analysis of this type of data, we have made a collection of tools, which allow raw sequencing reads to be converted to normalized probing values using different published strategies. In addition, we also provide tools for visualization of the probing data in the UCSC Genome Browser and for converting RNA coordinates to genomic coordinates and vice versa. The collection is implemented as functions in the R statistical environment and as tools in the Galaxy platform, making them easily accessible for the scientific community. We demonstrate the usefulness of the collection by applying it to the analysis of sequencing-based hydroxyl radical probing data and comparing different normalization strategies.

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Reproducible analysis of sequencing-based RNA structure probing data with user-friendly tools

Abstract

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