RegRNA: an integrated web server for identifying regulatory RNA motifs and elements

Hsi-Yuan Huang¹, Chia-Hung Chien¹, Kuan-Hua Jen¹ and Hsien-Da Huang¹^,2^,3^,*

¹ Institute of Bioinformatics, National Chiao Tung University Hsin-Chu 300, Taiwan ² Department of Biological Science and Technology, National Chiao Tung University Hsin-Chu 300, Taiwan ³ Core Facility for Structural Bioinformatics, National Chiao Tung University Hsin-Chu 300, Taiwan

^*To whom correspondence should be addressed. Tel: +886 3 5712121, ext. 56952; Fax: +886 3 5739320; Email: bryan{at}mail.nctu.edu.tw

Received February 14, 2006. Revised March 7, 2006. Accepted April 14, 2006.

ABSTRACT

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Numerous regulatory structural motifs have been identified asplaying essential roles in transcriptional and post-transcriptionalregulation of gene expression. RegRNA is an integrated web serverfor identifying the homologs of regulatory RNA motifs and elementsagainst an input mRNA sequence. Both sequence homologs and structuralhomologs of regulatory RNA motifs can be recognized. The regulatoryRNA motifs supported in RegRNA are categorized into severalclasses: (i) motifs in mRNA 5'-untranslated region (5'-UTR)and 3'-UTR; (ii) motifs involved in mRNA splicing; (iii) motifsinvolved in transcriptional regulation; (iv) riboswitches; (v)splicing donor/acceptor sites; (vi) inverted repeats; and (vii)miRNA target sites. The experimentally validated regulatoryRNA motifs are extracted from literature survey and severalregulatory RNA motif databases, such as UTRdb, TRANSFAC, alternativesplicing database (ASD) and miRBase. A variety of computationalprograms are integrated for identifying the homologs of theregulatory RNA motifs. An intuitive user interface is designedto facilitate the comprehensive annotation of user-submittedmRNA sequences. The RegRNA web server is now available at http://RegRNA.mbc.NCTU.edu.tw/.

INTRODUCTION

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INTRODUCTION
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A substantial number of mRNA structural motifs have been identifiedas playing essential roles in transcriptional and post-transcriptionalregulation of gene expression, including transcription termination,mRNA localization and stability, mRNA alternative splicing andtranslation efficiency (1). For instance, riboswitches are complexfolded RNA domains found in non-coding parts of various mRNAs,where they control gene expression by harnessing allostericstructural changes (2). In numerous cases, specific functionalRNA elements whose biological activity relies on their primarysequences and specific secondary structures, act either as targetsites for RNA-binding factors or directly interact with translationmachinery (3). Since ligand-binding and base pairing are fundamentalfeatures of RNA interactions and activities, many of such smallregulatory RNA motifs likely exist in cells (4).

Previous research indicates that exonic splicing enhancer (ESE)is a binding site of serine/arginine-rich proteins (SR proteins),which belong to a family of conserved splicing factors and werefirst implicated in splicing when discovered that they are componentsof the spliceosome (5). MicroRNAs (miRNAs) are small RNA molecules,which are $~$ 22 nt sequences play critical roles in translationalregulation and degradation of mRNA by hybridizing to miRNA targetsites within the 3'-untranslated region (3'-UTR) of the mRNAs.

Rfam is a comprehensive collection of non-coding RNA (ncRNA)families, represented by multiple sequence alignments and profilestochastic context-free grammars (6). It facilitates the identificationand classification of new members of known sequence families,and distributes annotation of ncRNAs in over 200 complete genomesequences.

The PatSearch software (7) can search user-submitted sequencesfor any combination of sequence patterns represented as positionalweighted matrix (PWMs) and structural motifs and allow the mismatchand mispairing search under a user-designated threshold. Transterm(8) provides data for principal regions, such as UTRs and ORFs,in mRNA sequences and regulatory RNA motifs, and allows usersto investigate their own motifs or mRNA sequences. These motifsare typically located in the 3'-UTR, 5'-UTR and coding regions.Riboswitch finder (9) and RibEx (10) were developed to determineknown riboswitches in a given sequence. UTRscan (11) allowsusers searching in submitted sequences for regulatory motifscollected in UTRsite (3). ESEfinder (12) is a web resource foridentifying a series of ESEs in mRNA sequences. RNAMotif (13)devises the definition of RNA structural descriptor to describean RNA structure motif and scan the input sequences for structuralhomologs of regulatory RNA motifs and elements (13).

