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酰基硫代缩氨基脲类似物的合成及抗朊病毒聚集活性。

Synthesis and anti-prion aggregation activity of acylthiosemicarbazide analogues.

机构信息

Department of Pharmacy and Institute of Pharmaceutical Science and Technology, Hanyang University ERICA campus, Ansan, Republic of Korea.

Division of Developmental Biology and Physiology, Department of Biotechnology, Sungshin University, Seoul, Korea.

出版信息

J Enzyme Inhib Med Chem. 2023 Dec;38(1):2191164. doi: 10.1080/14756366.2023.2191164.

Abstract

Prions are infectious protein particles known to cause prion diseases. The biochemical entity of the pathogen is the misfolded prion protein (PrP) that forms insoluble amyloids to impair brain function. PrP interacts with the non-pathogenic, cellular prion protein (PrP) and facilitates conversion into a nascent misfolded isoform. Several small molecules have been reported to inhibit the aggregation of PrP but no pharmacological intervention was well established thus far. We, here, report that acylthiosemicarbazides inhibit the prion aggregation. Compounds and showed almost perfect inhibition (EC = 5 µM) in prion aggregation formation assay. The activity was further confirmed by atomic force microscopy, semi-denaturing detergent agarose gel electrophoresis and real-time quaking induced conversion assay (EC = 0.9 and 2.8 µM, respectively). These compounds also disaggregated pre-existing aggregates and one of them decreased the level of PrP in cultured cells with permanent prion infection, suggesting their potential as a treatment platform. In conclusion, hydroxy-2-naphthoylthiosemicarbazides can be an excellent scaffold for the discovery of anti-prion therapeutics.

摘要

朊病毒是已知可引起朊病毒病的传染性蛋白颗粒。病原体的生化实体是错误折叠的朊病毒蛋白 (PrP),它形成不溶性淀粉样蛋白,从而损害大脑功能。PrP 与非致病性的细胞朊病毒蛋白 (PrP) 相互作用,并促进其转化为新生的错误折叠异构体。已经报道了几种小分子可以抑制 PrP 的聚集,但迄今为止尚未建立良好的药理学干预措施。在这里,我们报告说酰基硫代半卡巴腙抑制朊病毒的聚集。化合物 和 在朊病毒聚集形成试验中表现出几乎完美的抑制作用(EC=5µM)。原子力显微镜、半变性去污剂琼脂糖凝胶电泳和实时振动诱导转换试验进一步证实了这一活性(EC=0.9 和 2.8µM)。这些化合物还可以解聚预先存在的聚集体,其中一种化合物降低了永生化朊病毒感染培养细胞中的 PrP 水平,表明它们具有作为治疗平台的潜力。总之,羟基-2-萘甲酰基硫代半卡巴腙可以成为发现抗朊病毒治疗药物的极好支架。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2a02/10038035/97d43d889b3a/IENZ_A_2191164_F0001_B.jpg

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