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MET∆14 促进配体依赖性、AKT 驱动的浸润性生长。

MET∆14 promotes a ligand-dependent, AKT-driven invasive growth.

机构信息

Istituto Fondazione di Oncologia Molecolare - La Fondazione Italiana per la Ricerca sul Cancro (IFOM - FIRC) Institute of Molecular Oncology, Milano, Italy.

Department of Molecular Biotechnology and Health Sciences, University of Torino, Torino, Italy.

出版信息

Life Sci Alliance. 2022 May 30;5(10). doi: 10.26508/lsa.202201409. Print 2022 Oct.

Abstract

is an oncogene encoding the tyrosine kinase receptor for hepatocyte growth factor (HGF). Upon ligand binding, MET activates multiple signal transducers, including PI3K/AKT, STAT3, and MAPK. When mutated or amplified, becomes a "driver" for the onset and progression of cancer. The most frequent mutations in the gene affect the splicing sites of exon 14, leading to the deletion of the receptor's juxtamembrane domain (MET∆14). It is currently believed that, as in gene amplification, MET∆14 kinase is constitutively active. Our analysis of MET in carcinoma cell lines showed that MET∆14 strictly depends on HGF for kinase activation. Compared with wt MET, ∆14 is sensitive to lower HGF concentrations, with more sustained kinase response. Using three different models, we have demonstrated that MET∆14 activation leads to robust phosphorylation of AKT, leading to a distinctive transcriptomic signature. Functional studies revealed that ∆14 activation is predominantly responsible for enhanced protection from apoptosis and cellular migration. Thus, the unique HGF-dependent ∆14 oncogenic activity suggests consideration of HGF in the tumour microenvironment to select patients for clinical trials.

摘要

是一种癌基因,编码肝细胞生长因子(HGF)的酪氨酸激酶受体。配体结合后,MET 激活多种信号转导物,包括 PI3K/AKT、STAT3 和 MAPK。当发生突变或扩增时,就成为癌症发生和进展的“驱动基因”。基因中最常见的突变影响外显子 14 的剪接位点,导致受体的跨膜区缺失(MET∆14)。目前认为,与基因扩增一样,MET∆14 激酶是持续激活的。我们对癌细胞系中的 MET 分析表明,MET∆14 严格依赖 HGF 进行激酶激活。与 wt MET 相比,∆14 对较低的 HGF 浓度更敏感,激酶反应更持久。通过三种不同的模型,我们证明了 MET∆14 的激活导致 AKT 的强烈磷酸化,从而产生独特的转录组特征。功能研究表明,∆14 的激活主要负责增强对细胞凋亡和细胞迁移的保护。因此,独特的 HGF 依赖性 ∆14 致癌活性表明,在肿瘤微环境中应考虑 HGF,以选择适合临床试验的患者。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b0e4/9152130/39b51b87d981/LSA-2022-01409_Fig1.jpg

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