癌症细胞从治疗暴露中恢复的表观遗传调控及其作为预防疾病复发的新治疗策略的意义。

2区 医学 Q1 Medicine Advances in Cancer Research Pub Date : 2023-01-01 DOI:10.1016/bs.acr.2022.11.001
Christiana O Appiah, Manjulata Singh, Lauren May, Ishita Bakshi, Ashish Vaidyanathan, Paul Dent, Gordon Ginder, Steven Grant, Harry Bear, Joseph Landry
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引用次数: 1

摘要

癌症治疗的最终目标是消除病人身上的疾病。最直接的方式是通过治疗诱导的细胞死亡。治疗诱导的生长停滞如果延长,也是一个理想的结果。不幸的是,治疗引起的生长停滞很少是持久的,恢复的细胞群可能导致癌症复发。因此,消除残留癌细胞的治疗策略减少了复发的机会。恢复可以通过多种机制发生,包括静止或滞育、退出衰老、抑制凋亡、细胞保护性自噬和由多倍体引起的还原性分裂。基因组的表观遗传调控是癌症特异性生物学的基本调控机制,包括治疗后的恢复。表观遗传途径是特别有吸引力的治疗靶点,因为它们是可逆的,不改变DNA,并由药物酶催化。由于不可接受的毒性或有限的疗效,先前使用表观遗传靶向疗法与癌症治疗药物联合使用尚未广泛成功。在初始癌症治疗后的一段时间内使用表观遗传靶向治疗可能会潜在地降低联合策略的毒性,并可能利用治疗暴露后的基本表观遗传状态。这篇综述探讨了使用顺序方法靶向表观遗传机制的可行性,以消除残留的治疗阻滞种群,这可能会防止恢复和疾病复发。
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The epigenetic regulation of cancer cell recovery from therapy exposure and its implications as a novel therapeutic strategy for preventing disease recurrence.

The ultimate goal of cancer therapy is the elimination of disease from patients. Most directly, this occurs through therapy-induced cell death. Therapy-induced growth arrest can also be a desirable outcome, if prolonged. Unfortunately, therapy-induced growth arrest is rarely durable and the recovering cell population can contribute to cancer recurrence. Consequently, therapeutic strategies that eliminate residual cancer cells reduce opportunities for recurrence. Recovery can occur through diverse mechanisms including quiescence or diapause, exit from senescence, suppression of apoptosis, cytoprotective autophagy, and reductive divisions resulting from polyploidy. Epigenetic regulation of the genome represents a fundamental regulatory mechanism integral to cancer-specific biology, including the recovery from therapy. Epigenetic pathways are particularly attractive therapeutic targets because they are reversible, without changes in DNA, and are catalyzed by druggable enzymes. Previous use of epigenetic-targeting therapies in combination with cancer therapeutics has not been widely successful because of either unacceptable toxicity or limited efficacy. The use of epigenetic-targeting therapies after a significant interval following initial cancer therapy could potentially reduce the toxicity of combination strategies, and possibly exploit essential epigenetic states following therapy exposure. This review examines the feasibility of targeting epigenetic mechanisms using a sequential approach to eliminate residual therapy-arrested populations, that might possibly prevent recovery and disease recurrence.

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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.
期刊最新文献
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