Growth-limiting role of endothelial cells in endoderm development

Fredrik Wolfhagen Sand; Andreas Hörnblad; Jenny K. Johansson; Christina Lorén; Josefina Edsbagge; Anders Ståhlberg; Judith Magenheim; Ohad Ilovich; Eyal Mishani; Yuval Dor; Ulf Ahlgren; Henrik Semb

doi:10.1016/j.ydbio.2011.01.026

Growth-limiting role of endothelial cells in endoderm development

Fredrik Wolfhagen Sand, Andreas Hörnblad, Jenny K. Johansson, Christina Lorén, Josefina Edsbagge, Anders Ståhlberg, Judith Magenheim, Ohad Ilovich, Eyal Mishani, Yuval Dor, Ulf Ahlgren, Henrik Semb

Department of Developmental Biology and Cancer Research

The Hebrew University of Jerusalem

Research output: Contribution to journal › Article › peer-review

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.

Original language	English
Pages (from-to)	267-277
Number of pages	11
Journal	Developmental Biology
Volume	352
Issue number	2
DOIs	https://doi.org/10.1016/j.ydbio.2011.01.026
State	Published - 15 Apr 2011

Keywords

Blood vessel
Endoderm
Mesenchyme
Morphogenesis
Pancreas
Sphingosine-1-phosphate 1 receptor

All Science Journal Classification (ASJC) codes

Molecular Biology
Developmental Biology
Cell Biology

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10.1016/j.ydbio.2011.01.026

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@article{9e6394b782c341999782551fa4808b88,

title = "Growth-limiting role of endothelial cells in endoderm development",

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 = "Blood vessel, Endoderm, Mesenchyme, Morphogenesis, Pancreas, Sphingosine-1-phosphate 1 receptor",

author = "Sand, \{Fredrik Wolfhagen\} and Andreas H{\"o}rnblad and Johansson, \{Jenny K.\} and Christina Lor{\'e}n and Josefina Edsbagge and Anders St{\aa}hlberg and Judith Magenheim and Ohad Ilovich and Eyal Mishani and Yuval Dor and Ulf Ahlgren and Henrik Semb",

note = "Funding Information: We thank Dr. R. Proia for providing the S1P 1 deficient mouse line and for valuable comments on the manuscript, Dr. K. Gaengel and Dr. C. Betsholtz for constructive discussions and for sharing unpublished data, Dr. C. Wright and BCBC for providing antibodies, Dr. I. Artner for valuable comments on the manuscript, M. Magnusson and C. Ekenstierna for mouse breeding. This work was supported by the Swedish Research Council , Stem Cell Center , Lund University , Swedish Foundation for Strategic Research , NIH Beta Cell Biology Consortium , Juvenile Diabetes Research Foundation , and in part by the Intramural Research Program of the National Institutes of Health, National Institute of Diabetes and Digestive and Kidney Diseases , The Kempe Foundations , The Swedish Medical Research Council and Ume{\aa} University Biotech Grants.",

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T1 - Growth-limiting role of endothelial cells in endoderm development

AU - Sand, Fredrik Wolfhagen

AU - Hörnblad, Andreas

AU - Johansson, Jenny K.

AU - Lorén, Christina

AU - Edsbagge, Josefina

AU - Ståhlberg, Anders

AU - Magenheim, Judith

AU - Ilovich, Ohad

AU - Mishani, Eyal

AU - Dor, Yuval

AU - Ahlgren, Ulf

AU - Semb, Henrik

N1 - Funding Information: We thank Dr. R. Proia for providing the S1P 1 deficient mouse line and for valuable comments on the manuscript, Dr. K. Gaengel and Dr. C. Betsholtz for constructive discussions and for sharing unpublished data, Dr. C. Wright and BCBC for providing antibodies, Dr. I. Artner for valuable comments on the manuscript, M. Magnusson and C. Ekenstierna for mouse breeding. This work was supported by the Swedish Research Council , Stem Cell Center , Lund University , Swedish Foundation for Strategic Research , NIH Beta Cell Biology Consortium , Juvenile Diabetes Research Foundation , and in part by the Intramural Research Program of the National Institutes of Health, National Institute of Diabetes and Digestive and Kidney Diseases , The Kempe Foundations , The Swedish Medical Research Council and Umeå University Biotech Grants.

PY - 2011/4/15

Y1 - 2011/4/15

N2 - 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.

AB - 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.

KW - Blood vessel

KW - Endoderm

KW - Mesenchyme

KW - Morphogenesis

KW - Pancreas

KW - Sphingosine-1-phosphate 1 receptor

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U2 - 10.1016/j.ydbio.2011.01.026

DO - 10.1016/j.ydbio.2011.01.026

M3 - مقالة

SN - 0012-1606

VL - 352

SP - 267

EP - 277

JO - Developmental Biology

JF - Developmental Biology

IS - 2

ER -

Growth-limiting role of endothelial cells in endoderm development

Abstract

Keywords

All Science Journal Classification (ASJC) codes

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