首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Targeting IL-17B–IL-17RB signaling with an anti–IL-17RB antibody blocks pancreatic cancer metastasis by silencing multiple chemokines
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Targeting IL-17B–IL-17RB signaling with an anti–IL-17RB antibody blocks pancreatic cancer metastasis by silencing multiple chemokines

机译:用抗IL-17RB抗体靶向IL-17B–IL-17RB信号传导可通过沉默多种趋化因子来阻断胰腺癌转移

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摘要

Pancreatic cancer has an extremely high mortality rate due to its aggressive metastatic nature. Resolving the underlying mechanisms will be crucial for treatment. Here, we found that overexpression of IL-17B receptor (IL-17RB) strongly correlated with postoperative metastasis and inversely correlated with progression-free survival in pancreatic cancer patients. Consistently, results from ex vivo experiments further validated that IL-17RB and its ligand, IL-17B, plays an essential role in pancreatic cancer metastasis and malignancy. Signals from IL-17B–IL-17RB activated CCL20/CXCL1/IL-8/TFF1 chemokine expressions via the ERK1/2 pathway to promote cancer cell invasion, macrophage and endothelial cell recruitment at primary sites, and cancer cell survival at distant organs. Treatment with a newly derived monoclonal antibody against IL-17RB blocked tumor metastasis and promoted survival in a mouse xenograft model. These findings not only illustrate a key mechanism underlying the highly aggressive characteristics of pancreatic cancer but also provide a practical approach to tackle this disease.
机译:胰腺癌具有侵袭性转移特性,因此死亡率极高。解决潜在的机制对于治疗至关重要。在这里,我们发现胰腺癌患者中IL-17B受体(IL-17RB)的过表达与术后转移密切相关,而与无进展生存则呈负相关。一致地,来自离体实验的结果进一步证实了IL-17RB及其配体IL-17B在胰腺癌转移和恶性肿瘤中起着重要作用。 IL-17B–IL-17RB的信号通过ERK1 / 2途径激活CCL20 / CXCL1 / IL-8 / TFF1趋化因子的表达,从而促进癌细胞侵袭,巨噬细胞和内皮细胞在主要部位的募集以及远端器官的癌细胞存活。在小鼠异种移植模型中,用新获得的针对IL-17RB的单克隆抗体治疗可阻断肿瘤转移并提高生存率。这些发现不仅说明了胰腺癌高度侵袭性特征的关键机制,而且为解决该疾病提供了一种实用的方法。

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