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Publication : Ezh2 restricts the smooth muscle lineage during mouse lung mesothelial development.

First Author  Snitow M Year  2016
Journal  Development Volume  143
Issue  20 Pages  3733-3741
PubMed ID  27578795 Mgi Jnum  J:240484
Mgi Id  MGI:5883662 Doi  10.1242/dev.134932
Citation  Snitow M, et al. (2016) Ezh2 restricts the smooth muscle lineage during mouse lung mesothelial development. Development 143(20):3733-3741
abstractText  During development, the lung mesoderm generates a variety of cell lineages, including airway and vascular smooth muscle. Epigenetic changes in adult lung mesodermal lineages are thought to contribute towards diseases such as idiopathic pulmonary fibrosis and chronic obstructive pulmonary disease, although the factors that regulate early lung mesoderm development are unknown. We show in mouse that the PRC2 component Ezh2 is required to restrict smooth muscle differentiation in the developing lung mesothelium. Mesodermal loss of Ezh2 leads to the formation of ectopic smooth muscle in the submesothelial region of the developing lung mesoderm. Loss of Ezh2 specifically in the developing mesothelium reveals a mesothelial cell-autonomous role for Ezh2 in repression of the smooth muscle differentiation program. Loss of Ezh2 derepresses expression of myocardin and Tbx18, which are important regulators of smooth muscle differentiation from the mesothelium and related cell lineages. Together, these findings uncover an Ezh2-dependent mechanism to restrict the smooth muscle gene expression program in the developing mesothelium and allow appropriate cell fate decisions to occur in this multipotent mesoderm lineage.
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