SRNAbench and sRNAtoolbox 2019: intuitive fast small RNA profiling and differential expression

Ernesto Aparicio-Puerta; Ricardo Lebrón; Antonio Rueda; Cristina Gómez-Martín; Stavros Giannoukakos; David Jaspez; José María Medina; Andreja Zubkovic; Igor Jurak; Bastian Fromm; Juan Antonio Marchal; José Oliver; Michael Hackenberg

doi:https://doi.org/10.1093/nar/gkz415

SRNAbench and sRNAtoolbox 2019: intuitive fast small RNA profiling and differential expression

Ernesto Aparicio-Puerta, Ricardo Lebrón, Antonio Rueda, Cristina Gómez-Martín, Stavros Giannoukakos, David Jaspez, José María Medina, Andreja Zubkovic, Igor Jurak, Bastian Fromm, Juan Antonio Marchal, José Oliver, Michael Hackenberg

Pathology (VUmc)

Research output: Contribution to journal › Article › Academic › peer-review

111 Citations (Scopus)

Abstract

Since the original publication of sRNAtoolbox in 2015, small RNA research experienced notable advances in different directions. New protocols for small RNA sequencing have become available to address important issues such as adapter ligation bias, PCR amplification artefacts or to include internal controls such as spike-in sequences. New microRNA reference databases were developed with different foci, either prioritizing accuracy (low number of false positives) or completeness (low number of false negatives). Additionally, other small RNA molecules as well as microRNA sequence and length variants (isomiRs) have continued to gain importance. Finally, the number of microRNA sequencing studies deposited in GEO nearly triplicated from 2014 (280) to 2018 (764). These developments imply that fast and easy-to-use tools for expression profiling and subsequent downstream analysis of miRNA-seq data are essential to many researchers. Key features in this sRNAtoolbox release include addition of all major RNA library preparation protocols to sRNAbench and improvements in sRNAde, a tool that summarizes several aspects of small RNA sequencing studies including the detection of consensus differential expression. A special emphasis was put on the user-friendliness of the tools, for instance sRNAbench now supports parallel launching of several jobs to improve reproducibility and user time efficiency.

Original language	English
Pages (from-to)	W530-W535
Journal	Nucleic Acids Research
Volume	47
Issue number	W1
DOIs	https://doi.org/10.1093/nar/gkz415
Publication status	Published - 1 Jul 2019

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Aparicio-Puerta, E., Lebrón, R., Rueda, A., Gómez-Martín, C., Giannoukakos, S., Jaspez, D., Medina, J. M., Zubkovic, A., Jurak, I., Fromm, B., Marchal, J. A., Oliver, J., & Hackenberg, M. (2019). SRNAbench and sRNAtoolbox 2019: intuitive fast small RNA profiling and differential expression. Nucleic Acids Research, 47(W1), W530-W535. https://doi.org/10.1093/nar/gkz415

@article{85da005ddbc24d2086fafd633ccca052,

title = "SRNAbench and sRNAtoolbox 2019: intuitive fast small RNA profiling and differential expression",

abstract = "Since the original publication of sRNAtoolbox in 2015, small RNA research experienced notable advances in different directions. New protocols for small RNA sequencing have become available to address important issues such as adapter ligation bias, PCR amplification artefacts or to include internal controls such as spike-in sequences. New microRNA reference databases were developed with different foci, either prioritizing accuracy (low number of false positives) or completeness (low number of false negatives). Additionally, other small RNA molecules as well as microRNA sequence and length variants (isomiRs) have continued to gain importance. Finally, the number of microRNA sequencing studies deposited in GEO nearly triplicated from 2014 (280) to 2018 (764). These developments imply that fast and easy-to-use tools for expression profiling and subsequent downstream analysis of miRNA-seq data are essential to many researchers. Key features in this sRNAtoolbox release include addition of all major RNA library preparation protocols to sRNAbench and improvements in sRNAde, a tool that summarizes several aspects of small RNA sequencing studies including the detection of consensus differential expression. A special emphasis was put on the user-friendliness of the tools, for instance sRNAbench now supports parallel launching of several jobs to improve reproducibility and user time efficiency.",