Survey results indicate that various approaches can be usedfor predicting regulatory RNA motifs. Additionally, variousdatabases and web servers have accumulated regulatory RNA motifsduring the last few decades. Therefore, in order to annotateregulatory RNA motifs in messenger RNAs, the integration ofnumerous databases of regulatory RNA motifs and computationalanalytical tools are crucial.

The purpose of this work is to develop an integrated web server,RegRNA, to identify homologs of the regulatory RNA motifs andelements against an input mRNA sequence. Both sequence homologsand structural homologs of regulatory RNA motifs can be recognized.RegRNA not only extracts known regulatory RNA motifs by surveyingliteratures and several regulatory RNA motif databases, suchas UTRdb (3), TRANSFAC (14), alternative splicing database (ASD)(15) and miRBase (16), but also collects known regulatory RNAmotifs including motifs in 5'-UTR and 3'-UTR, and motifs involvedin transcriptional regulation, exonic/intronic splicing motifs,splicing donor/acceptor sites, inverted repeats, and miRNA targetsites. A variety of computational programs for different typesof regulatory RNA motifs were also implemented. Moreover, RegRNAdisplays prediction results in a graphical interface generatedby various integrated analytical tools, and allows users toannotate their own experimental sequences or to discover homologsof their desired motifs.

DESIGN AND IMPLEMENTATION

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INTRODUCTION
DESIGN AND IMPLEMENTATION
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CASE STUDY
DISCUSSION AND CONCLUSION
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Data collection
The regulatory RNA motifs supported in RegRNA are categorizedinto several classes: (i) motifs in mRNA 5'-UTR and 3'-UTR;(ii) motifs involved in mRNA splicing; (iii) motifs involvedin transcriptional regulation; (iv) riboswitches; (v) splicingdonor/acceptor sites; (vi) inverted repeat; and (vii) miRNAtarget sites. Figure 1 shows the information and processingflow of RegRNA

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Figure 1 RegRNA information and processing flow.

This work collected known regulatory RNA motifs and elementsvia literature survey and by integrating a variety of regulatoryRNA motif databases, such as UTRSite (3), TRANSFAC (14), ASD(15), miRBase (16) and miRNAMap (17). The UTRSite (Release 16)stores a collection of regulatory RNA located in 5'-UTR and3'-UTR, whose function and structure were experimentally determined(3). The TRANSFAC database (Release 7.4) (14) collects knowntranscriptional factors, their binding sites, nucleotide distributionmatrices and regulated genes. Those transcriptional regulatorysites located in pre-mRNA or mature mRNA sequences were extracted.Such sites can occur in 5'-UTR, introns or exons. Riboswitchesare natural genetic control elements typically located in UTRof mRNA sequence to form a binding pocket for a metabolite thatregulates that gene expression. Other features, such as riboswitchstructural motifs, were also extracted by surveying literatures.

The ASD is a literature-based dataset containing sequences andproperties of alternatively spliced exons, functional enumerationof observed splicing events, and characterization of splicingregulatory elements (15). In addition to the well-known splicesites, such as donor sites and acceptor sites, the conservedsequences in exonic and intronic regions are reportedly involvedin an alternative splicing mechanism. Besides the splicing motifsfrom ASD, numerous ESE and exonic splicing silencers (ESS) wereobtained from literatures. The miRBase database (Release 7.1)(16) provides comprehensive microRNA sequence data, annotationand predicted gene targets. The known miRNA genes in three mammaliangenomes—human, mouse and rat—were obtained frommiRBase (16).

Therefore, the RegRNA currently collects 1274 regulatory motifs(Table 1). For instance, there are 40 regulatory RNA motifslocated in 5'-UTR and 3'-UTR. The number of motifs involvedin splicing is 43. Totally, 744 known miRNAs in humans, miceand rats were obtained.

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Table 1 Statistics of types of regulatory RNA motifs in RegRNA

Integrated analytical tools
As to the regulatory RNA motifs in the form of primary structuresrepresented as consensus patterns or sequence patterns, RegRNAintegrates several motif identification tools, such as EMBOSS—fuzznuc(18), EMBOSS—einverted (18), and GeneSplicer (19) to detectthe homologs of the regulatory RNA motifs (Table 2).

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Table 2 Computational analysis tools applied in RegRNA

The fuzznuc of EMBOSS package is applied to search a consensuspattern against a sequence. The einverted of EMBOSS packageis utilized to detect inverted repeats in a nucleotide sequence.GeneSplicer (19) was developed for determining splice sitesin eukaryotic mRNA by combining several schemes that have alreadyproven successful in characterizing the patterns surroundingdonor and acceptor sites. Moreover, in identifying miRNA targets,miRanda (20) is employed to detect the miRNA target sites ina sequence that complimentary hybridizes to the mature miRNAs.The minimum free energy (MFE) of miRNA–target duplex isdetermined by miRanda when predicting miRNA target sites.

