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Identification of Novel Vacuolin-1 Analogues as Autophagy Inhibitors by Virtual Drug Screening and Chemical Synthesis

机译:通过虚拟药物筛选和化学合成鉴定新型Vacuolin-1类似物作为自噬抑制剂

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Autophagy is a fundamental cellular degradation process which is essential for cell homeostasis, and dysfunctional autophagy has been associated with a variety of human diseases, such as cancer. Several autophagy chemical modulators have been applied in a number of preclinical or clinical trials against these autophagy related diseases, especially cancer. Small molecule vacuolin-1 potently and reversibly inhibits both endosomal-lysosomal trafficking and autophagosome-lysosome fusion, yet the molecular mechanisms underlying vacuolin-1 mediated autophagy inhibition remain unknown. Here, we first performed the virtual drug screening and identified 14 vacuolin-1 analogues as autophagy inhibitors. Based on these virtual screening results, we further designed and synthesized 17 vacuolin-1 analogues, and found that 13 of them are autophagy inhibitors and a couple of them are as potent as vacuolin-1. In summary, these studies expanded the pool of useful autophagy inhibitors and reveal the structural-activity relationship of vacuolin-1 analogues, which is useful for future development of vacuolin-1 analogues with high potency and for identification of the molecular targets of vacuolin-1.
机译:自噬是细胞稳态的基本细胞降解过程,而自噬功能失调已与多种人类疾病(例如癌症)相关。在针对这些自噬相关疾病,特别是癌症的许多临床前或临床试验中,已经使用了几种自噬化学调节剂。小分子fluxlin-1有效且可逆地抑制内体-溶酶体运输和自噬体-溶酶体融合,但仍然未知的空泡蛋白-1介导的自噬抑制的分子机制。在这里,我们首先进行了虚拟药物筛选,并确定了14个vacuumlin-1类似物作为自噬抑制剂。基于这些虚拟的筛选结果,我们进一步设计和合成了17个vacuumlin-1类似物,发现其中13种是自噬抑制剂,其中有2种具有与vacuumlin-1一样的效力。总之,这些研究扩大了有用的自噬抑制剂的范围,并揭示了空泡蛋白-1类似物的结构-活性关系,这对于未来开发具有高效能的空泡蛋白-1类似物和鉴定空泡蛋白-1的分子靶标很有用。 。

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