Epigenetic adaptations in drug-tolerant tumor cells.

2区 医学 Q1 Medicine Advances in Cancer Research Pub Date : 2023-01-01 DOI:10.1016/bs.acr.2022.12.006
Nilanjana Mani, Ankita Daiya, Rajdeep Chowdhury, Sudeshna Mukherjee, Shibasish Chowdhury
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引用次数: 3

Abstract

Traditional chemotherapy against cancer is often severely hampered by acquired resistance to the drug. Epigenetic alterations and other mechanisms like drug efflux, drug metabolism, and engagement of survival pathways are crucial in evading drug pressure. Herein, growing evidence suggests that a subpopulation of tumor cells can often tolerate drug onslaught by entering a "persister" state with minimal proliferation. The molecular features of these persister cells are gradually unraveling. Notably, the "persisters" act as a cache of cells that can eventually re-populate the tumor post-withdrawal drug pressure and contribute to acquiring stable drug-resistant features. This underlines the clinical significance of the tolerant cells. Accumulating evidence highlights the importance of modulation of the epigenome as a critical adaptive strategy for evading drug pressure. Chromatin remodeling, altered DNA methylation, and de-regulation of non-coding RNA expression and function contribute significantly to this persister state. No wonder targeting adaptive epigenetic modifications is increasingly recognized as an appropriate therapeutic strategy to sensitize them and restore drug sensitivity. Furthermore, manipulating the tumor microenvironment and "drug holiday" is also explored to maneuver the epigenome. However, heterogeneity in adaptive strategies and lack of targeted therapies have significantly hindered the translation of epigenetic therapy to the clinics. In this review, we comprehensively analyze the epigenetic alterations adapted by the drug-tolerant cells, the therapeutic strategies employed to date, and their limitations and future prospects.

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耐药肿瘤细胞的表观遗传适应。
传统的癌症化疗往往受到获得性耐药性的严重阻碍。表观遗传改变和其他机制如药物外排、药物代谢和参与生存途径是逃避药物压力的关键。在此,越来越多的证据表明,肿瘤细胞亚群通常可以通过进入最小增殖的“持久”状态来耐受药物攻击。这些持久性细胞的分子特征正在逐渐揭示。值得注意的是,“持久者”作为细胞的缓存,最终可以在停药后重新填充肿瘤,并有助于获得稳定的耐药特征。这强调了耐受性细胞的临床意义。越来越多的证据强调了表观基因组调节作为逃避药物压力的关键适应策略的重要性。染色质重塑、DNA甲基化改变和非编码RNA表达和功能的去调控对这种持续状态有重要作用。难怪靶向适应性表观遗传修饰越来越被认为是使它们增敏和恢复药物敏感性的适当治疗策略。此外,还探索了操纵肿瘤微环境和“药物假期”来操纵表观基因组。然而,适应性策略的异质性和靶向治疗的缺乏严重阻碍了表观遗传治疗的临床应用。在这篇综述中,我们全面分析了耐药细胞适应的表观遗传改变,迄今为止采用的治疗策略,以及它们的局限性和未来前景。
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来源期刊
Advances in Cancer Research
Advances in Cancer Research 医学-肿瘤学
CiteScore
10.00
自引率
0.00%
发文量
52
期刊介绍: Advances in Cancer Research (ACR) has covered a remarkable period of discovery that encompasses the beginning of the revolution in biology. Advances in Cancer Research (ACR) has covered a remarkable period of discovery that encompasses the beginning of the revolution in biology. The first ACR volume came out in the year that Watson and Crick reported on the central dogma of biology, the DNA double helix. In the first 100 volumes are found many contributions by some of those who helped shape the revolution and who made many of the remarkable discoveries in cancer research that have developed from it.
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