Department of Physiology and Pharmacology, Karolinska Institutet, Stockholm, Sweden.
Department of Immunology, Genetics and Pathology, Uppsala University, Rudbeck Laboratory, Uppsala, Sweden.
Mol Cancer Res. 2020 Oct;18(10):1522-1533. doi: 10.1158/1541-7786.MCR-20-0292. Epub 2020 Jul 14.
Children suffering from neurologic cancers undergoing chemotherapy and radiotherapy are at high risk of reduced neurocognitive abilities likely via damage to proliferating neural stem cells (NSC). Therefore, strategies to protect NSCs are needed. We argue that induced cell-cycle arrest/quiescence in NSCs during cancer treatment can represent such a strategy. Here, we show that hyperpolarization-activated cyclic nucleotide-gated (HCN) ion channels are dynamically expressed over the cell cycle in NSCs, depolarize the membrane potential, underlie spontaneous calcium oscillations and are required to maintain NSCs in the actively proliferating pool. Hyperpolarizing pharmacologic inhibition of HCN channels during exposure to ionizing radiation protects NSCs cells in neurogenic brain regions of young mice. In contrast, brain tumor-initiating cells, which also express HCN channels, remain proliferative during HCN inhibition. IMPLICATIONS: Our finding that NSCs can be selectively rescued while cancer cells remain sensitive to the treatment, provide a foundation for reduction of cognitive impairment in children with neurologic cancers.
正在接受化疗和放疗的神经癌患儿存在神经认知能力下降的高风险,这可能是由于增殖中的神经干细胞 (NSC) 受损所致。因此,需要寻找保护 NSC 的策略。我们认为,在癌症治疗过程中诱导 NSC 中的细胞周期停滞/静止可以作为一种策略。在这里,我们表明,在 NSC 中,超极化激活环核苷酸门控 (HCN) 离子通道在细胞周期中动态表达,去极化膜电位,构成自发性钙震荡的基础,并需要维持 NSC 处于活跃增殖池中。在暴露于电离辐射期间,超极化药理学抑制 HCN 通道可保护年轻小鼠神经发生脑区的 NSC 细胞。相比之下,也表达 HCN 通道的脑肿瘤起始细胞在 HCN 抑制期间仍保持增殖。意义:我们的发现表明,在保留癌细胞对治疗敏感性的同时,可以选择性地拯救 NSC,为减少神经癌患儿的认知障碍提供了基础。
