TetR and OmpR family regulators in natural product biosynthesis and resistance.

IF 3.2 4区 生物学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY
Proteins-Structure Function and Bioinformatics Pub Date : 2025-01-01 Epub Date: 2023-10-24 DOI:10.1002/prot.26621
Rachit S Patil, Siddhant Sharma, Aditya V Bhaskarwar, Souparnika Nambiar, Niharika A Bhat, Mani Kanta Koppolu, Hussain Bhukya
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引用次数: 0

Abstract

This article provides a comprehensive review and sequence-structure analysis of transcription regulator (TR) families, TetR and OmpR/PhoB, involved in specialized secondary metabolite (SSM) biosynthesis and resistance. Transcription regulation is a fundamental process, playing a crucial role in orchestrating gene expression to confer a survival advantage in response to frequent environmental stress conditions. This process, coupled with signal sensing, enables bacteria to respond to a diverse range of intra and extracellular signals. Thus, major bacterial signaling systems use a receptor domain to sense chemical stimuli along with an output domain responsible for transcription regulation through DNA-binding. Sensory and output domains on a single polypeptide chain (one component system, OCS) allow response to stimuli by allostery, that is, DNA-binding affinity modulation upon signal presence/absence. On the other hand, two component systems (TCSs) allow cross-talk between the sensory and output domains as they are disjoint and transmit information by phosphorelay to mount a response. In both cases, however, TRs play a central role. Biosynthesis of SSMs, which includes antibiotics, is heavily regulated by TRs as it diverts the cell's resources towards the production of these expendable compounds, which also have clinical applications. These TRs have evolved to relay information across specific signals and target genes, thus providing a rich source of unique mechanisms to explore towards addressing the rapid escalation in antimicrobial resistance (AMR). Here, we focus on the TetR and OmpR family TRs, which belong to OCS and TCS, respectively. These TR families are well-known examples of regulators in secondary metabolism and are ubiquitous across different bacteria, as they also participate in a myriad of cellular processes apart from SSM biosynthesis and resistance. As a result, these families exhibit higher sequence divergence, which is also evident from our bioinformatic analysis of 158 389 and 77 437 sequences from TetR and OmpR family TRs, respectively. The analysis of both sequence and structure allowed us to identify novel motifs in addition to the known motifs responsible for TR function and its structural integrity. Understanding the diverse mechanisms employed by these TRs is essential for unraveling the biosynthesis of SSMs. This can also help exploit their regulatory role in biosynthesis for significant pharmaceutical, agricultural, and industrial applications.

天然产物生物合成和抗性中的TetR和OmpR家族调控因子。
本文对参与特异性次级代谢产物(SSM)生物合成和抗性的转录调节因子(TR)家族TetR和OmpR/PhoB进行了全面的综述和序列结构分析。转录调节是一个基本过程,在协调基因表达以在频繁的环境应激条件下获得生存优势方面发挥着至关重要的作用。这一过程,再加上信号传感,使细菌能够对多种细胞内和细胞外信号做出反应。因此,主要的细菌信号系统使用受体结构域来感知化学刺激,以及通过DNA结合负责转录调节的输出结构域。单个多肽链(单组分系统,OCS)上的感觉和输出结构域允许通过异源性对刺激做出反应,即在信号存在/不存在时进行DNA结合亲和力调节。另一方面,双组分系统(TCS)允许感觉域和输出域之间的串扰,因为它们是不相交的,并通过磷光体传输信息以产生响应。然而,在这两种情况下,TR都发挥着核心作用。包括抗生素在内的SSM的生物合成受到TR的严格调控,因为它将细胞的资源转移到这些消耗性化合物的生产上,这些化合物也有临床应用。这些TR已经进化为在特定信号和靶基因之间传递信息,从而为解决抗微生物耐药性(AMR)的快速升级提供了丰富的独特机制。在这里,我们重点关注TetR和OmpR家族TR,它们分别属于OCS和TCS。这些TR家族是次级代谢调节因子的众所周知的例子,在不同的细菌中普遍存在,因为除了SSM生物合成和抗性之外,它们还参与了无数的细胞过程。因此,这些家族表现出更高的序列差异,这从我们对158的生物信息学分析中也很明显 389和77 分别来自TetR和OmpR家族TR的437个序列。序列和结构的分析使我们能够识别出除了已知的负责TR功能及其结构完整性的基序之外的新基序。了解这些TR所采用的多种机制对于揭示SSM的生物合成至关重要。这也有助于利用它们在生物合成中的调节作用,用于重要的制药、农业和工业应用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Proteins-Structure Function and Bioinformatics
Proteins-Structure Function and Bioinformatics 生物-生化与分子生物学
CiteScore
5.90
自引率
3.40%
发文量
172
审稿时长
3 months
期刊介绍: PROTEINS : Structure, Function, and Bioinformatics publishes original reports of significant experimental and analytic research in all areas of protein research: structure, function, computation, genetics, and design. The journal encourages reports that present new experimental or computational approaches for interpreting and understanding data from biophysical chemistry, structural studies of proteins and macromolecular assemblies, alterations of protein structure and function engineered through techniques of molecular biology and genetics, functional analyses under physiologic conditions, as well as the interactions of proteins with receptors, nucleic acids, or other specific ligands or substrates. Research in protein and peptide biochemistry directed toward synthesizing or characterizing molecules that simulate aspects of the activity of proteins, or that act as inhibitors of protein function, is also within the scope of PROTEINS. In addition to full-length reports, short communications (usually not more than 4 printed pages) and prediction reports are welcome. Reviews are typically by invitation; authors are encouraged to submit proposed topics for consideration.
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