Genome-wide characterization of the routes to pluripotency | Zendy

Samer M.I. Hussein | Zendy; Mira C. Puri | Zendy; Peter D. Tonge | Zendy; Marco Benevento | Zendy; Andrew J. Corso | Zendy; Jennifer L. Clancy | Zendy; Rowland Mosbergen | Zendy; Mira Li | Zendy; Dong Sung Lee | Zendy; Nicole Cloonan | Zendy; David Wood | Zendy; Javier Muñoz | Zendy; Robert Middleton | Zendy; Othmar Korn | Zendy; Hardip R. Patel | Zendy; Carl A. White | Zendy; Jong Yeon Shin | Zendy; Marie Gauthier | Zendy; Kim Anh Lê Cao | Zendy; JongIl Kim | Zendy; Jessica C. Mar | Zendy; Nika Shakiba | Zendy; William Ritchie | Zendy; John E.J. Rasko | Zendy; Sean M. Grimmond | Zendy; Peter W. Zandstra | Zendy; Christine A. Wells | Zendy; Thomas Preiß | Zendy; Jeong Sun Seo | Zendy; Albert J. R. Heck | Zendy; Ian Rogers | Zendy; András Nagy | Zendy

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Genome-wide characterization of the routes to pluripotency

Author(s) -

Samer M.I. Hussein,

Mira C. Puri,

Peter D. Tonge,

Marco Benevento,

Andrew J. Corso,

Jennifer L. Clancy,

Rowland Mosbergen,

Mira Li,

Dong Sung Lee,

Nicole Cloonan,

David Wood,

Javier Muñoz,

Robert Middleton,

Othmar Korn,

Hardip R. Patel,

Carl A. White,

Jong Yeon Shin,

Marie Gauthier,

Kim Anh Lê Cao,

JongIl Kim,

Jessica C. Mar,

Nika Shakiba,

William Ritchie,

John E.J. Rasko,

Sean M. Grimmond,

Peter W. Zandstra,

Christine A. Wells,

Thomas Preiß,

Jeong Sun Seo,

Albert J. R. Heck,

Ian Rogers,

András Nagy

Publication year - 2014

Publication title -

nature

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 15.993

H-Index - 1226

eISSN - 1476-4687

pISSN - 0028-0836

DOI - 10.1038/nature14046

Subject(s) - reprogramming , induced pluripotent stem cell , chromatin , biology , epigenomics , embryonic stem cell , epigenetics , somatic cell , dna methylation , histone , microbiology and biotechnology , genetics , computational biology , gene , gene expression

Somatic cell reprogramming to a pluripotent state continues to challenge many of our assumptions about cellular specification, and despite major efforts, we lack a complete molecular characterization of the reprograming process. To address this gap in knowledge, we generated extensive transcriptomic, epigenomic and proteomic data sets describing the reprogramming routes leading from mouse embryonic fibroblasts to induced pluripotency. Through integrative analysis, we reveal that cells transition through distinct gene expression and epigenetic signatures and bifurcate towards reprogramming transgene-dependent and -independent stable pluripotent states. Early transcriptional events, driven by high levels of reprogramming transcription factor expression, are associated with widespread loss of histone H3 lysine 27 (H3K27me3) trimethylation, representing a general opening of the chromatin state. Maintenance of high transgene levels leads to re-acquisition of H3K27me3 and a stable pluripotent state that is alternative to the embryonic stem cell (ESC)-like fate. Lowering transgene levels at an intermediate phase, however, guides the process to the acquisition of ESC-like chromatin and DNA methylation signature. Our data provide a comprehensive molecular description of the reprogramming routes and is accessible through the Project Grandiose portal at http://www.stemformatics.org.

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