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稳定的核糖核酸酶Y-RicT(YaaT)复合物的形成需要RicA(YmcA)和RicF(YlbF)。

Formation of a stable RNase Y-RicT (YaaT) complex requires RicA (YmcA) and RicF (YlbF).

作者信息

Dubnau Eugenie, DeSantis Micaela, Dubnau David

机构信息

Public Health Research Institute, Rutgers University, 225 Warren Street, Newark, New Jersey, 07103, USA.

Department of Microbiology, Biochemistry and Molecular Genetics, New Jersey Medical School, Rutgers University, 225 Warren Street, Newark, New Jersey, 07103, USA.

出版信息

bioRxiv. 2023 May 23:2023.05.22.541740. doi: 10.1101/2023.05.22.541740.

Abstract

UNLABELLED

In , the RicT (YaaT), RicA (YmcA) and RicF (YlbF) proteins, which form a stable ternary complex, are needed together with RNase Y (Rny), to cleave and thereby stabilize several key transcripts encoding enzymes of intermediary metabolism. We show here that RicT, but not RicA or RicF, forms a stable complex with Rny, and that this association requires the presence of RicA and RicF. We propose that RicT is handed off from the ternary complex to Rny. We show further that the two iron-sulfur clusters carried by the ternary Ric complex are required for the formation of the stable RicT-Rny complex. We demonstrate that proteins of the degradosome-like network of , which also interact with Rny, are dispensable for processing of the operon. Thus, Rny participates in distinct RNA-related processes, determined by its binding partners, and a RicT-Rny complex is likely the functional entity for mRNA maturation.

IMPORTANCE

The action of nucleases on RNA is universal and essential for all forms of life and includes processing steps that lead to the mature and functional forms of certain transcripts. In it has been shown that key transcripts for energy producing steps of glycolysis, for nitrogen assimilation and for oxidative phosphorylation, all of them crucial processes of intermediary metabolism, are cleaved at specific locations, resulting in mRNA stabilization. The proteins required for these cleavages in (Rny (RNase Y), RicA (YmcA), RicF (YlbF) and RicT (YaaT)) are broadly conserved among the firmicutes, including in several important pathogens, hinting that regulatory mechanisms they control may also be conserved. Several aspects of these regulatory events have been explored: phenotypes associated with the absence of these proteins have been described, the impact of these absences on the transcriptome has been documented, and there has been significant exploration of the biochemistry and structural biology of Rny and the Ric proteins. The present study further advances our understanding of the association of Ric proteins and Rny and shows that a complex of Rny with RicT is probably the entity that carries out mRNA maturation.

摘要

未标记

在[具体物种或环境]中,形成稳定三元复合物的RicT(YaaT)、RicA(YmcA)和RicF(YlbF)蛋白,需要与核糖核酸酶Y(Rny)一起,来切割并稳定几种编码中间代谢酶的关键转录本。我们在此表明,RicT而非RicA或RicF与Rny形成稳定复合物,且这种结合需要RicA和RicF的存在。我们提出RicT从三元复合物传递给Rny。我们进一步表明,三元Ric复合物携带的两个铁硫簇对于稳定的RicT - Rny复合物的形成是必需的。我们证明,[具体物种或环境]中类似降解体网络的蛋白,它们也与Rny相互作用,对于[具体操纵子名称]操纵子的加工是可有可无的。因此,Rny参与由其结合伙伴决定的不同RNA相关过程,并且RicT - Rny复合物可能是[具体物种或环境]mRNA成熟的功能实体。

重要性

核酸酶对RNA的作用是普遍的,对所有生命形式都至关重要,包括导致某些转录本成熟和功能形式的加工步骤。在[具体物种或环境]中已表明,糖酵解能量产生步骤、氮同化和氧化磷酸化的关键转录本,所有这些都是中间代谢的关键过程,在特定位置被切割,从而导致mRNA稳定。[具体物种或环境]中这些切割所需的蛋白(Rny(核糖核酸酶Y)、RicA(YmcA)、RicF(YlbF)和RicT(YaaT))在厚壁菌门中广泛保守,包括在几种重要病原体中,这暗示它们所控制的调控机制可能也保守。这些调控事件的几个方面已被探索:已描述了与这些蛋白缺失相关的表型,记录了这些缺失对转录组的影响,并且对Rny和Ric蛋白的生物化学和结构生物学进行了大量探索。本研究进一步推进了我们对Ric蛋白与Rny关联的理解,并表明Rny与RicT的复合物可能是进行mRNA成熟的实体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/32b9/10245838/39501e4de035/nihpp-2023.05.22.541740v1-f0001.jpg

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