A subset of metastatic pancreatic ductal adenocarcinomas depends quantitatively on oncogenic Kras/Mek/Erk-induced hyperactive mTOR signalling

克拉斯 MAPK/ERK通路 PI3K/AKT/mTOR通路 胰腺导管腺癌 癌症研究 医学 信号 胰腺 内科学 生物 肿瘤科 胰腺癌 激酶 癌症 信号转导 细胞生物学 结直肠癌
作者
Bo Kong,Weiwei Wu,Tao Cheng,Anna Melissa Schlitter,Chengjia Qian,Philipp Bruns,Ziying Jian,Carsten Jäger,Ivonne Regel,Susanne Raulefs,Nora Behler,Martin Irmler,Johannes Beckers,Helmut Friess,Mert Erkan,Jens T. Siveke,Andrea Tannapfel,Stephan A. Hahn,Fabian J. Theis,Iréne Esposito
出处
期刊:Gut [BMJ]
卷期号:65 (4): 647-657 被引量:111
标识
DOI:10.1136/gutjnl-2014-307616
摘要

Objective Oncogenic Kras-activated robust Mek/Erk signals phosphorylate to the tuberous sclerosis complex (Tsc) and deactivates mammalian target of rapamycin (mTOR) suppression in pancreatic ductal adenocarcinoma (PDAC); however, Mek and mTOR inhibitors alone have demonstrated minimal clinical antitumor activity. Design We generated transgenic mouse models in which mTOR was hyperactivated either through the Kras/Mek/Erk cascade, by loss of Pten or through Tsc1 haploinsufficiency. Primary cancer cells were isolated from mouse tumours. Oncogenic signalling was assessed in vitro and in vivo, with and without single or multiple targeted molecule inhibition. Transcriptional profiling was used to identify biomarkers predictive of the underlying pathway alterations and of therapeutic response. Results from the preclinical models were confirmed on human material. Results Reduction of Tsc1 function facilitated activation of Kras/Mek/Erk-mediated mTOR signalling, which promoted the development of metastatic PDACs. Single inhibition of mTOR or Mek elicited strong feedback activation of Erk or Akt, respectively. Only dual inhibition of Mek and PI3K reduced mTOR activity and effectively induced cancer cell apoptosis. Analysis of downstream targets demonstrated that oncogenic activity of the Mek/Erk/Tsc/mTOR axis relied on Aldh1a3 function. Moreover, in clinical PDAC samples, ALDH1A3 specifically labelled an aggressive subtype. Conclusions These results advance our understanding of Mek/Erk-driven mTOR activation and its downstream targets in PDAC, and provide a mechanistic rationale for effective therapeutic matching for Aldh1a3-positive PDACs.
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