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Growth-limiting role of endothelial cells in endoderm development
Authors:Sand Fredrik Wolfhagen  Hörnblad Andreas  Johansson Jenny K  Lorén Christina  Edsbagge Josefina  Ståhlberg Anders  Magenheim Judith  Ilovich Ohad  Mishani Eyal  Dor Yuval  Ahlgren Ulf  Semb Henrik
Affiliation:aStem Cell and Pancreas Developmental Biology, Stem Cell Center, Department of Laboratory Medicine, Lund, Lund University, BMC B10, Klinikgatan 26, SE-221 84 Lund, Sweden;bUmeå Centre for Molecular Medicine, Umeå University, SE-901 87 Umeå, Sweden;cCellartis AB, Arvid Wallgrens Backe 20, SE-413 46 Göteborg, Sweden;dDepartment of Developmental Biology and Cancer Research, The Institute for Medical Research Israel–Canada, The Hebrew University-Hadassah Medical School, Jerusalem 91120, Israel;eDepartment of Nuclear Medicine, Cyclotron Unit, Hadassah Hebrew University Hospital, Jerusalem, Israel
Abstract:Endoderm development is dependent on inductive signals from different structures in close vicinity, including the notochord, lateral plate mesoderm and endothelial cells. Recently, we demonstrated that a functional vascular system is necessary for proper pancreas development, and that sphingosine-1-phosphate (S1P) exhibits the traits of a blood vessel-derived molecule involved in early pancreas morphogenesis. To examine whether S1P1-signaling plays a more general role in endoderm development, S1P1-deficient mice were analyzed. S1P1 ablation results in compromised growth of several foregut-derived organs, including the stomach, dorsal and ventral pancreas and liver. Within the developing pancreas the reduction in organ size was due to deficient proliferation of Pdx1+ pancreatic progenitors, whereas endocrine cell differentiation was unaffected. Ablation of endothelial cells in vitro did not mimic the S1P1 phenotype, instead, increased organ size and hyperbranching were observed. Consistent with a negative role for endothelial cells in endoderm organ expansion, excessive vasculature was discovered in S1P1-deficient embryos. Altogether, our results show that endothelial cell hyperplasia negatively influences organ development in several foregut-derived organs.
Keywords:Pancreas   Endoderm   Morphogenesis   Blood vessel   Mesenchyme   Sphingosine-1-phosphate 1 receptor
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