School of Integrative Medicine, Tianjin University of Traditional Chinese Medicine, Tianjin, China.
Department of Pathology, Tianjin Union Medical Center, Tianjin, China.
Clin Transl Med. 2024 Feb;14(2):e1567. doi: 10.1002/ctm2.1567.
Tumour cell dormancy is critical for metastasis and resistance to chemoradiotherapy. Polyploid giant cancer cells (PGCCs) with giant or multiple nuclei and high DNA content have the properties of cancer stem cell and single PGCCs can individually generate tumours in immunodeficient mice. PGCCs represent a dormant form of cancer cells that survive harsh tumour conditions and contribute to tumour recurrence. Hypoxic mimics, chemotherapeutics, radiation and cytotoxic traditional Chinese medicines can induce PGCCs formation through endoreduplication and/or cell fusion. After incubation, dormant PGCCs can recover from the treatment and produce daughter cells with strong proliferative, migratory and invasive abilities via asymmetric cell division. Additionally, PGCCs can resist hypoxia or chemical stress and have a distinct protein signature that involves chromatin remodelling and cell cycle regulation. Dormant PGCCs form the cellular basis for therapeutic resistance, metastatic cascade and disease recurrence. This review summarises regulatory mechanisms governing dormant cancer cells entry and exit of dormancy, which may be used by PGCCs, and potential therapeutic strategies for targeting PGCCs.
肿瘤细胞休眠对于转移和化学放射治疗抵抗至关重要。具有巨大或多个核和高 DNA 含量的多倍体巨癌细胞 (PGCC) 具有癌症干细胞的特性,单个 PGCC 可以在免疫缺陷小鼠中单独生成肿瘤。PGCC 代表了一种休眠形式的癌细胞,能够在恶劣的肿瘤条件下存活,并促进肿瘤复发。缺氧模拟物、化疗药物、辐射和细胞毒性中药可以通过内复制和/或细胞融合诱导 PGCC 的形成。孵育后,休眠的 PGCC 可以从治疗中恢复,并通过不对称细胞分裂产生具有强大增殖、迁移和侵袭能力的子细胞。此外,PGCC 可以抵抗缺氧或化学应激,并且具有独特的蛋白质特征,涉及染色质重塑和细胞周期调控。休眠的 PGCC 形成了治疗抵抗、转移级联和疾病复发的细胞基础。本文综述了调控休眠肿瘤细胞进入和退出休眠的机制,这些机制可能被 PGCC 利用,以及针对 PGCC 的潜在治疗策略。
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