As to the regulatory RNA motifs in the form of secondary structuresrepresented as RNA structural descriptors (13), RegRNA integratesRNAMotif to identify homologs of regulatory RNA structural motifsin user-submitted sequences (Table 2). Some of regulatory RNAmotifs in 5'-UTR and 3'-UTR and riboswitches are representedas RNA structural descriptors in advance for searching the homologsagainst the user-submitted sequences.

INTERFACE

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The RegRNA web server devised a variety of interface to facilitatethe analysis for the homologs of the regulatory RNA motifs.Users can submit a sequence by inputting the accession numberfor retrieving mRNA sequence from RefSeq database (21), inputtinga single sequence in FASTA format, or uploading a sequence file(Figure 2a, label 1). Subsequently, users select the sequencetype—pre-mRNA or mature mRNA (Figure 2a, label 2). Whenthe input sequence is specified as a mature mRNA sequence, theprediction of the splicing site and the identification of intronicregulatory RNA motifs are not applied. Finally, users must decidewhich types of regulatory RNA motifs to be investigated by justclicking the checkbox (Figure 2a, label 3). Additionally, inpredicting miRNA target sites, users can adjust the MFE thresholdand score threshold to filter miRNA targets of interest.

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Figure 2 (a) Prediction page of the RegRNA website. (b) The result web page to graphically reveal the location of the homologs in regulatory RNA motifs and elements.

Upon submission to the website, the input sequence is then analyzedand the prediction results are presented via both textual interfaceand graphical interface (Figure 2b). Users can dsitinguish clearlybetween different regulatory RNA motifs and link to detaileddescriptions via hyperlinks. If the detected homologs are regulatoryRNA structural motifs, the RNA secondary structure of the detectedhomologs are generated by mfold (22) and provided on the web.

CASE STUDY

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In order to demonstrate the functionality of RegRNA, the authorsuse a case study, such as iron response element (IRE), whichis a particular hairpin structure located in the 5'-UTR or 3'-UTRof various mRNAs involved in cellular iron metabolism (23).Supplementary Figure S1 (See Supplementary Data) illustrateshow the IRE structural motif regulates iron concentrations.For example, two different IREs present their conservation ofsequence and structure determinants (Supplementary Figure S2)(23).

Subsequently, RegRNA detected homologs of IRE motif in a givenRNA sequence. For instance, a sequence with the accession numberof EMBL, AF068225, was obtained from Rfam (6). SupplementaryFigure S3 (See Supplementary Data) presents the predictive resultsof this case study. The IRE motif in the given RNA sequencewas accurately identified by the proposed RegRNA.

DISCUSSION AND CONCLUSION

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The RegRNA is capable of identifying homologs of plentiful typesof regulatory RNA motifs. Table 3 gives the comparison of RegRNAwith other previously developed tools including RNAMotif (13),PatSearch (7), RibEx (10), Riboswitch Finder (9), UTRScan (3)and Transterm (8). RibEx and Riboswitch Finder are developedto specially identify known riboswitches. Besides RNAMotif,all of the tools collected specific regulatory RNA motifs foridentifying their homologs in sequences. RNAMotif, PatSearchand RegRNA allow the user-defined RNA structural motif for theanalysis. In summary, the RegRNA provides more plentiful typesof regulatory RNA motifs than other tools.

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Table 3 Comparison of RegRNA to other tools and web sites

During the miRNA target prediction, the lower MFE values ofthe miRNAs and the target sites reveal that the energeticallymore probable hybridizations between the miRNAs and the targetgenes. Additionally, the predictive parameters including miRandaMFE and miRanda score were adjusted for the miRNA target predictionby comparing the predictive results to known miRNA/targets dataaccording to our previous works (17). The MFE threshold of themiRNA and target duplex was suggested as –16 kcal/moland the miRanda score was specified as 160.

Comparing the proposed RegRNA with Rfam database (6), the substantialdifference between the two resources is that RegRNA aims onthe annotation of regulatory RNA motifs and structural elementspotentially involving in gene post-transcriptional regulation,while Rfam mainly aims on the collection of ncRNA families anda variety of regulatory RNA structural motifs. The authors comparethe Rfam database and RegRNA web server in two aspects, thetypes of RNA data collected and the analyzing functions supported.Firstly, the comparing lists of the types of RNA data collectedin the two resources are given in Supplementary Table S1 (SeeSupplementary Data). Rfam collects the ncRNA families includingrRNA, tRNA, frameshift elements, riboswitches, thermoregulators,IRES and functional elements in UTR. However, RegRNA does notcollect the ncRNA sequences, frameshift elements, thermoregulatorsand IRES. For the investigation the transcriptional and post-transcriptionalregulation, RegRNA specially collects other regulatory RNA motifsincluding transcriptional regulatory motifs, splicing sites,exonic and intronic splicing motifs and microRNAs.

