Dynamic changes in the epigenomic landscape regulate human organogenesis and link to developmental disorders

Author:

Gerrard Dave T.ORCID,Berry Andrew A.,Jennings Rachel E.,Birket Matthew J.ORCID,Zarrineh Peyman,Garstang Myles G.,Withey Sarah L.,Short PatrickORCID,Jiménez-Gancedo Sandra,Firbas Panos N.,Donaldson IanORCID,Sharrocks Andrew D.,Hanley Karen PiperORCID,Hurles Matthew E.,Gomez-Skarmeta José Luis,Bobola Nicoletta,Hanley Neil A.ORCID

Abstract

AbstractHow the genome activates or silences transcriptional programmes governs organ formation. Little is known in human embryos undermining our ability to benchmark the fidelity of stem cell differentiation or cell programming, or interpret the pathogenicity of noncoding variation. Here, we study histone modifications across thirteen tissues during human organogenesis. We integrate the data with transcription to build an overview of how the human genome differentially regulates alternative organ fates including by repression. Promoters from nearly 20,000 genes partition into discrete states. Key developmental gene sets are actively repressed outside of the appropriate organ without obvious bivalency. Candidate enhancers, functional in zebrafish, allow imputation of tissue-specific and shared patterns of transcription factor binding. Overlaying more than 700 noncoding mutations from patients with developmental disorders allows correlation to unanticipated target genes. Taken together, the data provide a comprehensive genomic framework for investigating normal and abnormal human development.

Funder

RCUK | Medical Research Council

Academy of Medical Sciences

Wellcome Trust

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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