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首页> 外文期刊>Journal of Medicinal Chemistry >Identification of SNAIL1 Peptide-Based Irreversible Lysine-Specific Demethylase 1-Selective Inactivators
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Identification of SNAIL1 Peptide-Based Irreversible Lysine-Specific Demethylase 1-Selective Inactivators

机译:基于SNAIL1肽的不可逆赖氨酸特异性脱甲基酶1-选择性失活剂的鉴定。

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摘要

Inhibition of lysine-specific demethylase 1 (LSD1), a flavin-dependent histone demethylase, has recently emerged as a new strategy for treating cancer and other diseases. LSD1 interacts physically with SNAIL]., a member of the SNAIL/SCRATCH family of transcription factors. This study describes the discovery of SNAIL1 peptide-based inactivators of LSD1. We designed and prepared SNAIL]. peptides bearing a propargyl amine, hydrazine, or phenylcyclopropane moiety. Among them, peptide 3, bearing hydrazine, displayed the most potent LSD1-inhibitory activity in enzyme assays. Kinetic study and mass spectrometric analysis indicated that peptide 3 is a mechanism based LSD1 inhibitor. Furthermore, peptides 37 and 38, which consist of cell membrane-permeable oligoarginine conjugated with peptide 3, induced a dose-dependent increase of dimethylated Lys4 of histone H3 in HeLa cells, suggesting that they are likely to exhibit LSD1-inhibitory activity intracellularly. In addition, peptide 37 decreased the viability of HeLa cells. We believe this new approach for targeting LSD1 provides a basis for development of potent selective inhibitors and biological probes for LSD1.
机译:抑制赖氨酸特异性脱甲基酶1(LSD1),一种黄素依赖性组蛋白脱甲基酶,最近已成为治疗癌症和其他疾病的新策略。 LSD1与SNAIL / SCRATCH转录因子家族的成员SNAIL物理相互作用。这项研究描述了基于SNAIL1肽的LSD1灭活剂的发现。我们设计并准备了SNAIL]。具有炔丙基胺,肼或苯基环丙烷部分的肽。其中,带有肼的肽3在酶测定中显示出最有效的LSD1抑制活性。动力学研究和质谱分析表明,肽3是一种基于LSD1抑制剂的机制。此外,由与膜3缀合的细胞膜可渗透性寡精氨酸组成的肽37和38诱导HeLa细胞中组蛋白H3的二甲基化Lys4剂量依赖性增加,表明它们很可能在细胞内表现出对LSD1的抑制活性。另外,肽37降低了HeLa细胞的活力。我们相信,这种针对LSD1的新方法为开发LSD1的有效选择性抑制剂和生物探针提供了基础。

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