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对盐孢菌素A介导的人20S蛋白酶体抑制作用的结构见解。

Structural insights into Salinosporamide A mediated inhibition of the human 20S proteasome.

作者信息

Sülzen Hagen, Fajtova Pavla, O'Donoghue Anthony J, Boura Evzen, Silhan Jan

机构信息

Institute of Organic Chemistry and Biochemistry AS CR, v.v.i., Flemingovo nam. 2., 166 10 Prague 6, Czech Republic.

Skaggs School of Pharmacy and Pharmaceutical Sciences, University of California San Diego, La Jolla, CA, 92037, USA.

出版信息

bioRxiv. 2025 Jan 28:2025.01.28.635221. doi: 10.1101/2025.01.28.635221.

Abstract

The 20S proteasome, a critical component of the ubiquitin-proteasome system, plays a central role in regulating protein degradation in eukaryotic cells. Marizomib (MZB), a natural γ-lactam-β-lactone compound derived from , is a potent 20S proteasome covalent inhibitor with demonstrated anticancer properties. Its broad-spectrum inhibition of all three proteasome subunits and ability to cross the blood-brain barrier has made it a promising therapeutic candidate for glioblastoma. Here, we present the cryo-EM structure of the human 20S proteasome in complex with MZB at 2.55 Å resolution. This structure reveals the binding mode of MZB to all six catalytic subunits within the two β-rings of the 20S proteasome, providing a detailed molecular understanding of its irreversible inhibitory mechanism. These findings explain the therapeutic potential of MZB at the molecular level and highlight marine-derived natural products in targeting the proteasome for anticancer treatment.

摘要

20S蛋白酶体是泛素-蛋白酶体系统的关键组成部分,在真核细胞中蛋白质降解调控方面发挥着核心作用。马里佐米布(MZB)是一种源自[具体来源未给出]的天然γ-内酰胺-β-内酯化合物,是一种具有抗癌特性的强效20S蛋白酶体共价抑制剂。它对所有三种蛋白酶体亚基的广谱抑制作用以及穿越血脑屏障的能力,使其成为胶质母细胞瘤颇具前景的治疗候选药物。在此,我们展示了人20S蛋白酶体与MZB复合物在2.55 Å分辨率下的冷冻电镜结构。该结构揭示了MZB与20S蛋白酶体两个β环内所有六个催化亚基的结合模式,为其不可逆抑制机制提供了详细的分子层面理解。这些发现从分子水平解释了MZB的治疗潜力,并突出了海洋来源天然产物在靶向蛋白酶体进行抗癌治疗方面的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e5a5/11838377/118a62d9d5ec/nihpp-2025.01.28.635221v1-f0001.jpg

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