| Literature DB >> 28009287 |
Shilu Amin1, Roel Neijts1, Salvatore Simmini1, Carina van Rooijen1, Sander C Tan1, Lennart Kester1, Alexander van Oudenaarden1, Menno P Creyghton1, Jacqueline Deschamps2.
Abstract
In vertebrate embryos, anterior tissues are generated early, followed by the other axial structures that emerge sequentially from a posterior growth zone. The genetic network driving posterior axial elongation in mice, and its disturbance in mutants with posterior truncation, is not yet fully understood. Here, we show that the combined expression of Cdx2 and T Brachyury is essential to establish the core signature of posterior axial progenitors. Cdx2 and T Brachyury are required for extension of a similar trunk portion of the axis. Simultaneous loss of function of these two genes disrupts axial elongation to a much greater extent than each single mutation alone. We identify and validate common targets for Cdx2 and T Brachyury in vivo, including Wnt and Fgf pathway components active in the axial progenitor niche. Our data demonstrate that integration of the Cdx/Hox and T Brachyury transcriptional networks controls differential axial growth during vertebrate trunk elongation.Entities:
Keywords: axial progenitors; elongation of the anteroposterior axis; genetics of posterior tissue generation; mouse embryonic development; regulatory elements
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Year: 2016 PMID: 28009287 DOI: 10.1016/j.celrep.2016.11.069
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423