PML 核体:与癌症的联系及其他。

Nucleus (Austin, Tex.) Pub Date : 2024-12-01 Epub Date: 2024-02-27 DOI:10.1080/19491034.2024.2321265
Majdouline Abou-Ghali, Valérie Lallemand-Breitenbach
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引用次数: 0

摘要

早幼粒细胞白血病(PML)核体是细胞核中的无膜细胞器,在细胞平衡中发挥着至关重要的作用。这些动态结构是由支架 PML 蛋白和各种伙伴组装而成的。最近的晶体结构分析揭示了重要的自相互作用结构域,而液相-液相分离有助于它们的形成。PML 机构可协调翻译后修饰,尤其是应激诱导的 SUMOylation,从而影响目标蛋白质的功能。作为多种信号通路的枢纽,它们会影响衰老等细胞过程。PML 表达失调会导致包括癌症在内的各种疾病,这凸显了它们的重要性。在治疗方面,PML 体是很有希望的靶点,用三氧化二砷和维甲酸治疗急性早幼粒细胞白血病成功地恢复了 PML 体就是一个例子。了解它们的功能可以阐明正常和病理细胞生理学,为潜在疗法提供指导。本综述探讨了 PML 体生物发生、生化活性及其不断演变的生物学作用方面的最新进展。
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PML Nuclear bodies: the cancer connection and beyond.

Promyelocytic leukemia (PML) nuclear bodies, membrane-less organelles in the nucleus, play a crucial role in cellular homeostasis. These dynamic structures result from the assembly of scaffolding PML proteins and various partners. Recent crystal structure analyses revealed essential self-interacting domains, while liquid-liquid phase separation contributes to their formation. PML bodies orchestrate post-translational modifications, particularly stress-induced SUMOylation, impacting target protein functions. Serving as hubs in multiple signaling pathways, they influence cellular processes like senescence. Dysregulation of PML expression contributes to diseases, including cancer, highlighting their significance. Therapeutically, PML bodies are promising targets, exemplified by successful acute promyelocytic leukemia treatment with arsenic trioxide and retinoic acid restoring PML bodies. Understanding their functions illuminates both normal and pathological cellular physiology, guiding potential therapies. This review explores recent advancements in PML body biogenesis, biochemical activity, and their evolving biological roles.

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