Crosstalk between small-cell lung cancer cells and astrocytes mimics brain development to promote brain metastasis

串扰 脑转移 星形胶质细胞 生物 神经科学 癌症研究 神经元 转移 细胞生物学 中枢神经系统 癌症 物理 光学 遗传学
作者
Fangfei Qu,Siqi Cao,Wojciech Michno,Chioma J. Madubata,Griffin G. Hartmann,Alyssa Puno,Alexandros P. Drainas,Debadrita Bhattacharya,Erwin Tomasich,Myung Chang Lee,Dian Yang,Jun Kim,Maria Peiris‐Pagès,Kathryn Simpson,Caroline Dive,Matthias Preusser,Angus Toland,Christina S. Kong,Millie Das,Monte M. Winslow
出处
期刊:Nature Cell Biology [Nature Portfolio]
卷期号:25 (10): 1506-1519 被引量:50
标识
DOI:10.1038/s41556-023-01241-6
摘要

Brain metastases represent an important clinical problem for patients with small-cell lung cancer (SCLC). However, the mechanisms underlying SCLC growth in the brain remain poorly understood. Here, using intracranial injections in mice and assembloids between SCLC aggregates and human cortical organoids in culture, we found that SCLC cells recruit reactive astrocytes to the tumour microenvironment. This crosstalk between SCLC cells and astrocytes drives the induction of gene expression programmes that are similar to those found during early brain development in neurons and astrocytes. Mechanistically, the brain development factor Reelin, secreted by SCLC cells, recruits astrocytes to brain metastases. These astrocytes in turn promote SCLC growth by secreting neuronal pro-survival factors such as SERPINE1. Thus, SCLC brain metastases grow by co-opting mechanisms involved in reciprocal neuron–astrocyte interactions during brain development. Targeting such developmental programmes activated in this cancer ecosystem may help prevent and treat brain metastases. Qu et al. identify and characterize reciprocal crosstalk between small-cell lung cancer cells and astrocytes, which mimics neuron–astrocyte interactions during brain development and promotes brain metastasis.
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