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泛素和类泛素激活酶形成警报素二腺苷三磷酸和四磷酸。

Formation of the Alarmones Diadenosine Triphosphate and Tetraphosphate by Ubiquitin- and Ubiquitin-like-Activating Enzymes.

机构信息

Department of Chemistry, Konstanz Research School Chemical Biology, University of Konstanz, Universitätsstrasse 10, 78464 Konstanz, Germany.

Department of Chemistry, Konstanz Research School Chemical Biology, University of Konstanz, Universitätsstrasse 10, 78464 Konstanz, Germany; Department of Biology, Konstanz Research School Chemical Biology, University of Konstanz, Universitätsstrasse 10, 78464 Konstanz, Germany.

出版信息

Cell Chem Biol. 2019 Nov 21;26(11):1535-1543.e5. doi: 10.1016/j.chembiol.2019.08.004. Epub 2019 Sep 3.

Abstract

Diadenosine polyphosphates (ApAs) such as diadenosine tri- and tetraphosphates are formed in prokaryotic as well as eukaryotic cells. Since upon stress intracellular ApA concentrations increase, it was postulated that ApAs are alarmones triggering stress-adaptive processes. The major synthesis pathway of ApAs is assumed to be a side reaction of amino acid activation. How this process is linked to stress adaptation remains enigmatic. The first step of one of the most prominent eukaryotic post-translational modification systems-the conjugation of ubiquitin (Ub) and ubiquitin-like proteins (Ubl) to target proteins-involves the formation of an adenylate as intermediate. Like ApA formation, Ub and Ubl conjugation is significantly enhanced during stress conditions. Here, we demonstrate that diadenosine tri- and tetraphosphates are indeed synthesized during activation of Ub and Ubls. This links one of the most prevalent eukaryotic protein-modification systems to ApA formation for the first time.

摘要

双腺苷多磷酸盐(ApAs),如二腺苷三磷酸和四磷酸,在原核细胞和真核细胞中形成。由于在应激条件下细胞内 ApA 浓度增加,因此有人假设 ApAs 是引发应激适应过程的警报素。ApAs 的主要合成途径被认为是氨基酸激活的副反应。这个过程如何与应激适应相关仍然是个谜。最显著的真核后翻译修饰系统之一——泛素(Ub)和类泛素蛋白(Ubl)与靶蛋白的缀合的第一步——涉及到腺苷酸作为中间产物的形成。与 ApA 形成一样,Ub 和 Ubl 缀合在应激条件下显著增强。在这里,我们证明了在 Ub 和 Ubls 的激活过程中确实合成了二腺苷三磷酸和四磷酸。这是第一次将最普遍的真核蛋白修饰系统之一与 ApA 形成联系起来。

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