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Colon tumour cell death causes mTOR dependence by paracrine P2X4 stimulation

旁分泌信号 PI3K/AKT/mTOR通路 癌症研究 程序性细胞死亡 细胞凋亡 刺激 结直肠癌 生物 癌症 医学 细胞生物学 化学 内科学 信号转导 受体 遗传学
作者
Mark R. Schmitt,Fatih Ceteci,J. R. P. Gupta,Marina Pešić,Tim W. Böttger,Adele M. Nicolas,Kilian B. Kennel,Esther Engel,Matthias Schewe,Asude Callak Kirisözü,Valentina Petrocelli,Yasamin Dabiri,Júlia Varga,Mallika Ramakrishnan,Madina Karimova,Andrea Ablasser,Toshiro Sato,Melek C. Arkan,Frédéric J. de Sauvage,Florian R. Greten
出处
期刊:Nature [Nature Portfolio]
卷期号:612 (7939): 347-353 被引量:84
标识
DOI:10.1038/s41586-022-05426-1
摘要

Solid cancers exhibit a dynamic balance between cell death and proliferation ensuring continuous tumour maintenance and growth1,2. Increasing evidence links enhanced cancer cell apoptosis to paracrine activation of cells in the tumour microenvironment initiating tissue repair programs that support tumour growth3,4, yet the direct effects of dying cancer cells on neighbouring tumour epithelia and how this paracrine effect potentially contributes to therapy resistance are unclear. Here we demonstrate that chemotherapy-induced tumour cell death in patient-derived colorectal tumour organoids causes ATP release triggering P2X4 (also known as P2RX4) to mediate an mTOR-dependent pro-survival program in neighbouring cancer cells, which renders surviving tumour epithelia sensitive to mTOR inhibition. The induced mTOR addiction in persisting epithelial cells is due to elevated production of reactive oxygen species and subsequent increased DNA damage in response to the death of neighbouring cells. Accordingly, inhibition of the P2X4 receptor or direct mTOR blockade prevents induction of S6 phosphorylation and synergizes with chemotherapy to cause massive cell death induced by reactive oxygen species and marked tumour regression that is not seen when individually applied. Conversely, scavenging of reactive oxygen species prevents cancer cells from becoming reliant on mTOR activation. Collectively, our findings show that dying cancer cells establish a new dependency on anti-apoptotic programs in their surviving neighbours, thereby creating an opportunity for combination therapy in P2X4-expressing epithelial tumours. Chemotherapy-induced death of colon cancer cells causes ATP release triggering P2X4 to mediate an mTOR-dependent pro-survival program in neighbouring cancer cells, which renders them sensitive to mTOR inhibition.
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