author = "Ernesto Aparicio-Puerta and Ricardo Lebr{\'o}n and Antonio Rueda and Cristina G{\'o}mez-Mart{\'i}n and Stavros Giannoukakos and David Jaspez and Medina, {Jos{\'e} Mar{\'i}a} and Andreja Zubkovic and Igor Jurak and Bastian Fromm and Marchal, {Juan Antonio} and Jos{\'e} Oliver and Michael Hackenberg",

note = "Funding Information: European Union [765492 to M.H.]; Spanish Government [AGL2017-88702-C2-2-R to M.H., J.L.O.]; Instituto de Salud Carlos III, FEDER funds [PIE16/00045 to J.A.M.]; Chair {\textquoteleft}Doctors Galera-Requena in cancer stem cell research{\textquoteright} to JMA and by the Ministry of Education of Spain [FPU13/05662 to R.L., IFI16/00041 to E.A.]; Strategic Research Area (SFO) program of the Swedish Research Council (to V.R.) through Stockholm University (to B.F.). Funding for open access charge: Spanish Government [AGL2017-88702-C2-2-R]. Conflict of interest statement. None declared. Publisher Copyright: {\textcopyright} 2019 The Author(s).",

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doi = "https://doi.org/10.1093/nar/gkz415",

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T1 - SRNAbench and sRNAtoolbox 2019

T2 - intuitive fast small RNA profiling and differential expression

AU - Aparicio-Puerta, Ernesto

AU - Lebrón, Ricardo

AU - Rueda, Antonio

AU - Gómez-Martín, Cristina

AU - Giannoukakos, Stavros

AU - Jaspez, David

AU - Medina, José María

AU - Zubkovic, Andreja

AU - Jurak, Igor

AU - Fromm, Bastian

AU - Marchal, Juan Antonio

AU - Oliver, José

AU - Hackenberg, Michael

N1 - Funding Information: European Union [765492 to M.H.]; Spanish Government [AGL2017-88702-C2-2-R to M.H., J.L.O.]; Instituto de Salud Carlos III, FEDER funds [PIE16/00045 to J.A.M.]; Chair ‘Doctors Galera-Requena in cancer stem cell research’ to JMA and by the Ministry of Education of Spain [FPU13/05662 to R.L., IFI16/00041 to E.A.]; Strategic Research Area (SFO) program of the Swedish Research Council (to V.R.) through Stockholm University (to B.F.). Funding for open access charge: Spanish Government [AGL2017-88702-C2-2-R]. Conflict of interest statement. None declared. Publisher Copyright: © 2019 The Author(s).

PY - 2019/7/1

Y1 - 2019/7/1

N2 - Since the original publication of sRNAtoolbox in 2015, small RNA research experienced notable advances in different directions. New protocols for small RNA sequencing have become available to address important issues such as adapter ligation bias, PCR amplification artefacts or to include internal controls such as spike-in sequences. New microRNA reference databases were developed with different foci, either prioritizing accuracy (low number of false positives) or completeness (low number of false negatives). Additionally, other small RNA molecules as well as microRNA sequence and length variants (isomiRs) have continued to gain importance. Finally, the number of microRNA sequencing studies deposited in GEO nearly triplicated from 2014 (280) to 2018 (764). These developments imply that fast and easy-to-use tools for expression profiling and subsequent downstream analysis of miRNA-seq data are essential to many researchers. Key features in this sRNAtoolbox release include addition of all major RNA library preparation protocols to sRNAbench and improvements in sRNAde, a tool that summarizes several aspects of small RNA sequencing studies including the detection of consensus differential expression. A special emphasis was put on the user-friendliness of the tools, for instance sRNAbench now supports parallel launching of several jobs to improve reproducibility and user time efficiency.

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SP - W530-W535

JO - Nucleic Acids Research

JF - Nucleic Acids Research

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ER -

SRNAbench and sRNAtoolbox 2019: intuitive fast small RNA profiling and differential expression

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