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利用活性位点突变设计 AAA 蛋白 spastin 的化学抑制剂。

Designing a chemical inhibitor for the AAA protein spastin using active site mutations.

机构信息

Laboratory of Chemistry and Cell Biology, The Rockefeller University, New York, NY, USA.

Tri-Institutional PhD program in Chemical Biology, The Rockefeller University, New York, NY, USA.

出版信息

Nat Chem Biol. 2019 May;15(5):444-452. doi: 10.1038/s41589-019-0225-6. Epub 2019 Feb 18.

Abstract

Spastin is a microtubule-severing AAA (ATPases associated with diverse cellular activities) protein needed for cell division and intracellular vesicle transport. Currently, we lack chemical inhibitors to probe spastin function in such dynamic cellular processes. To design a chemical inhibitor of spastin, we tested selected heterocyclic scaffolds against wild-type protein and constructs with engineered mutations in the nucleotide-binding site that do not substantially disrupt ATPase activity. These data, along with computational docking, guided improvements in compound potency and selectivity and led to spastazoline, a pyrazolyl-pyrrolopyrimidine-based cell-permeable probe for spastin. These studies also identified spastazoline-resistance-conferring point mutations in spastin. Spastazoline, along with the matched inhibitor-sensitive and inhibitor-resistant cell lines we generated, were used in parallel experiments to dissect spastin-specific phenotypes in dividing cells. Together, our findings suggest how chemical probes for AAA proteins, along with inhibitor resistance-conferring mutations, can be designed and used to dissect dynamic cellular processes.

摘要

痉挛蛋白是一种微管切割 AAA(与多种细胞活动相关的 ATP 酶)蛋白,对于细胞分裂和细胞内囊泡运输是必需的。目前,我们缺乏化学抑制剂来研究痉挛蛋白在这些动态细胞过程中的功能。为了设计痉挛蛋白的化学抑制剂,我们测试了选定的杂环支架对野生型蛋白和在核苷酸结合位点进行工程改造的构建体的抑制作用,这些突变不会显著破坏 ATP 酶活性。这些数据,以及计算对接,指导了化合物效力和选择性的改进,并导致了 spastazoline 的产生,这是一种基于吡唑基-吡咯并嘧啶的、可渗透细胞的痉挛蛋白探针。这些研究还鉴定出了痉挛蛋白中的 spastazoline 抗性赋予突变。spastazoline 以及我们生成的匹配的抑制剂敏感和抑制剂抗性细胞系,被用于平行实验中以解析分裂细胞中的痉挛蛋白特异性表型。总之,我们的发现表明,如何设计和使用 AAA 蛋白的化学探针以及抑制剂抗性赋予突变,可以用于解析动态细胞过程。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6252/6558985/47e125c89f8c/nihms-1517346-f0001.jpg

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