PUBLICATION
Semaphorin3a1 regulates angioblast migration and vascular development in zebrafish embryos
- Authors
- Shoji, W., Isogai, S., Sato-Maeda, M., Obinata, M., and Kuwada, J.Y.
- ID
- ZDB-PUB-030707-2
- Date
- 2003
- Source
- Development (Cambridge, England) 130(14): 3227-3236 (Journal)
- Registered Authors
- Isogai, Sumio, Kuwada, John, Shoji, Wataru
- Keywords
- Cell migration, Semaphorin, Zebrafish, Angioblast, Neuropilin
- MeSH Terms
-
- Animals
- Animals, Genetically Modified
- Blotting, Western
- Cell Movement
- Green Fluorescent Proteins
- In Situ Hybridization
- Luminescent Proteins/metabolism
- Mesoderm/pathology
- Microscopy, Fluorescence
- Models, Biological
- Neovascularization, Physiologic*
- Neuropilins/metabolism
- Oligonucleotides, Antisense/metabolism
- Semaphorin-3A/metabolism*
- Semaphorin-3A/physiology*
- Zebrafish
- PubMed
- 12783793 Full text @ Development
Citation
Shoji, W., Isogai, S., Sato-Maeda, M., Obinata, M., and Kuwada, J.Y. (2003) Semaphorin3a1 regulates angioblast migration and vascular development in zebrafish embryos. Development (Cambridge, England). 130(14):3227-3236.
Abstract
Semaphorins are a large family of secreted and cell surface molecules that guide neural growth cones to their targets during development. Some semaphorins are expressed in cells and tissues beyond the nervous system suggesting the possibility that they function in the development of non-neural tissues as well. In the trunk of zebrafish embryos endothelial precursors (angioblasts) are located ventral and lateral to the somites. The angioblasts migrate medially and dorsally along the medial surface of the somites to form the dorsal aorta just ventral to the notochord. Here we show that in zebrafish Sema3a1 is involved in angioblast migration in vivo. Expression of sema3a1 in somites and neuropilin 1, which encodes for a component of the Sema3a receptor, in angioblasts suggested that Sema3a1 regulates the pathway of the dorsally migrating angioblasts. Antisense knockdown of Sema3a1 inhibited the formation of the dorsal aorta. Induced ubiquitous expression of sema3a1 in hsp70:gfpsema3a1myc transgenic embryos inhibited migration of angioblasts ventral and lateral to the somites and retarded development of the dorsal aorta, resulting in severely reduced blood circulation. Furthermore, analysis of cells that express angioblast markers following induced expression of sema3a1 or in a mutant that changes the expression of sema3a1 in the somites confirmed these results. These data implicate Sema3a1, a guidance factor for neural growth cones, in the development of the vascular system.
Genes / Markers
Expression
Phenotype
Mutations / Transgenics
Human Disease / Model
Sequence Targeting Reagents
Fish
Orthology
Engineered Foreign Genes
Mapping