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Disease-Associated Mutations That Alter the RNA Structural Ensemble 英文参考文献
Disease-AssociatedMutationsThatAltertheRNA
StructuralEnsemble
MatthewHalvorsen1,JoshuaS.Martin2,SamBroadaway2,AlainLaederach1,2*
1BiomedicalSciencesDepartment,UniversityatAlbany,Albany,NewYork,UnitedStatesofAmerica,2DevelopmentalGeneticsandBioinformatics,WadsworthCenter,
Albany,NewYork,UnitedStatesofAmerica
Abstract
Genome-wideassociationstudies(GWAS)oftenidentifydisease-associatedmutationsinintergenicandnon-codingregions
ofthegenome.Giventhehighpercentageofthehumangenomethatistranscribed,wepostulatethatforsomeobserved
associationsthediseasephenotypeiscausedbyastructuralrearrangementinaregulatoryregionoftheRNAtranscript.To
identify such mutations, we have performed a genome-wide analysis of all known disease-associated Single Nucleotide
Polymorphisms(SNPs)fromtheHumanGeneMutationDatabase(HGMD)thatmaptotheuntranslatedregions(UTRs)ofa
gene.Ratherthanusingminimumfreeenergyapproaches(e.g.mFold),weuseapartitionfunctioncalculationthattakes
intoconsiderationtheensembleofpossibleRNAconformationsforagivensequence.Weidentifiedinthehumangenome
disease-associatedSNPsthatsignificantlyaltertheglobalconformationoftheUTRtowhichtheymap.Forsixdisease-states
(Hyperferritinemia Cataract Syndrome, b-Thalassemia, Cartilage-Hair Hypoplasia, Retinoblastoma, Chronic Obstructive
PulmonaryDisease(COPD),andHypertension),weidentifiedmultipleSNPsinUTRsthatalterthemRNAstructuralensemble
oftheassociatedgenes.UsingaBoltzmannsamplingprocedureforsub-optimalRNAstructures,weareabletocharacterize
and visualize the nature of the conformational changes induced by the disease-associated mutations in the structural
ensemble. We observe in several cases (specifically the 59 UTRs of FTL and RB1) SNP–induced conformational changes
analogoustothoseobservedinbacterialregulatoryRiboswitcheswhenspecificligandsbind.WeproposethattheUTRand
SNPcombinationsweidentifyconstitutea‘‘RiboSNitch,’’thatisaregulatoryRNAinwhichaspecificSNPhasastructural
consequence that results in a disease phenotype. Our SNPfold algorithm can
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