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Nerve-to-cancer transfer of mitochondria during cancer metastasis

癌细胞 癌症 线粒体 转移 癌症干细胞 重编程 神经科学 神经系统 癌症研究 生物 细胞 细胞生物学 生物化学 遗传学
作者
Gregory Hoover,Shila Gilbert,Olivia Curley,Clémence Obellianne,Mike T. Lin,William Hixson,Terry W. Pierce,Joel Andrews,Mikhail Alexeyev,Yi Ding,Ping Bu,Fariba Behbod,Daniel Medina,Jeffrey T. Chang,Gustavo Ayala,Simon Grelet
出处
期刊:Nature [Nature Portfolio]
卷期号:644 (8075): 252-262 被引量:88
标识
DOI:10.1038/s41586-025-09176-8
摘要

The nervous system has a pivotal role in cancer biology, and pathological investigations have linked intratumoural nerve density to metastasis1. However, the precise impact of cancer-associated neurons and the communication channels at the nerve–cancer interface remain poorly understood. Previous cancer denervation models in rodents and humans have highlighted robust cancer dependency on nerves, but the underlying mechanisms that drive nerve-mediated cancer aggressivity remain unknown2,3. Here we show that cancer-associated neurons enhance cancer metabolic plasticity by transferring mitochondria to cancer cells. Breast cancer denervation and nerve–cancer coculture models confirmed that neurons significantly improve tumour energetics. Neurons cocultured with cancer cells undergo metabolic reprogramming, resulting in increased mitochondrial mass and subsequent transfer of mitochondria to adjacent cancer cells. To precisely track the fate of recipient cells, we developed MitoTRACER, a reporter of cell-to-cell mitochondrial transfer that permanently labels recipient cancer cells and their progeny. Lineage tracing and fate mapping of cancer cells acquiring neuronal mitochondria in primary tumours revealed their selective enrichment at metastatic sites following dissemination. Collectively, our data highlight the enhanced metastatic capabilities of cancer cells that receive mitochondria from neurons in primary tumours, shedding new light on how the nervous system supports cancer metabolism and metastatic dissemination. A study reports the development of a method to trace intercellular transfer of mitochondria, and demonstrates that cancer cells that receive mitochondria from neurons have enhanced metastatic capabilities.
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