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Merck

Mechanosensitive brain tumor cells construct blood-tumor barrier to mask chemosensitivity.

Neuron (2022-11-03)
Xin Chen, Ali Momin, Siyi Wanggou, Xian Wang, Hyun-Kee Min, Wenkun Dou, Zheyuan Gong, Jade Chan, Weifan Dong, Jerry J Fan, Yi Xiong, Kamilia Talipova, Hongyu Zhao, Yuki X Chen, Kelly Veerasammy, Adam Fekete, Sachin A Kumar, Hongwei Liu, Qi Yang, Joe Eun Son, Zhengchao Dou, Malini Hu, Parnian Pardis, Kyle Juraschka, Laura K Donovan, Jiao Zhang, Vijay Ramaswamy, Hayden J Selvadurai, Peter B Dirks, Michael D Taylor, Lu-Yang Wang, Chi-Chung Hui, Rinat Abzalimov, Ye He, Yu Sun, Xuejun Li, Xi Huang
ABSTRAKT

Major obstacles in brain cancer treatment include the blood-tumor barrier (BTB), which limits the access of most therapeutic agents, and quiescent tumor cells, which resist conventional chemotherapy. Here, we show that Sox2+ tumor cells project cellular processes to ensheathe capillaries in mouse medulloblastoma (MB), a process that depends on the mechanosensitive ion channel Piezo2. MB develops a tissue stiffness gradient as a function of distance to capillaries. Sox2+ tumor cells perceive substrate stiffness to sustain local intracellular calcium, actomyosin tension, and adhesion to promote cellular process growth and cell surface sequestration of β-catenin. Piezo2 knockout reverses WNT/β-catenin signaling states between Sox2+ tumor cells and endothelial cells, compromises the BTB, reduces the quiescence of Sox2+ tumor cells, and markedly enhances the MB response to chemotherapy. Our study reveals that mechanosensitive tumor cells construct the BTB to mask tumor chemosensitivity. Targeting Piezo2 addresses the BTB and tumor quiescence properties that underlie treatment failures in brain cancer.

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