1. Universidade do Minho
  2. Escola de Medicina | School of Medicine
  3. Instituto de Investigação em Ciências da Vida e da Saúde
  4. ICVS - Artigos em revistas internacionais / Papers in international journals
Utilize este identificador para referenciar este registo: https://hdl.handle.net/1822/57785

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Campo DCValorIdioma
dc.contributor.authorBarbosa, Mafaldapor
dc.contributor.authorJoshi, Ricky S.por
dc.contributor.authorGarg, Paraspor
dc.contributor.authorMartin-Trujillo, Alejandropor
dc.contributor.authorPatel, Nihirpor
dc.contributor.authorJadhav, Bharatipor
dc.contributor.authorWatson, Corey T.por
dc.contributor.authorGibson, Williampor
dc.contributor.authorChetnik, Kelseypor
dc.contributor.authorTessereau, Chloepor
dc.contributor.authorMei, Huipor
dc.contributor.authorDe Rubeis, Silviapor
dc.contributor.authorReichert, Jenniferpor
dc.contributor.authorLopes, Fátima Daniela Teixeirapor
dc.contributor.authorVissers, Lisenka E. L. M.por
dc.contributor.authorKleefstra, Tjitskepor
dc.contributor.authorGrice, Dorothy E.por
dc.contributor.authorEdelmann, Lisapor
dc.contributor.authorSoares, Gabrielapor
dc.contributor.authorMaciel, P.por
dc.contributor.authorBrunner, Han G.por
dc.contributor.authorBuxbaum, Joseph D.por
dc.contributor.authorGelb, Bruce D.por
dc.contributor.authorSharp, Andrew J.por
dc.date.accessioned2019-01-04T09:45:47Z-
dc.date.available2019-01-04T09:45:47Z-
dc.date.issued2018-
dc.identifier.issn2041-1723por
dc.identifier.urihttps://hdl.handle.net/1822/57785-
dc.description.abstractCertain human traits such as neurodevelopmental disorders (NDs) and congenital anomalies (CAs) are believed to be primarily genetic in origin. However, even after whole-genome sequencing (WGS), a substantial fraction of such disorders remain unexplained. We hypothesize that some cases of ND-CA are caused by aberrant DNA methylation leading to dysregulated genome function. Comparing DNA methylation profiles from 489 individuals with ND-CAs against 1534 controls, we identify epivariations as a frequent occurrence in the human genome. De novo epivariations are significantly enriched in cases, while RNAseq analysis shows that epivariations often have an impact on gene expression comparable to loss-of-function mutations. Additionally, we detect and replicate an enrichment of rare sequence mutations overlapping CTCF binding sites close to epivariations, providing a rationale for interpreting non-coding variation. We propose that epivariations contribute to the pathogenesis of some patients with unexplained ND-CAs, and as such likely have diagnostic relevance.por
dc.description.sponsorshipThe authors are grateful to the patients and families who participated in this study and to the collaborators who supported patient recruitment. This work was supported by NIH grant HG006696 and research grant 6-FY13-92 from the March of Dimes to A.J.S., grant HL098123 to B.D.G. and A.J.S., Gulbenkian Programme for Advanced Medical Education and the Portuguese Foundation for Science and Technology (SFRH/BDINT/51549/ 2011, PIC/IC/83026/2007, PIC/IC/83013/2007, SFRH/BD/90167/2012, Portugal) to P.M., F.L., and M.B., by the Northern Portugal Regional Operational Programme (NORTE 2020), under the Portugal 2020 Partnership Agreement, through the European Regional Development Fund (FEDER) (NORTE-01-0145-FEDER-000013) to P.M., a Beatriu de Pinos Postdoctoral Fellowship to R.S.J. (2011BP-A00515), and a Seaver Foundation fellowship to S.D.R. The views expressed are those of the authors and do not necessarily reflect those of the National Heart, Lung, and Blood Institute or the National Institutes of Health. Research reported in this paper was supported by the Office of Research Infrastructure of the National Institutes of Health under award number S10OD018522. This work was supported in part through the computational resources and staff expertise provided by Scientific Computing at the Icahn School of Medicine at Mount Sinai.por
dc.description.sponsorshipThe authors are grateful to the patients and families who participated in this study and to the collaborators who supported patient recruitment. This work was supported by NIH grant HG006696 and research grant 6-FY13-92 from the March of Dimes to A.J.S., grant HL098123 to B.D.G. and A.J.S., Gulbenkian Programme for Advanced Medical Education and the Portuguese Foundation for Science and Technology (SFRH/BDINT/51549/ 2011, PIC/IC/83026/2007, PIC/IC/83013/2007, SFRH/BD/90167/2012, Portugal) to P.M., F.L., and M.B., by the Northern Portugal Regional Operational Programme (NORTE 2020), under the Portugal 2020 Partnership Agreement, through the European Regional Development Fund (FEDER) (NORTE-01-0145-FEDER-000013) to P.M., a Beatriu de Pinos Postdoctoral Fellowship to R.S.J. (2011BP-A00515), and a Seaver Foundation fellowship to S.D.R. The views expressed are those of the authors and do not necessarily reflect those of the National Heart, Lung, and Blood Institute or the National Institutes of Health. Research reported in this paper was supported by the Office of Research Infrastructure of the National Institutes of Health under award number S10OD018522. This work was supported in part through the computational resources and staff expertise provided by Scientific Computing at the Icahn School of Medicine at Mount Sinai.-
dc.language.isoengpor
dc.publisherNature Research-
dc.relationinfo:eu-repo/grantAgreement/FCT/SFRH/SFRH%2FBDINT%2F51549%2F2011/PT-
dc.relationPIC/IC/83026/2007-
dc.relationPIC/IC/83013/2007-
dc.relationinfo:eu-repo/grantAgreement/FCT/SFRH/SFRH%2FBD%2F90167%2F2012/PT-
dc.rightsopenAccesspor
dc.subjectAdolescentpor
dc.subjectAdultpor
dc.subjectCase-Control Studiespor
dc.subjectChildpor
dc.subjectChild, Preschoolpor
dc.subjectCohort Studiespor
dc.subjectCongenital Abnormalitiespor
dc.subjectDNA Methylationpor
dc.subjectDatasets as Topicpor
dc.subjectEpigenomicspor
dc.subjectGenome, Humanpor
dc.subjectHumanspor
dc.subjectInfantpor
dc.subjectInfant, Newbornpor
dc.subjectLoss of Function Mutationpor
dc.subjectMalepor
dc.subjectMiddle Agedpor
dc.subjectNeurodevelopmental Disorderspor
dc.subjectSequence Analysis, DNApor
dc.subjectSequence Analysis, RNApor
dc.subjectYoung Adultpor
dc.subjectEpigenesis, Geneticpor
dc.titleIdentification of rare de novo epigenetic variations in congenital disorderspor
dc.typearticlepor
dc.peerreviewedyespor
oaire.citationStartPage2064por
oaire.citationIssue1por
oaire.citationVolume9por
dc.identifier.doi10.1038/s41467-018-04540-xpor
dc.identifier.pmid29802345por
dc.subject.wosScience & Technologypor
sdum.journalNature Communicationspor
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