Oncogenic ERRB2 signals through the AP-1 transcription factor to control mesenchymal-like properties of oesophageal adenocarcinoma.

NAR Cancer Pub Date : 2023-01-23 eCollection Date: 2023-03-01 DOI:10.1093/narcan/zcad001
Samuel Ogden, Ibrahim Ahmed, Shen-Hsi Yang, Paul Fullwood, Chiara Francavilla, Andrew D Sharrocks
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Abstract

Oesophageal adenocarcinoma (OAC) is a deadly disease with poor survival statistics and few targeted therapies available. One of the most common molecular aberrations in OAC is amplification or activation of the gene encoding the receptor tyrosine kinase ERBB2, and ERBB2 is targeted in the clinic for this subset of patients. However, the downstream consequences of these ERBB2 activating events are not well understood. Here we used a combination of phosphoproteomics, open chromatin profiling and transcriptome analysis on cell line models and patient-derived datasets to interrogate the molecular pathways operating downstream from ERBB2. Integrated analysis of these data sets converge on a model where dysregulated ERBB2 signalling is mediated at the transcriptional level by the transcription factor AP-1. AP-1 in turn controls cell behaviour by acting on cohorts of genes that regulate cell migration and adhesion, features often associated with EMT. Our study therefore provides a valuable resource for the cancer cell signalling community and reveals novel molecular determinants underlying the dysregulated behaviour of OAC cells.

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致癌物质ERRB2通过AP-1转录因子发出信号,控制食管腺癌的间质样特性。
食管腺癌(OAC)是一种致命疾病,存活率很低,而且几乎没有靶向疗法。食管腺癌最常见的分子畸变之一是编码受体酪氨酸激酶ERBB2的基因扩增或激活,ERBB2在临床上是这部分患者的靶向药物。然而,人们对这些ERBB2激活事件的下游后果还不甚了解。在这里,我们在细胞系模型和患者数据集上结合使用了磷蛋白组学、开放染色质图谱分析和转录组分析,以探究ERBB2下游的分子通路。对这些数据集的综合分析汇聚到一个模型上,即ERBB2信号失调是由转录因子AP-1在转录水平上介导的。AP-1反过来又通过作用于调控细胞迁移和粘附的基因群来控制细胞行为,这些基因群通常与EMT相关。因此,我们的研究为癌细胞信号社区提供了宝贵的资源,并揭示了 OAC 细胞行为失调的新分子决定因素。
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