An Adaptor Molecule Afadin Regulates Lymphangiogenesis by Modulating RhoA Activity in the Developing Mouse Embryo

Afadin is an intracellular binding partner of nectins, cell-cell adhesion molecules, and plays important roles in the formation of cell-cell junctions. Afadin-knockout mice show early embryonic lethality, therefore little is known about the function of afadin during organ development. In this study,...

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Bibliographic Details
Published in:PloS one 2013-06, Vol.8 (6), p.e68134-e68134
Main Authors: Majima, Takashi, Takeuchi, Keisuke, Sano, Keigo, Hirashima, Masanori, Zankov, Dimitar P, Tanaka-Okamoto, Miki, Ishizaki, Hiroyoshi, Miyoshi, Jun, Ogita, Hisakazu
Format: Article
Language:English
Subjects:
Actin
Activation
Angiogenesis
Animals
Biochemistry
Biology
Blood
Blood vessels
Cadherins
Cancer
Cardiovascular disease
Cell adhesion
Cell adhesion & migration
Cell Adhesion - physiology
Cell adhesion molecules
Cell junctions
Cell morphology
Cell Proliferation
Cells, Cultured
Cytology
Cytoskeleton
Defects
Edema
Elongation
Embryo, Mammalian - cytology
Embryo, Mammalian - metabolism
Embryonic Development
Embryos
Endothelial cells
Endothelium, Vascular - cytology
Endothelium, Vascular - metabolism
Humans
Intercellular Junctions - physiology
Kinases
Lethality
Lymphangiogenesis - physiology
Lymphatic system
Medicine
Mice
Mice, Knockout
Mice, Transgenic
Microfilament Proteins - physiology
Microvasculature
Molecular biology
Physiology
rhoA GTP-Binding Protein - metabolism
RhoA protein
Rodents
Science
Skin
Stem cells
Transgenic animals
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Summary:Afadin is an intracellular binding partner of nectins, cell-cell adhesion molecules, and plays important roles in the formation of cell-cell junctions. Afadin-knockout mice show early embryonic lethality, therefore little is known about the function of afadin during organ development. In this study, we generated mice lacking afadin expression in endothelial cells, and found that the majority of these mice were embryonically lethal as a result of severe subcutaneous edema. Defects in the lymphatic vessels of the skin were observed, although the morphology in the blood vessels was almost normal. Severe disruption of VE-cadherin-mediated cell-cell junctions occurred only in lymphatic endothelial cells, but not in blood endothelial cells. Knockout of afadin did not affect the differentiation and proliferation of lymphatic endothelial cells. Using in vitro assays with blood and lymphatic microvascular endothelial cells (BMVECs and LMVECs, respectively), knockdown of afadin caused elongated cell shapes and disruption of cell-cell junctions among LMVECs, but not BMVECs. In afadin-knockdown LMVECs, enhanced F-actin bundles at the cell periphery and reduced VE-cadherin immunostaining were found, and activation of RhoA was strongly increased compared with that in afadin-knockdown BMVECs. Conversely, inhibition of RhoA activation in afadin-knockdown LMVECs restored the cell morphology. These results indicate that afadin has different effects on blood and lymphatic endothelial cells by controlling the levels of RhoA activation, which may critically regulate the lymphangiogenesis of mouse embryos.
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0068134