A novel endothelial cell surface receptor tyrosine kinase with extracellular epidermal growth factor homology domains.

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Mol Cell Biol. 1992 April; 12(4): 1698-1707

A novel endothelial cell surface receptor tyrosine kinase with extracellular epidermal growth factor homology domains.

J Partanen, E Armstrong, T P Mäkelä, J Korhonen, M Sandberg, R Renkonen, S Knuutila, K Huebner and K Alitalo

Department of Virology, University of Helsinki, Finland.

ABSTRACT

Endothelial cell surfaces play key roles in several importantphysiological and pathological processes such as blood clotting,angiogenic responses, and inflammation. Here we describe thecloning and characterization of tie, a novel type of human endothelialcell surface receptor tyrosine kinase. The extracellular domainof the predicted tie protein product has an exceptional multidomainstructure consisting of a cluster of three epidermal growthfactor homology motifs embedded between two immunoglobulinlikeloops, which are followed by three fibronectin type III repeatsnext to the transmembrane region. Additionally, a cDNA formlacking the first of the three epidermal growth factor homologydomains was isolated, suggesting that alternative splicing createsdifferent tie-type receptors. Cells transfected with tie cDNAexpression vector produce glycosylated polypeptides of 117 kDawhich are reactive to antisera raised against the tie carboxyterminus. The tie gene was located in chromosomal region 1p33to 1p34. Expression of the tie gene appeared to be restrictedin some cell lines; large amounts of tie mRNA were detectedin endothelial cell lines and in some myeloid leukemia celllines with erythroid and megakaryoblastoid characteristics.In addition, mRNA in situ studies further indicated the endothelialexpression of the tie gene. The tie receptor tyrosine kinasemay have evolved for multiple protein-protein interactions,possibly including cell adhesion to the vascular endothelium.

Mol Cell Biol. 1992 April; 12(4): 1698-1707

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