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蛇孢菌素A共价靶向复合物IV导致癌细胞线粒体代谢崩溃

Ophiobolin A Covalently Targets Complex IV Leading to Mitochondrial Metabolic Collapse in Cancer Cells.

作者信息

Gowans Flor A, Thach Danny Q, Wang Yangzhi, Altamirano Poblano Belen E, Dovala Dustin, Tallarico John A, McKenna Jeffrey M, Schirle Markus, Maimone Thomas J, Nomura Daniel K

机构信息

Department of Nutritional Sciences and Toxicology, University of California, Berkeley, Berkeley, CA 94720 USA.

Department of Chemistry, University of California, Berkeley, Berkeley, CA 94720 USA.

出版信息

bioRxiv. 2023 Mar 9:2023.03.09.531918. doi: 10.1101/2023.03.09.531918.

Abstract

Ophiobolin A (OPA) is a sesterterpenoid fungal natural product with broad anti-cancer activity. While OPA possesses multiple electrophilic moieties that can covalently react with nucleophilic amino acids on proteins, the proteome-wide targets and mechanism of OPA remain poorly understood in many contexts. In this study, we used covalent chemoproteomic platforms to map the proteome-wide reactivity of OPA in a highly sensitive lung cancer cell line. Among several proteins that OPA engaged, we focused on two targets-cysteine C53 of HIG2DA and lysine K72 of COX5A-that are part of complex IV of the electron transport chain and contributed significantly to the anti-proliferative activity. OPA activated mitochondrial respiration in a HIG2DA and COX5A-dependent manner, led to an initial spike in mitochondrial ATP, but then compromised mitochondrial membrane potential leading to ATP depletion. We have used chemoproteomic strategies to discover a unique anti-cancer mechanism of OPA through activation of complex IV leading to compromised mitochondrial energetics and rapid cell death.

摘要

蛇孢菌素A(OPA)是一种具有广泛抗癌活性的倍半萜类真菌天然产物。虽然OPA具有多个可与蛋白质上的亲核氨基酸发生共价反应的亲电基团,但在许多情况下,OPA的全蛋白质组靶点和作用机制仍知之甚少。在本研究中,我们使用共价化学蛋白质组学平台来绘制OPA在高敏感性肺癌细胞系中的全蛋白质组反应性。在OPA作用的几种蛋白质中,我们聚焦于两个靶点——HIG2DA的半胱氨酸C53和COX5A的赖氨酸K72,它们是电子传递链复合体IV的一部分,并且对其抗增殖活性有显著贡献。OPA以HIG2DA和COX5A依赖的方式激活线粒体呼吸,导致线粒体ATP最初激增,但随后线粒体膜电位受损,导致ATP耗竭。我们利用化学蛋白质组学策略,通过激活复合体IV导致线粒体能量代谢受损和细胞快速死亡,发现了OPA独特的抗癌机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/11f2/10029012/c653d61e11ff/nihpp-2023.03.09.531918v1-f0001.jpg

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