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蛋白质-配体相互作用在稀缺中:从细菌到后生动物的严格反应,以及未解决的问题。

Protein-Ligand Interactions in Scarcity: The Stringent Response from Bacteria to Metazoa, and the Unanswered Questions.

机构信息

EonBio, 3780 Pelham Drive, Mobile, AL 36619, USA.

出版信息

Int J Mol Sci. 2023 Feb 16;24(4):3999. doi: 10.3390/ijms24043999.

Abstract

The stringent response, originally identified in as a signal that leads to reprogramming of gene expression under starvation or nutrient deprivation, is now recognized as ubiquitous in all bacteria, and also as part of a broader survival strategy in diverse, other stress conditions. Much of our insight into this phenomenon derives from the role of hyperphosphorylated guanosine derivatives (pppGpp, ppGpp, pGpp; guanosine penta-, tetra- and tri-phosphate, respectively) that are synthesized on starvation cues and act as messengers or alarmones. These molecules, collectively referred to here as (p)ppGpp, orchestrate a complex network of biochemical steps that eventually lead to the repression of stable RNA synthesis, growth, and cell division, while promoting amino acid biosynthesis, survival, persistence, and virulence. In this analytical review, we summarize the mechanism of the major signaling pathways in the stringent response, consisting of the synthesis of the (p)ppGpp, their interaction with RNA polymerase, and diverse factors of macromolecular biosynthesis, leading to differential inhibition and activation of specific promoters. We also briefly touch upon the recently reported stringent-like response in a few eukaryotes, which is a very disparate mechanism involving MESH1 (Metazoan SpoT Homolog 1), a cytosolic NADPH phosphatase. Lastly, using ppGpp as an example, we speculate on possible pathways of simultaneous evolution of alarmones and their multiple targets.

摘要

严格响应最初在 中被鉴定为一种信号,可在饥饿或营养缺乏时导致基因表达的重编程,现在被认为在所有细菌中普遍存在,也是在各种其他胁迫条件下生存策略的一部分。我们对这一现象的认识很大程度上来自于磷酸化鸟苷衍生物(pppGpp、ppGpp、pGpp;鸟苷五、四、三磷酸,分别)的作用,这些衍生物在饥饿信号下合成,并作为信使或警报素发挥作用。这些分子在这里统称为(p)ppGpp,它们协调着一个复杂的生化步骤网络,最终导致稳定 RNA 合成、生长和细胞分裂的抑制,同时促进氨基酸生物合成、存活、持久和毒力。在这篇分析评论中,我们总结了严格响应中主要信号通路的机制,包括(p)ppGpp 的合成、它们与 RNA 聚合酶的相互作用以及大分子生物合成的各种因素,导致特定启动子的差异抑制和激活。我们还简要介绍了一些真核生物中最近报道的严格样反应,这是一种非常不同的机制,涉及 MESH1(后生动物 SpoT 同源物 1),一种细胞质 NADPH 磷酸酶。最后,我们以 ppGpp 为例,推测了警报素及其多个靶标的同时进化的可能途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7411/9965611/4b9f1705f0a1/ijms-24-03999-g001.jpg

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