TGF beta in murine morphogenetic processes: the early embryo and cardiogenesis
pmid: 1696875
TGF beta in murine morphogenetic processes: the early embryo and cardiogenesis
Abstract The tissue distribution of TGF beta-1 RNA was examined within whole mouse embryos from implantation to 10.5 days gestational age and, in the developing heart, up to 8 days postpartum. The earliest high level expression of TGF beta-1 RNA is at 7.0 days postcoUum ip.c.) in the cardiac mesoderm. At 8.0 days gestational age, cardiac TGF beta-1 RNA expression is limited to endocardia! cells. By 9.5 days p.c, this expression pattern becomes regionalised to those cells that overlie cardiac cushion tissue. High TGF beta-1 RNA levels continue to persist in endothelial cells of the heart valves until approximately one week postpartum. The TGF beta-1 RNA distribution was compared with the extracellular distributions of polypeptides for TGF beta and Jl/tenascin. As previously reported, endothelial expression of TGF beta-1 RNA is correlated with mesenchymal expression of TGF beta polypeptide, suggesting a paracrine mode of action for this growth factor in cardiac development. Minor discrepancies in the distributions of TGF beta-1 RNA and the extracellular form of the TGF beta polypeptide suggest that translational or post-translational control of protein levels occurs and/or the possibility that the antibody used may also recognise other members of the TGF beta polypeptide family. A correlation between endothelial TGF beta-1 expression and distribution of Jl/tenascin in the mesenchyme gives further support to the proposition that the biological effects of TGF beta-1 may, in part, be mediated by Jl/tenascin.
- University of Glasgow United Kingdom
Male, Neovascularization, Pathologic, Cell Adhesion Molecules, Neuronal, Myocardium, Heart, Tenascin, Gastrula, Heart Valves, Mice, Transforming Growth Factors, Cell Adhesion, Morphogenesis, Animals, Female, RNA, Messenger, DNA Probes
Male, Neovascularization, Pathologic, Cell Adhesion Molecules, Neuronal, Myocardium, Heart, Tenascin, Gastrula, Heart Valves, Mice, Transforming Growth Factors, Cell Adhesion, Morphogenesis, Animals, Female, RNA, Messenger, DNA Probes
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