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用于研究肌醇焦磷酸结构和功能的化学工具。

Chemical tools for interrogating inositol pyrophosphate structure and function.

机构信息

Princeton University, Frick Chemistry Laboratory, Washington Road, Princeton, NJ 08544, USA and Leibniz-Institut für Molekulare Pharmakologie, Robert-Rössle-Str 10, 13125 Berlin, Berlin, Germany.

出版信息

Chem Soc Rev. 2016 Nov 7;45(22):6311-6326. doi: 10.1039/c6cs00193a.

Abstract

The inositol pyrophosphates (PP-InsPs) are a unique group of intracellular messengers that represent some of the most highly phosphorylated molecules in nature. Genetic perturbation of the PP-InsP biosynthetic network indicates a central role for these metabolites in maintaining cellular energy homeostasis and in controlling signal transduction networks. However, despite their discovery over two decades ago, elucidating their physiologically relevant isomers, the biochemical pathways connecting these molecules to their associated phenotypes, and their modes of signal transduction has often been stymied by technical challenges. Many of the advances in understanding these molecules to date have been facilitated by the total synthesis of the various PP-InsP isomers and by the development of new methods that are capable of identifying their downstream signalling partners. Chemical tools have also been developed to distinguish between the proposed PP-InsP signal transduction mechanisms: protein binding, and a covalent modification of proteins termed protein pyrophosphorylation. In this article, we review these recent developments, discuss how they have helped to illuminate PP-InsP structure and function, and highlight opportunities for future discovery.

摘要

肌醇六磷酸(PP-InsPs)是一组独特的细胞内信使,它们代表了自然界中一些磷酸化程度最高的分子。对 PP-InsP 生物合成网络的遗传干扰表明,这些代谢物在维持细胞能量平衡和控制信号转导网络方面发挥着核心作用。然而,尽管它们在二十多年前被发现,但阐明其生理相关的异构体、将这些分子与其相关表型联系起来的生化途径,以及它们的信号转导方式,常常受到技术挑战的阻碍。迄今为止,许多对这些分子的理解进展都是通过各种 PP-InsP 异构体的全合成以及能够识别其下游信号伙伴的新方法的发展来实现的。化学工具也被开发出来,以区分所提出的 PP-InsP 信号转导机制:蛋白质结合和蛋白质的共价修饰,即蛋白质焦磷酸化。在本文中,我们回顾了这些最新的发展,讨论了它们如何帮助阐明 PP-InsP 的结构和功能,并强调了未来发现的机会。

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