Experimental measurement and computational prediction of bacterial Hanks-type Ser/Thr signaling system regulatory targets.

IF 2.6 2区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY Molecular Microbiology Pub Date : 2024-08-01 Epub Date: 2024-01-03 DOI:10.1111/mmi.15220
Noam Grunfeld, Erel Levine, Elizabeth Libby
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Abstract

Bacteria possess diverse classes of signaling systems that they use to sense and respond to their environments and execute properly timed developmental transitions. One widespread and evolutionarily ancient class of signaling systems are the Hanks-type Ser/Thr kinases, also sometimes termed "eukaryotic-like" due to their homology with eukaryotic kinases. In diverse bacterial species, these signaling systems function as critical regulators of general cellular processes such as metabolism, growth and division, developmental transitions such as sporulation, biofilm formation, and virulence, as well as antibiotic tolerance. This multifaceted regulation is due to the ability of a single Hanks-type Ser/Thr kinase to post-translationally modify the activity of multiple proteins, resulting in the coordinated regulation of diverse cellular pathways. However, in part due to their deep integration with cellular physiology, to date, we have a relatively limited understanding of the timing, regulatory hierarchy, the complete list of targets of a given kinase, as well as the potential regulatory overlap between the often multiple kinases present in a single organism. In this review, we discuss experimental methods and curated datasets aimed at elucidating the targets of these signaling pathways and approaches for using these datasets to develop computational models for quantitative predictions of target motifs. We emphasize novel approaches and opportunities for collecting data suitable for the creation of new predictive computational models applicable to diverse species.

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细菌汉克斯型 Ser/Thr 信号系统调控目标的实验测量和计算预测。
细菌拥有多种多样的信号系统,它们利用这些系统来感知和响应环境,并适时地进行发育转换。汉克斯(Hanks)型丝氨酸/半胱氨酸激酶是一类广泛存在且进化历史悠久的信号系统,由于与真核激酶同源,有时也被称为 "类真核 "激酶。在不同的细菌物种中,这些信号系统是一般细胞过程(如新陈代谢、生长和分裂)、发育转换(如孢子形成、生物膜形成和毒力)以及抗生素耐受性的关键调节因子。这种多方面的调控是由于单个汉克斯型 Ser/Thr 激酶能够在翻译后改变多个蛋白质的活性,从而协调调控不同的细胞通路。然而,部分由于激酶与细胞生理学的深度结合,迄今为止,我们对特定激酶的作用时机、调控层次、靶标的完整列表以及单个生物体中通常存在的多个激酶之间的潜在调控重叠的了解相对有限。在这篇综述中,我们讨论了旨在阐明这些信号通路靶标的实验方法和数据集,以及利用这些数据集开发定量预测靶标图案的计算模型的方法。我们强调了收集数据的新方法和机会,这些数据适合创建适用于不同物种的新预测计算模型。
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
Molecular Microbiology
Molecular Microbiology 生物-生化与分子生物学
CiteScore
7.20
自引率
5.60%
发文量
132
审稿时长
1.7 months
期刊介绍: Molecular Microbiology, the leading primary journal in the microbial sciences, publishes molecular studies of Bacteria, Archaea, eukaryotic microorganisms, and their viruses. Research papers should lead to a deeper understanding of the molecular principles underlying basic physiological processes or mechanisms. Appropriate topics include gene expression and regulation, pathogenicity and virulence, physiology and metabolism, synthesis of macromolecules (proteins, nucleic acids, lipids, polysaccharides, etc), cell biology and subcellular organization, membrane biogenesis and function, traffic and transport, cell-cell communication and signalling pathways, evolution and gene transfer. Articles focused on host responses (cellular or immunological) to pathogens or on microbial ecology should be directed to our sister journals Cellular Microbiology and Environmental Microbiology, respectively.
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