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死亡决定:细胞恢复力与癌症治疗抗性之间的联系。

Death-ision: the link between cellular resilience and cancer resistance to treatments.

作者信息

Baldassarre Gustavo, L de la Serna Ivana, Vallette François M

机构信息

Division of Molecular Oncology, Centro di Riferimento Oncologico di Aviano (CRO) IRCCS, National Cancer Institute, Aviano, 33081, Italy.

Department of Cell and Cancer Biology, University of Toledo College of Medicine and Life Sciences, Toledo, OH, 43614, USA.

出版信息

Mol Cancer. 2025 May 15;24(1):144. doi: 10.1186/s12943-025-02339-1.

Abstract

One of the key challenges in defeating advanced tumors is the ability of cancer cells to evade the selective pressure imposed by chemotherapy, targeted therapies, immunotherapy and cellular therapies. Both genetic and epigenetic alterations contribute to the development of resistance, allowing cancer cells to survive initially effective treatments. In this narration, we explore how genetic and epigenetic regulatory mechanisms influence the state of tumor cells and their responsiveness to different therapeutic strategies. We further propose that an altered balance between cell growth and cell death is a fundamental driver of drug resistance. Cell death programs exist in various forms, shaped by cell type, triggering factors, and microenvironmental conditions. These processes are governed by temporal and spatial constraints and appear to be more heterogeneous than previously understood. To capture the intricate interplay between death-inducing signals and survival mechanisms, we introduce the concept of Death-ision. This framework highlights the dynamic nature of cell death regulation, determining whether specific cancer cell clones evade or succumb to therapy. Building on this understanding offers promising strategies to counteract resistant clones and enhance therapeutic efficacy. For instance, combining DNMT inhibitors with immune checkpoint blockade may counteract YAP1-driven resistance or the use of transcriptional CDK inhibitors could prevent or overcome chemotherapy resistance. Death-ision aims to provide a deeper understanding of the diversity and evolution of cell death programs, not only at diagnosis but also throughout disease progression and treatment adaptation.

摘要

攻克晚期肿瘤的关键挑战之一在于癌细胞逃避化疗、靶向治疗、免疫治疗和细胞治疗所施加的选择性压力的能力。遗传和表观遗传改变均有助于耐药性的产生,使癌细胞能够在起初有效的治疗中存活下来。在本文中,我们探讨遗传和表观遗传调控机制如何影响肿瘤细胞的状态及其对不同治疗策略的反应。我们进一步提出,细胞生长与细胞死亡之间平衡的改变是耐药性的根本驱动因素。细胞死亡程序以多种形式存在,由细胞类型、触发因素和微环境条件所塑造。这些过程受时间和空间限制,且似乎比之前所理解的更加异质性。为了捕捉死亡诱导信号与生存机制之间复杂的相互作用,我们引入了“死亡决策”的概念。该框架突出了细胞死亡调控的动态性质,决定特定癌细胞克隆是逃避还是屈服于治疗。基于这种理解提供了对抗耐药克隆和提高治疗效果的有前景的策略。例如,将DNA甲基转移酶抑制剂与免疫检查点阻断相结合可能对抗YAP1驱动的耐药性,或者使用转录CDK抑制剂可以预防或克服化疗耐药性。“死亡决策”旨在不仅在诊断时,而且在整个疾病进展和治疗调整过程中,更深入地理解细胞死亡程序的多样性和演变。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e063/12080166/2e43598c39cd/12943_2025_2339_Fig1_HTML.jpg

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