Kutz Craig J, Holshouser Steven L, Marrow Ethan A, Woster Patrick M
Department of Drug Discovery and Biomedical Sciences, College of Pharmacy, Medical University of South Carolina, 70 President St., Charleston, SC 29425.
Medchemcomm. 2014 Dec;5(12):1863-1870. doi: 10.1039/C4MD00283K.
The chromatin remodeling amine oxidase lysine-specific demethylase 1 (LSD1) has become an attractive target for the design of specific inhibitors with therapeutic potential. We, and others, have described LSD1 inhibitors that have potential as antitumor agents. Many of the currently known LSD1 inhibitors are poor drug candidates, or are structurally based on the tranylcypromine backbone, thus increasing the potential for off-target effects mediated by other amine oxidases. We now describe a series of potent LSD1 inhibitors based on a novel 1,2,4-triazole scaffold; these inhibitors show a high degree of specificity for LSD1 in vitro, and cause increases in cellular histone 3 dimethyllysine 4 (H3K4me2), a gene transcription activating mark. Importantly, these inhibitors are not toxic to mammalian cells in vitro, and thus they may show utility in the treatment of epigenetically-based diseases where cell death is not a desired endpoint Figure 1. Structures of LSD1 inhibitors , verlindamycin , (bis)thioureas , amidoxime , cyclic peptide , N-(2-chloro-6-phenoxybenzyl)-4H-1,2,4-triazole-3,5-diamine and N,N-bis(2-methoxybenzyl)-1H-1,2,4-triazole-3,5-diamine .
染色质重塑胺氧化酶赖氨酸特异性去甲基化酶1(LSD1)已成为设计具有治疗潜力的特异性抑制剂的一个有吸引力的靶点。我们和其他人已经描述了具有抗肿瘤药物潜力的LSD1抑制剂。目前已知的许多LSD1抑制剂都是不理想的候选药物,或者其结构基于反苯环丙胺骨架,因此增加了由其他胺氧化酶介导的脱靶效应的可能性。我们现在描述了一系列基于新型1,2,4 - 三唑支架的强效LSD1抑制剂;这些抑制剂在体外对LSD1表现出高度特异性,并导致细胞组蛋白3二甲基赖氨酸4(H3K4me2)增加,这是一种基因转录激活标记。重要的是,这些抑制剂在体外对哺乳动物细胞无毒,因此它们可能在治疗不以细胞死亡为预期终点的表观遗传疾病中显示出效用 图1. LSD1抑制剂、维林达霉素、(双)硫脲、偕胺肟、环肽、N-(2-氯-6-苯氧基苄基)-4H-1,2,4-三唑-3,5-二胺和N,N-双(2-甲氧基苄基)-1H-1,2,4-三唑-3,5-二胺的结构。
