Sharjah Institute for Medical Research, University of Sharjah, Sharjah, United Arab Emirates.
College of Pharmacy, University of Sharjah, Sharjah, United Arab Emirates.
Ann Med. 2023 Dec;55(1):2203946. doi: 10.1080/07853890.2023.2203946.
Altered epigenetic map is frequently observed in cancer and recent investigations have demonstrated a pertinent role of epigenetic modifications in the response to many anticancer drugs including the DNA damaging agents. Topoisomerase I (Top I) is a well-known nuclear enzyme that is critical for DNA function and cell survival and its inhibition causes DNA strand breaks and cell cycle arrest. Inhibitors of human Top I have proven to be a prosperous chemotherapeutic treatment for a vast number of cancer patients. While the treatment is efficacious in many cases, resistance and altered cellular response remain major therapeutic issues.
This review highlights the evidence available till date on the influence of different epigenetic modifications on the response to Top I inhibitors as well as the implications of targeting epigenetic alterations for improving the efficacy and safety of Top I inhibitors.
The field of epigenetic research is steadily growing. With its assistance, we could gain better understanding on how drug response and resistance work. Epigenetics can evolve as possible biomarkers and predictors of response to many medications including Top I inhibitors, and could have significant clinical implications that necessitate deeper attention.HIGHLIGHTSEpigenetic alterations, including DNA methylation and histone modifications, play a pertinent role in the response to several anticancer treatments, including DNA damaging agents like Top I inhibitors.Although camptothecin derivatives are used clinically as Top I inhibitors for management of cancer, certain types of cancer have inherent and or acquired resistance that limit the curative potential of them.Epigenetic modifications like DNA hypomethylation can either increase or decrease sensitivity to Top I inhibitors by different mechanisms.The combination of Top I inhibitors with the inhibitors of histone modifying enzymes can result in enhanced cytotoxic effects and sensitization of resistant cells to Top I inhibitors.MicroRNAs were found to directly influence the expression of Top I and other proteins in cancer cells resulting in positive or negative alteration of the response to Top I inhibitors.lncRNAs and their genetic polymorphisms have been found to be associated with Top I function and the response to its inhibitors.Clinical trials of epigenetic drugs in combination with Top I inhibitors are plentiful and some of them showed potentially promising outcomes.
在癌症中经常观察到表观遗传图谱的改变,最近的研究表明,表观遗传修饰在许多抗癌药物(包括 DNA 损伤剂)的反应中起着重要作用。拓扑异构酶 I(Top I)是一种众所周知的核酶,对 DNA 功能和细胞存活至关重要,其抑制作用会导致 DNA 链断裂和细胞周期停滞。人类 Top I 的抑制剂已被证明是为数众多的癌症患者的一种有前途的化疗治疗方法。虽然在许多情况下这种治疗是有效的,但耐药性和细胞反应改变仍然是主要的治疗问题。
本综述重点介绍了迄今为止关于不同表观遗传修饰对 Top I 抑制剂反应的影响的证据,以及针对表观遗传改变的靶向治疗对提高 Top I 抑制剂疗效和安全性的意义。
表观遗传研究领域正在稳步发展。有了它的帮助,我们可以更好地了解药物反应和耐药性的工作原理。表观遗传学可以作为许多药物(包括 Top I 抑制剂)反应和耐药性的可能生物标志物和预测因子,并具有重要的临床意义,需要引起更深入的关注。
表观遗传改变,包括 DNA 甲基化和组蛋白修饰,在包括 DNA 损伤剂如 Top I 抑制剂在内的几种抗癌治疗的反应中起着重要作用。
虽然喜树碱衍生物临床上被用作 Top I 抑制剂来治疗癌症,但某些类型的癌症具有内在的或获得性的耐药性,限制了它们的治疗潜力。
通过不同的机制,DNA 低甲基化等表观遗传修饰可以增加或降低对 Top I 抑制剂的敏感性。
Top I 抑制剂与组蛋白修饰酶抑制剂的联合使用可以导致细胞毒性作用增强,并使耐药细胞对 Top I 抑制剂敏感。
microRNAs 被发现可以直接影响癌细胞中 Top I 和其他蛋白质的表达,从而导致对 Top I 抑制剂反应的正向或负向改变。
lncRNAs 及其遗传多态性与 Top I 功能和对其抑制剂的反应有关。
有大量关于 Top I 抑制剂联合表观遗传药物的临床试验,其中一些显示出有希望的结果。
Zotero 插件
