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首页> 外文期刊>European Journal of Medicinal Chemistry: Chimie Therapeutique >Novel electrophilic amides amenable by the Ugi reaction perturb thioredoxin system via thioredoxin reductase 1 (TrxR1) inhibition: Identification of DVD-445 as a new lead compound for anticancer therapy
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Novel electrophilic amides amenable by the Ugi reaction perturb thioredoxin system via thioredoxin reductase 1 (TrxR1) inhibition: Identification of DVD-445 as a new lead compound for anticancer therapy

机译:通过硫氧嗪还原酶1(TRXR1)抑制的UGI反应性肝细胞素系统的新型电泳酰胺促进氧化酰胺系统:鉴定DVD-445作为抗癌治疗的新型铅化合物

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A series of peptidomimetic compounds incorporating an electrophilic moiety was synthesized using the Ugi reaction. These compounds (termed the Ugi Michael acceptors or UMAs) were designed to target the selenocysteine catalytic residue of thioredoxin reductase 1 (TrxR1), a promising cancer target. The compounds were assessed for their potential to inhibit TrxR1 using human neuroblastoma (SH-SY5Y) cell lysate. Based on this initial screening, six compounds were selected for testing against recombinant rat TrxR1 and in the insulin assay to reveal low-micromolar to submicromolar potency of these inhibitors. The same frontrunner compounds were evaluated for their ability to exert antiproliferative activity and induce cell death and this activity was compared to the UMA effects on the levels of reactive oxygen and nitrogen species (RONS). Collectively, the UMA compounds class presented itself as a rich source of leads for TrxR1 inhibitor discovery for anticancer application. Compound 7 (DVD-445) was nominated a lead for further optimization. (C) 2019 Elsevier Masson SAS. All rights reserved.
机译:使用UGI反应合成含有电泳部分的一系列肽染色剂化合物。这些化合物(称为UGI Michael受体或UMAS)被设计用于靶向硫氧化酶还原酶1(TRXR1)的硒酰氯芹菜催化残基,这是一个有前途的癌症靶标。评估化合物的潜力以使用人神经母细胞瘤(SH-SY5Y)细胞裂解物抑制TRXR1。基于该初始筛选,选择六种化合物用于对重组大鼠TrxR1和胰岛素测定进行测试以显示低微粗大到这些抑制剂的亚微粒效力。评估相同的Frontrunner化合物,以促进抗增殖活性的能力,并诱导细胞死亡,并且将该活性与UMA对反应性氧和氮物质(rons)的影响进行比较。集体,UMA化合物阶级作为抗癌应用的TRXR1抑制剂发现的丰富源。提名化合物7(DVD-445)的铅以进一步优化。 (c)2019年Elsevier Masson SAS。版权所有。

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