| Literature DB >> 30554961 |
Stefan Frank1, Gaurav Ahuja1, Deniz Bartsch1, Nicole Russ1, Wenjie Yao1, Joseph Chao-Chung Kuo2, Jens-Peter Derks1, Vijay Suresh Akhade3, Yulia Kargapolova4, Theodore Georgomanolis4, Jan-Erik Messling1, Marie Gramm1, Lilija Brant4, Rizwan Rehimi5, Natalia Emilse Vargas1, Alina Kuroczik1, Tsun-Po Yang6, Raja Ghazanfar Ali Sahito7, Julia Franzen8, Juergen Hescheler7, Agapios Sachinidis7, Martin Peifer6, Alvaro Rada-Iglesias5, Meena Kanduri9, Ivan G Costa2, Chandrasekhar Kanduri3, Argyris Papantonis4, Leo Kurian10.
Abstract
Human protein-coding genes are often accompanied by divergently transcribed non-coding RNAs whose functions, especially in cell fate decisions, are poorly understood. Using an hESC-based cardiac differentiation model, we define a class of divergent lncRNAs, termed yin yang lncRNAs (yylncRNAs), that mirror the cell-type-specific expression pattern of their protein-coding counterparts. yylncRNAs are preferentially encoded from the genomic loci of key developmental cell fate regulators. Most yylncRNAs are spliced polyadenylated transcripts showing comparable expression patterns in vivo in mouse and in human embryos. Signifying their developmental function, the key mesoderm specifier BRACHYURY (T) is accompanied by yylncT, which localizes to the active T locus during mesoderm commitment. yylncT binds the de novo DNA methyltransferase DNMT3B, and its transcript is required for activation of the T locus, with yylncT depletion specifically abolishing mesodermal commitment. Collectively, we report a lncRNA-mediated regulatory layer safeguarding embryonic cell fate transitions.Entities:
Keywords: Brachyury; DNMT3B; cardiac development; cell-fate decision; cellular identity; divergent lncRNAs; embryonic development; lncRNA; mesoderm; regulation of DNA methylation
Mesh:
Substances:
Year: 2018 PMID: 30554961 DOI: 10.1016/j.stem.2018.11.005
Source DB: PubMed Journal: Cell Stem Cell ISSN: 1875-9777 Impact factor: 24.633