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靶向组蛋白甲基化用于癌症治疗:酶、抑制剂、生物学活性及前景

Targeting histone methylation for cancer therapy: enzymes, inhibitors, biological activity and perspectives.

作者信息

Song Yongcheng, Wu Fangrui, Wu Jingyu

机构信息

Department of Pharmacology, Baylor College of Medicine, 1 Baylor Plaza, Houston, TX, 77030, USA.

Dan L. Duncan Cancer Center, Baylor College of Medicine, 1 Baylor Plaza, Houston, TX, 77030, USA.

出版信息

J Hematol Oncol. 2016 Jun 17;9(1):49. doi: 10.1186/s13045-016-0279-9.

Abstract

Post-translational methylation of histone lysine or arginine residues plays important roles in gene regulation and other physiological processes. Aberrant histone methylation caused by a gene mutation, translocation, or overexpression can often lead to initiation of a disease such as cancer. Small molecule inhibitors of such histone modifying enzymes that correct the abnormal methylation could be used as novel therapeutics for these diseases, or as chemical probes for investigation of epigenetics. Discovery and development of histone methylation modulators are in an early stage and undergo a rapid expansion in the past few years. A number of highly potent and selective compounds have been reported, together with extensive preclinical studies of their biological activity. Several compounds have been in clinical trials for safety, pharmacokinetics, and efficacy, targeting several types of cancer. This review summarizes the biochemistry, structures, and biology of cancer-relevant histone methylation modifying enzymes, small molecule inhibitors and their preclinical and clinical antitumor activities. Perspectives for targeting histone methylation for cancer therapy are also discussed.

摘要

组蛋白赖氨酸或精氨酸残基的翻译后甲基化在基因调控和其他生理过程中发挥着重要作用。由基因突变、易位或过表达引起的异常组蛋白甲基化通常会导致诸如癌症等疾病的发生。能够纠正异常甲基化的此类组蛋白修饰酶的小分子抑制剂可作为这些疾病的新型治疗药物,或作为用于表观遗传学研究的化学探针。组蛋白甲基化调节剂的发现和开发尚处于早期阶段,并且在过去几年中迅速发展。已经报道了许多高效且选择性的化合物,以及对其生物活性的广泛临床前研究。有几种化合物已针对多种类型的癌症进行安全性、药代动力学和疗效的临床试验。本综述总结了与癌症相关的组蛋白甲基化修饰酶、小分子抑制剂及其临床前和临床抗肿瘤活性的生物化学、结构和生物学特性。还讨论了针对组蛋白甲基化进行癌症治疗的前景。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bb83/4912745/4920a20815b1/13045_2016_279_Fig1_HTML.jpg

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