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Soluble monomeric EphrinA1 is released from tumor cells and is a functional ligand for the EphA2 receptor

机译:可溶性单体EphrinA1从肿瘤细胞释放出来,是EphA2受体的功能性配体

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The ephrinA1 ligand exerts antioncogenic effects in tumor cells through activation and downregulation of the EphA2 receptor and has been described as a membrane-anchored protein requiring clustering for function. However, while investigating the ephrinA1/EphA2 system in the pathobiology of glioblastoma multiforme (GBM), we uncovered that ephrinA1 is released from GBM and breast adenocarcinoma cells as a soluble, monomeric protein and is a functional form of the ligand in this state. Conditioned media containing a soluble monomer of ephrinA1 caused EphA2 internalization and downregulation, dramatic alteration of cell morphology and suppression of the Ras–MAPK pathway. Moreover, soluble monomeric ephrinA1 was functional in a physiological context, eliciting collapse of embryonic neuronal growth cones. We also found that ephrinA1 is cleaved from the plasma membrane of GBM cells, an event which involves the action of a metalloprotease. Thus, the ephrinA1 ligand can, indeed, function as a soluble monomer and may act in a paracrine manner on the EphA2 receptor without the need for juxtacrine interactions. These findings have important implications for further deciphering the function of these proteins in pathology and physiology, as well as for the design of ephrinA1-based EphA2-targeted antitumor therapeutics.
机译:ephrinA1配体通过激活和下调EphA2受体在肿瘤细胞中发挥抗癌作用,已被描述为需要功能聚集的膜锚定蛋白。但是,在研究多形性胶质母细胞瘤(GBM)病理生物学中的ephrinA1 / EphA2系统时,我们发现ephrinA1作为可溶单体蛋白从GBM和乳腺腺癌细胞中释放出来,并且在此状态下是配体的功能形式。含有ephrinA1可溶性单体的条件培养基会引起EphA2内在化和下调,细胞形态发生显着变化,并抑制Ras-MAPK通路。此外,可溶性单体ephrinA1在生理环境中起作用,引起胚胎神经元生长锥的崩溃。我们还发现,ephrinA1从GBM细胞的质膜上裂解,这一事件涉及金属蛋白酶的作用。因此,ephrinA1配体确实可以充当可溶性单体,并可以旁分泌的方式作用于EphA2受体,而无需邻分泌相互作用。这些发现对于进一步破译这些蛋白质在病理学和生理学中的功能,以及对基于以ephrinA1为基础的EphA2的抗肿瘤治疗药物的设计具有重要意义。

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