The Campylobacter jejuni BumS sensor phosphatase detects the branched short-chain fatty acids isobutyrate and isovalerate as direct cues for signal transduction.

IF 5.1 1区 生物学 Q1 MICROBIOLOGY mBio Pub Date : 2025-02-05 Epub Date: 2024-12-13 DOI:10.1128/mbio.03278-24
Nestor Ruiz, Jiawei Xing, Igor B Zhulin, Chad A Brautigam, David R Hendrixson
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Abstract

Two-component signal transduction systems (TCSs) are nearly ubiquitous across bacterial species and enable bacteria to sense and respond to specific cues for environmental adaptation. The Campylobacter jejuni BumSR TCS is unusual in that the BumS sensor exclusively functions as a phosphatase rather than a kinase to control phosphorylated levels of its cognate BumR response regulator (P-BumR). We previously found that BumSR directs a response to the short-chain fatty acid butyrate generated by resident microbiota so that C. jejuni identifies ideal lower intestinal niches in avian and human hosts for colonization. However, butyrate is an indirect cue for BumS and did not inhibit in vitro BumS phosphatase activity for P-BumR. In this work, we expanded the repertoire of lower intestinal metabolites that are cues sensed by BumS that modulate the expression of genes required for colonization to include the branched short-chain fatty acids isobutyrate and isovalerate. Unlike butyrate, isobutyrate and isovalerate inhibited in vitro BumS phosphatase activity for P-BumR, indicating that these metabolites are direct cues for BumS. Isobutyrate and isovalerate reduced the thermostability of BumS and caused a reorganization of protein structure to suggest how sensing these cues inhibits phosphatase activity. We also identified residues in the BumS sensory domain required to detect isobutyrate, isovalerate, and butyrate and for optimal colonization of hosts to reveal how gut bacteria can recognize these intestinal metabolites. Our work reveals how this unusual bacterial sensor phosphatase senses a repertoire of intestinal metabolites and how cues alter BumSR signal transduction to influence C. jejuni colonization of hosts.IMPORTANCETCSs are prevalent in many bacteria, but the cues sensed by each are not actually known for many of these systems. Microbiota-generated butyrate in human and avian hosts is detected by the Campylobacter jejuni BumS sensor phosphatase so that the bacterium identifies ideal lower intestinal niches for colonization. However, BumS only indirectly senses butyrate to inhibit dephosphorylation of its cognate BumR response regulator. Here, we expanded the repertoire of cues sensed by BumS to the branched-short chain fatty acids isobutyrate and isovalerate that are also abundant in the lower intestines. Both isobutyrate and isovalerate are potent, direct cues for BumS, whereas butyrate is an indirect cue. Leveraging isobutyrate and isovalerate as direct cues, we reveal BumS structure is altered upon cue detection to inhibit its phosphatase activity. We provide an understanding of the mechanics of an unusual mode of signal transduction executed by BumSR and other bacterial sensor phosphatase-driven TCSs.

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空肠弯曲杆菌 BumS 传感器磷酸酶可检测到支链短链脂肪酸异丁酸酯和异戊酸酯,作为信号转导的直接线索。
双组分信号转导系统(TCSs)在细菌物种中几乎无处不在,使细菌能够感知和响应特定的环境适应信号。空肠弯曲杆菌BumSR TCS是不寻常的,因为BumS传感器仅作为磷酸酶而不是激酶来控制其同源BumR反应调节因子(P-BumR)的磷酸化水平。我们之前发现,BumSR对常驻微生物群产生的短链脂肪酸丁酸盐产生反应,从而使空肠梭菌在鸟类和人类宿主中确定理想的下肠道生态位进行定植。然而,丁酸盐是BumS的间接线索,并没有抑制体外BumS磷酸酶对P-BumR的活性。在这项工作中,我们扩大了下肠代谢物的范围,这些代谢物是BumS感知的调节定植所需基因表达的线索,包括支链短链脂肪酸异丁酸和异戊酸。与丁酸盐不同,异丁酸盐和异戊酸盐抑制了体外BumS磷酸酶对P-BumR的活性,表明这些代谢物是BumS的直接线索。异丁酸盐和异戊酸盐降低了BumS的热稳定性,并引起蛋白质结构的重组,这表明感知这些线索如何抑制磷酸酶活性。我们还鉴定了检测异丁酸、异戊酸和丁酸所需的BumS感觉结构域的残基,以及宿主的最佳定植,以揭示肠道细菌如何识别这些肠道代谢物。我们的工作揭示了这种不寻常的细菌传感器磷酸酶如何感知一系列肠道代谢物,以及线索如何改变BumSR信号转导从而影响空肠梭菌在宿主中的定植。重要性etcs在许多细菌中都很普遍,但它们所感知的线索实际上在许多细菌系统中并不为人所知。空肠弯曲杆菌(Campylobacter jejuni BumS)感应磷酸酶检测人类和禽类宿主微生物产生的丁酸盐,以便细菌确定理想的下肠道生态位进行定植。然而,BumS仅间接感知丁酸盐来抑制其同源BumR反应调节因子的去磷酸化。在这里,我们将bum感知的线索扩展到分支短链脂肪酸异丁酸和异戊酸,这两种脂肪酸也存在于下肠中。异丁酸盐和异戊酸盐都是有效的,直接提示bum,而丁酸盐是间接提示。利用异丁酸盐和异戊酸盐作为直接线索,我们发现在线索检测时,BumS的结构会发生改变,从而抑制其磷酸酶活性。我们提供了对BumSR和其他细菌传感器磷酸酶驱动的tcs执行的不寻常信号转导模式的机制的理解。
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来源期刊
mBio
mBio MICROBIOLOGY-
CiteScore
10.50
自引率
3.10%
发文量
762
审稿时长
1 months
期刊介绍: mBio® is ASM''s first broad-scope, online-only, open access journal. mBio offers streamlined review and publication of the best research in microbiology and allied fields.
期刊最新文献
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