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首页> 外文期刊>ACS Chemical Biology >Boc(3)Arg-Linked Ligands Induce Degradation by Localizing Target Proteins to the 20S Proteasome
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Boc(3)Arg-Linked Ligands Induce Degradation by Localizing Target Proteins to the 20S Proteasome

机译:Boc(3)Arg链接的配体通过本地化目标蛋白到20S蛋白酶体诱导降解。

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摘要

Targeted protein degradation is a promising strategy for drug design and functional assessment. Several small molecule approaches have been developed that localize target proteins to ubiquitin ligases, inducing ubiquitination and subsequent degradation by the 26S proteasome. We discovered that the degradation of a target protein can also be induced by a recognition ligand linked to tert-butyl carbamate (Boc(3))-protected arginine (B(3)A). Here, we show that this process requires the proteasome but does not involve ubiquitination of the target protein. B(3)A does not perturb the structure of the target protein; instead, a B(3)A-ligand stabilizes its target protein. B(3)A ligands stimulate activity of purified 20S proteasome, demonstrating that the tag binds directly to the 20S proteasome. Moreover, purified 20S proteasome is sufficient to degrade target proteins in the presence of their respective B(3)A-linked recognition ligands. These observations suggest a simple model for B(3)A-mediated degradation wherein the B(3)A tag localizes target proteins directly to the 20S proteasome. Thus, B(3)A ligands are the first example of a ubiquitin-free strategy for targeted protein degradation.
机译:靶向蛋白质降解是药物设计和功能评估的有前途的策略。已经开发了几种将靶蛋白定位于泛素连接酶,诱导泛素化并随后被26S蛋白酶体降解的小分子方法。我们发现目标蛋白的降解也可以由与氨基甲酸叔丁酯(Boc(3))保护的精氨酸(B(3)A)连接的识别配体诱导。在这里,我们表明该过程需要蛋白酶体,但不涉及靶蛋白的泛素化。 B(3)A不会干扰目标蛋白质的结构;相反,B(3)A配体可稳定其目标蛋白。 B(3)A配体刺激纯化的20S蛋白酶体的活性,表明标签直接与20S蛋白酶体结合。此外,纯化的20S蛋白酶体足以在它们各自的B(3)A连接的识别配体存在下降解目标蛋白。这些观察结果表明B(3)A介导的降解的简单模型,其中B(3)A标签将目标蛋白直接定位于20S蛋白酶体。因此,B(3)A配体是针对目标蛋白降解的无泛素策略的第一个实例。

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