An integrated expression atlas of miRNAs and their promoters in human and mouse.
Derek de RieImad AbugessaisaTanvir AlamErik ArnerPeter ArnerHaitham AshoorGaby ÅströmMagda BabinaNicolas BertinA Maxwell BurroughsAilsa J CarlisleCarsten O DaubMichael DetmarRuslan DeviatiiarovAlexandre FortClaudia GebhardDaniel GoldowitzSven GuhlThomas J HaJayson HarshbargerAkira HasegawaKosuke HashimotoMeenhard HerlynPeter HeutinkKelly J HitchensChung-Chau HonEdward HuangYuri IshizuChieko KaiTakeya KasukawaPeter KlinkenTimo LassmannCharles-Henri LecellierWeonju LeeMarina LizioVsevolod J MakeevAnthony MathelierYulia A MedvedevaNiklas MejhertChristopher J MungallShohei NomaMitsuhiro OhshimaMariko Okada-HatakeyamaHelena PerssonPatrizia RizzuFilip RoudnickyPål SaetromHiroki SatoJessica SeverinJay W ShinRolf K SwobodaHiroshi TaruiHiroo ToyodaKristoffer Vitting-SeerupLouise WinteringhamYoko YamaguchiKayoko YasuzawaMisako YonedaNoriko YumotoSusan ZabierowskiPeter G ZhangChristine A WellsKim M SummersHideya KawajiAlbin SandelinMichael Rehlinull nullYoshihide HayashizakiPiero CarniciAlistair R R ForrestMichiel J L de HoonPublished in: Nature biotechnology (2017)
MicroRNAs (miRNAs) are short non-coding RNAs with key roles in cellular regulation. As part of the fifth edition of the Functional Annotation of Mammalian Genome (FANTOM5) project, we created an integrated expression atlas of miRNAs and their promoters by deep-sequencing 492 short RNA (sRNA) libraries, with matching Cap Analysis Gene Expression (CAGE) data, from 396 human and 47 mouse RNA samples. Promoters were identified for 1,357 human and 804 mouse miRNAs and showed strong sequence conservation between species. We also found that primary and mature miRNA expression levels were correlated, allowing us to use the primary miRNA measurements as a proxy for mature miRNA levels in a total of 1,829 human and 1,029 mouse CAGE libraries. We thus provide a broad atlas of miRNA expression and promoters in primary mammalian cells, establishing a foundation for detailed analysis of miRNA expression patterns and transcriptional control regions.