Loss of responsiveness to chemotactic factors by deletion of the C-terminal protein interaction site of angiomotin

doi:10.1242/jcs.00694

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First published online 5 August 2003
doi: 10.1242/jcs.00694

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Journal of Cell Science 116, 3803-3810 (2003)
doi: 10.1242/jcs.00694

Research Article

Loss of responsiveness to chemotactic factors by deletion of the C-terminal protein interaction site of angiomotin

Tetyana Levchenko, Karin Aase, Boris Troyanovsky, Anders Bratt and Lars Holmgren^*

Department of Oncology-Pathology, Cancer Center Karolinska Institutet, S-17176 Stockholm, Sweden

^* Author for correspondence (e-mail: lars.holmgren{at}cck.ki.se)

Accepted 29 May 2003

We have recently identified a novel protein, named angiomotin,by its ability to bind the angiogenesis inhibitor angiostatinin the yeast two-hybrid system. Angiomotin belongs to a familywith two other members, AmotL-1 and -2 characterized by coiled-coiland C-terminal PDZ binding domains. Here we show that the putativePDZ binding motif of angiomotin serves as a protein recognitionsite and that deletion of three amino acids in this site results in inhibition of chemotaxis. Furthermore, endothelial cellsexpressing mutant angiomotin failed to migrate and form tubesin an in vitro tube formation assay. To study the effect ofangiomotin on embryonic angiogenesis, we generated transgenicmice expressing wild-type angiomotin and the C-terminal deletionmutant driven by the endothelial cell-specific receptor tyrosine kinase (TIE) promoter. Expression of mutant angiomotin in endothelialcells inhibited migration into the neuroectoderm and intersomiticregions resulting in death at embryonic day 9.5. In contrast,mice expressing wild-type angiomotin developed normally andwere fertile. These results suggest that the putative PDZ bindingmotif of angiomotin plays a critical role in regulating theresponsiveness of endothelial cells to chemotactic cues.

Key words: Endothelium, Neovascularization, Migration, Plasminogen, Receptor

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