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Characterization of the Extracellular Domain in Vascular Endothelial Growth Factor Receptor‐1 (Flt‐1 Tyrosine Kinase)

机译:血管内皮生长因子受体1(Flt-1酪氨酸激酶)胞外域的表征。

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摘要

Flt‐1 tyrosine kinase, vascular endothelial growth factor (VEGF) receptor‐1, binds VEGF and a new VEGF‐related ligand, placenta growth factor, but KDR/Flk‐1 (VEGF receptor‐2) binds only VEGF. To characterize the functional regions in the Flt‐1 extracellular domain such as the ligand binding region and the dimer formation of the receptor, we constructed a series of mutants of the Flt‐1 extracellular domain as soluble forms in a baculovirus system. We found that a region carrying the N‐terminal 1st to 3rd immunoglobulin (Ig)‐like domains of Flt‐1 binds both ligands with high affinity. However, for dimer formation of soluble Flt‐1, a region further downstream in the Flt‐1 extracellular domain was required. Mutant Flt‐1 receptors expressed in COS cells confirmed the requirement of the 4th to 7th Ig region for the activation of Flt‐1 tyrosine kinase. Soluble Flt‐1 carrying the N‐terminal 1st to 3rd Ig region suppressed VEGF‐dependent endothelial proliferation in vitro to the same level as the larger forms of soluble Flt‐1, suggesting that the binding of one soluble Flt‐1 molecule to one subunit of the VEGF homodimer may be sufficient to block the VEGF activity.
机译:Flt-1酪氨酸激酶,血管内皮生长因子(VEGF)受体-1,结合VEGF和新的VEGF相关配体,胎盘生长因子,但KDR / Flk-1(VEGF受体-2)仅结合VEGF。为了表征Flt-1细胞外结构域中的功能区域,例如配体结合区和受体的二聚体形成,我们构建了一系列Flt-1细胞外结构域突变体,作为杆状病毒系统中的可溶形式。我们发现带有Flt-1的N端第1至第3免疫球蛋白(Ig)样结构域的区域可以高亲和力结合两个配体。但是,为了形成可溶性Flt-1的二聚体,需要在Flt-1细胞外域的更下游区域。 COS细胞中表达的突变Flt-1受体证实了激活Flt-1酪氨酸激酶需要4至7 Ig区。带有N端第1至第3 Ig区域的可溶性Flt-1在体外抑制VEGF依赖性内皮细胞的增殖,与较大形式的可溶性Flt-1抑制水平相同,这表明一个可溶性Flt-1分子与一个亚基结合VEGF同二聚体的“α”可能足以阻断VEGF的活性。

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