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Human Cerberus Prevents Nodal-Receptor Binding Inhibits Nodal Signaling and Suppresses Nodal-Mediated Phenotypes

机译:人类地狱鼠防止结节受体结合抑制结节信号并抑制结节介导的表型。

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摘要

The Transforming Growth Factor-ß (TGFß) family ligand Nodal is an essential embryonic morphogen that is associated with progression of breast and other cancers. It has therefore been suggested that Nodal inhibitors could be used to treat breast cancers where Nodal plays a defined role. As secreted antagonists, such as Cerberus, tightly regulate Nodal signaling during embryonic development, we undertook to produce human Cerberus, characterize its biochemical activities, and determine its effect on human breast cancer cells. Using quantitative methods, we investigated the mechanism of Nodal signaling, we evaluated binding of human Cerberus to Nodal and other TGFß family ligands, and we characterized the mechanism of Nodal inhibition by Cerberus. Using cancer cell assays, we examined the ability of Cerberus to suppress aggressive breast cancer cell phenotypes. We found that human Cerberus binds Nodal with high affinity and specificity, blocks binding of Nodal to its signaling partners, and inhibits Nodal signaling. Moreover, we showed that Cerberus profoundly suppresses migration, invasion, and colony forming ability of Nodal expressing and Nodal supplemented breast cancer cells. Taken together, our studies provide mechanistic insights into Nodal signaling and Nodal inhibition with Cerberus and highlight the potential value of Cerberus as anti-Nodal therapeutic.
机译:转化生长因子-β(TGFβ)家族配体Nodal是一种必需的胚胎形态发生原,与乳腺癌和其他癌症的进展有关。因此,已经提出,可以将Nodal抑制剂用于治疗Nodal发挥明确作用的乳腺癌。由于分泌的拮抗剂(例如Cerberus)在胚胎发育过程中严格调节Nodal信号传导,因此我们承诺生产人Cerberus,表征其生化活性,并确定其对人乳腺癌细胞的作用。使用定量方法,我们研究了Nodal信号传导的机制,评估了人类Cerberus与Nodal和其他TGFβ家族配体的结合,并表征了Cerberus抑制Nodal的机制。使用癌细胞分析,我们检查了地狱犬抑制侵袭性乳腺癌细胞表型的能力。我们发现人类地狱犬以高亲和力和特异性结合Nodal,阻断Nodal与其信号伴侣的结合,并抑制Nodal信号。此外,我们表明,地狱犬能够深刻抑制表达Nodal和补充Nodal的乳腺癌细胞的迁移,侵袭和集落形成能力。综上所述,我们的研究提供了有关Cerberus的节点信号传导和节点抑制作用的机械学见解,并突出了Cerberus作为抗节点治疗剂的潜在价值。

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