In the aspect of the supported analyzing functions (SupplementaryTable S2, See Supplementary Data), RegRNA provides the annotationof the input RNA sequences for candidates of regulatory RNAstructural motifs and regulatory RNA elements, which potentiallyinvolve in gene transcriptional and post-transcriptional regulation.Rfam facilitates the identification of the particular regionswithin the input sequences that are homologous to the ncRNAsand regulatory RNA motifs collected in Rfam. Moreover, our proposedRegRNA specially provides the identification of splicing sites,the detection of splicing-related regulatory motifs, the detectionof transcriptional regulatory motifs, the detection of invertedrepeats, and the identification of miRNA target sites in theinput messenger RNA sequences.

Besides the regulatory RNA motifs collected in RegRNA, additionalregulatory motifs were discovered in mRNA sequences, for example,pseudoknot, can be integrated into the RegRNA to make RegRNAmore comprehensive. Pseudoknots occur in the secondary structureof numerous RNA molecules, such as ribosomal RNAs, the catalyticcore of group I introns, RNase P RNAs and viral RNAs. In numerouscases, pseudoknots have functional roles in, e.g. ribosomalframeshifting, regulation of translation and splicing, and selinocysteinbiosynthesis (24). When considering to known miRNAs, miRNAMap(17) also collects putative miRNAs in human, mouse, rat anddog genomes. The putative miRNAs will be integrated into RegRNAin the future.

Although the proposed RegRNA provides comprehensive analysisfor regulatory RNA motifs, it requires about 20 s if all kindsof the regulatory RNA motifs are selected for analysis. Theconserved regions of the ncRNA families and the regulatory RNAmotifs collected in Rfam are suitable for the RNA structuralanalyses supported in RegRNA. The authors plan to convert theconsensus structures of ncRNA families in Rfam into the descriptorsof RNA structural motifs, which can be maintained in RegRNAto support the annotation of regulatory RNA motifs against theinput of RNA sequences. Consequently, reduction of the predictiontime is another task. Perhaps, utilizing the concept of a distributedsystem to parallel predict different regulatory motifs willdecrease the run time.

The RegRNA is an integrated web server for identifying knownregulatory RNA motif in RNA sequences. The main contributionsof this work are as follows: (i) the collection of the knownregulatory RNA motifs and elements from literatures and multiplebiological databases; (ii) the integration of a variety of motifidentification tools for regulatory RNA motifs both in primaryand secondary structure; (iii) providing intuitive interfaceto facilitate the presentation of plentiful information providedin the proposed RegRNA; (iv) providing a convenient solutionfor comprehensively annotating the mRNA sequence for regulatorymechanism involved by regulatory RNA motifs and elements.

AVAILABILITY

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The RegRNA web server will be continuously maintained and updated.The web server is now freely available at http://RegRNA.mbc.nctu.edu.tw/.

SUPPLEMENTARY DATA

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Supplementary Data are available at NAR Online.

ACKNOWLEDGEMENTS

The authors would like to thank the National Science Councilof the Republic of China for financially supporting this researchunder Contract No. NSC 95-3112-E-009-002. Special thanks forthe financial support from the National Research Program ForGenomic Medicine (NRPGM), Taiwan. This work was also partiallysupported by MOE ATU. Funding to pay the Open Access publicationcharges for this article was provided by National Science Councilof the Republic of China.

Conflict of interest statement. None declared.

REFERENCES

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				K. Nakata, B. K. Lipska, T. M. Hyde, T. Ye, E. N. Newburn, Y. Morita, R. Vakkalanka, M. Barenboim, Y. Sei, D. R. Weinberger, et al. DISC1 splice variants are upregulated in schizophrenia and associated with risk polymorphisms PNAS, September 15, 2009; 106(37): 15873 - 15878. [Abstract] [Full Text] [PDF]

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				W.-F. Shen, Y.-L. Hu, L. Uttarwar, E. Passegue, and C. Largman MicroRNA-126 Regulates HOXA9 by Binding to the Homeobox Mol. Cell. Biol., July 15, 2008; 28(14): 4609 - 4619. [Abstract] [Full Text] [PDF]

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RegRNA: an integrated web server for identifying regulatory RNA motifs and elements