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

机译:具有细胞外表皮生长因子同源域的新型内皮细胞表面受体酪氨酸激酶。

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摘要

Endothelial cell surfaces play key roles in several important physiological and pathological processes such as blood clotting, angiogenic responses, and inflammation. Here we describe the cloning and characterization of tie, a novel type of human endothelial cell surface receptor tyrosine kinase. The extracellular domain of the predicted tie protein product has an exceptional multidomain structure consisting of a cluster of three epidermal growth factor homology motifs embedded between two immunoglobulinlike loops, which are followed by three fibronectin type III repeats next to the transmembrane region. Additionally, a cDNA form lacking the first of the three epidermal growth factor homology domains was isolated, suggesting that alternative splicing creates different tie-type receptors. Cells transfected with tie cDNA expression vector produce glycosylated polypeptides of 117 kDa which are reactive to antisera raised against the tie carboxy terminus. The tie gene was located in chromosomal region 1p33 to 1p34. Expression of the tie gene appeared to be restricted in some cell lines; large amounts of tie mRNA were detected in endothelial cell lines and in some myeloid leukemia cell lines with erythroid and megakaryoblastoid characteristics. In addition, mRNA in situ studies further indicated the endothelial expression of the tie gene. The tie receptor tyrosine kinase may have evolved for multiple protein-protein interactions, possibly including cell adhesion to the vascular endothelium.
机译:内皮细胞表面在血液凝结,血管生成反应和炎症等几个重要的生理和病理过程中起着关键作用。在这里我们描述领带的克隆和表征,领带是一种新型的人类内皮细胞表面受体酪氨酸激酶。预测的结合蛋白产物的细胞外结构域具有特殊的多结构域结构,该结构由在两个免疫球蛋白样环之间嵌入的三个表皮生长因子同源性基序簇组成,随后是跨膜区附近的三个III型纤连蛋白重复序列​​。此外,分离出缺少三个表皮生长因子同源结构域中的第一个的cDNA形式,这表明选择性剪接产生了不同的领带型受体。用tie cDNA表达载体转染的细胞产生117 kDa的糖基化多肽,这些多肽与针对tie羧基末端的抗血清具有反应性。 tie基因位于染色体区域1p33至1p34。 tie基因的表达似乎在某些细胞系中受到限制。在内皮细胞系和某些具有类红细胞和巨核母细胞样特征的髓样白血病细胞系中检测到大量的tie mRNA。此外,mRNA原位研究进一步表明了tie基因的内皮表达。领带受体酪氨酸激酶可能已经进化为多种蛋白质-蛋白质相互作用,可能包括细胞对血管内皮的粘附。

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