ENO1 Promotes Lung Cancer Metastasis via HGFR and WNT Signaling-Driven Epithelial-to-Mesenchymal Transition.

IF 16.6 1区医学 Q1 ONCOLOGY

Cancer research Pub Date : 2021-08-01 Epub Date: 2021-06-18 DOI:10.1158/0008-5472.CAN-20-3543

Hsin-Jung Li, Feng-Yi Ke, Chia-Ching Lin, Mei-Yi Lu, Yi-Huei Kuo, Yi-Ping Wang, Kang-Hao Liang, Shin-Chang Lin, Ya-Hsuan Chang, Hsuan-Yu Chen, Pan-Chyr Yang, Han-Chung Wu

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引用次数: 42

Abstract

ENO1 (α-enolase) expression is significantly correlated with reduced survival and poor prognosis in many cancer types, including lung cancer. However, the function of ENO1 in carcinogenesis remains elusive. In this study, we found that high expression of ENO1 is present in metastatic lung cancer cell lines and malignant tumors and is associated with poor overall survival of patients with lung cancer. Knockdown of ENO1 decreased cancer cell proliferation and invasiveness, whereas overexpression of ENO1 enhanced these processes. Moreover, ENO1 expression promoted tumor growth in orthotopic models and enhanced lung tumor metastasis in tail-vein injection models. These effects were mediated by upregulation of mesenchymal markers N-cadherin and vimentin and the epithelial-to-mesenchymal transition regulator SLUG, along with concurrent downregulation of E-cadherin. Mechanistically, ENO1 interacted with hepatocyte growth factor receptor (HGFR) and activated HGFR and Wnt signaling via increased phosphorylation of HGFR and the Wnt coreceptor LRP5/6. Activation of these signaling axes decreased GSK3β activity via Src-PI3K-AKT signaling and inactivation of the β-catenin destruction complex to ultimately upregulate SLUG and β-catenin. In addition, we generated a chimeric anti-ENO1 mAb (chENO1-22) that can decrease cancer cell proliferation and invasion. chENO1-22 attenuated cancer cell invasion by inhibiting ENO1-mediated GSK3β inactivation to promote SLUG protein ubiquitination and degradation. Moreover, chENO1-22 prevented lung tumor metastasis and prolonged survival in animal models. Taken together, these findings illuminate the molecular mechanisms underlying the function of ENO1 in lung cancer metastasis and support the therapeutic potential of a novel antibody targeting ENO1 for treating lung cancer. SIGNIFICANCE: This study shows that ENO1 promotes lung cancer metastasis via HGFR and WNT signaling and introduces a novel anti-ENO1 antibody for potential therapeutic use in lung cancer.

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ENO1通过HGFR和WNT信号驱动的上皮-间质转化促进肺癌转移。

在包括肺癌在内的多种癌症中，ENO1 (α-烯醇化酶)的表达与生存率降低和预后不良显著相关。然而，ENO1在癌变中的作用尚不清楚。在本研究中，我们发现ENO1在转移性肺癌细胞系和恶性肿瘤中存在高表达，并与肺癌患者的总生存率低相关。敲低ENO1可降低癌细胞的增殖和侵袭性，而过表达ENO1可增强这些过程。此外，在原位模型中，ENO1的表达促进了肿瘤的生长，在尾静脉注射模型中，ENO1的表达促进了肺肿瘤的转移。这些作用是由间质标记物N-cadherin和vimentin以及上皮到间质转化调节因子SLUG上调介导的，同时E-cadherin下调。在机制上，ENO1与肝细胞生长因子受体(HGFR)相互作用，并通过增加HGFR和Wnt辅受体LRP5/6的磷酸化激活HGFR和Wnt信号传导。这些信号轴的激活通过Src-PI3K-AKT信号传导降低GSK3β活性，并使β-catenin破坏复合物失活，最终上调SLUG和β-catenin。此外，我们制备了一种嵌合抗eno1单抗(chENO1-22)，可以降低癌细胞的增殖和侵袭。chen01 -22通过抑制en01介导的GSK3β失活，促进SLUG蛋白泛素化和降解，从而减弱癌细胞的侵袭。此外，在动物模型中，chENO1-22可阻止肺肿瘤转移并延长生存期。综上所述，这些发现阐明了ENO1在肺癌转移中功能的分子机制，并支持一种靶向ENO1的新型抗体治疗肺癌的治疗潜力。意义:本研究表明ENO1通过HGFR和WNT信号通路促进肺癌转移，并引入了一种新的抗ENO1抗体，有望用于肺癌的治疗。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Cancer research 医学-肿瘤学

CiteScore

16.10

自引率

0.90%

发文量

7677

审稿时长

2.5 months

期刊介绍： Cancer Research, published by the American Association for Cancer Research (AACR), is a journal that focuses on impactful original studies, reviews, and opinion pieces relevant to the broad cancer research community. Manuscripts that present conceptual or technological advances leading to insights into cancer biology are particularly sought after. The journal also places emphasis on convergence science, which involves bridging multiple distinct areas of cancer research. With primary subsections including Cancer Biology, Cancer Immunology, Cancer Metabolism and Molecular Mechanisms, Translational Cancer Biology, Cancer Landscapes, and Convergence Science, Cancer Research has a comprehensive scope. It is published twice a month and has one volume per year, with a print ISSN of 0008-5472 and an online ISSN of 1538-7445. Cancer Research is abstracted and/or indexed in various databases and platforms, including BIOSIS Previews (R) Database, MEDLINE, Current Contents/Life Sciences, Current Contents/Clinical Medicine, Science Citation Index, Scopus, and Web of Science.