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Epigenome engineering: new technologies for precision medicine

机译:表观群落工程:精密医学的新技术

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摘要

Chromatin adopts different configurations that are regulated by reversible covalent modifications, referred to as epigenetic marks. Epigenetic inhibitors have been approved for clinical use to restore epigenetic aberrations that result in silencing of tumor-suppressor genes, oncogene addictions, and enhancement of immune responses. However, these drugs suffer from major limitations, such as a lack of locus selectivity and potential toxicities. Technological advances have opened a new era of precision molecular medicine to reprogram cellular physiology. The locus-specificity of CRISPR/dCas9/12a to manipulate the epigenome is rapidly becoming a highly promising strategy for personalized medicine. This review focuses on new state-of-the-art epigenome editing approaches to modify the epigenome of neoplasms and other disease models towards a more ‘normal-like state’, having characteristics of normal tissue counterparts. We highlight biomolecular engineering methodologies to assemble, regulate, and deliver multiple epigenetic effectors that maximize the longevity of the therapeutic effect, and we discuss limitations of the platforms such as targeting efficiency and intracellular delivery for future clinical applications.
机译:染色质采用不同的配置,其由可逆的共价修饰调节,称为表观遗传标记。表观遗传抑制剂已被批准用于临床用途,以恢复导致肿瘤抑制基因,癌基因成瘾和免疫应答的增强的表观遗传畸变。然而,这些药物患有主要限制,例如缺乏遗迹选择性和潜在毒性。技术进步开辟了一种新的精密分子药物的新时代,重新编程细胞生理学。 CRISPR / DCAS9 / 12A的轨迹特异性以操纵表观蛋白酶迅速成为个性化医学的高度有希望的策略。本综述侧重于新的最先进的外观蛋白酶编辑方法,以将肿瘤和其他疾病模型的外观蛋白酶朝向更常规的“正常状态”,具有正常组织对应物的特征。我们强调了生物分子工程方法来组装,调节和提供多种表观遗传效应,最大化治疗效果的寿命,并且我们讨论平台的局限性,例如针对未来的临床应用的靶向效率和细胞内递送。

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