Department of Microbiology, Hirszfeld Institute of Immunology and Experimental Therapy, Polish Academy of Sciences, Wrocław, Poland.
Department of Molecular Microbiology, Faculty of Biotechnology, University of Wrocław, Wrocław, Poland.
mSystems. 2024 Aug 20;9(8):e0078424. doi: 10.1128/msystems.00784-24. Epub 2024 Jul 9.
and are microaerobic food-borne human gastrointestinal pathogens that mainly cause diarrheal disease. These related species of the class face variable atmospheric environments during infection and transmission, ranging from nearly anaerobic to aerobic conditions. Consequently, their lifestyles require that both pathogens need to adjust their metabolism and respiration to the changing oxygen concentrations of the colonization sites. Our transcriptomic and proteomic studies revealed that and lacking a -specific regulatory protein, Cj1608, or a homolog, Abu0127, are unable to reprogram tricarboxylic acid cycle or respiration pathways, respectively, to produce ATP efficiently and, in consequence, adjust growth to changing oxygen supply. We propose that these energy and metabolism regulators (CemRs) are long-sought transcription factors controlling the metabolic shift related to oxygen availability, essential for these bacteria's survival and adaptation to the niches they inhabit. Besides their significant universal role in , CemRs, as pleiotropic regulators, control the transcription of many genes, often specific to the species, under microaerophilic conditions and in response to oxidative stress.
and are closely related pathogens that infect the human gastrointestinal tract. In order to infect humans successfully, they need to change their metabolism as nutrient and respiratory conditions change. A regulator called CemR has been identified, which helps them adapt their metabolism to changing conditions, particularly oxygen availability in the gastrointestinal tract so that they can produce enough energy for survival and spread. Without CemR, these bacteria, as well as a related species, , produce less energy, grow more slowly, or, in the case of , do not grow at all. Furthermore, CemR is a global regulator that controls the synthesis of many genes in each species, potentially allowing them to adapt to their ecological niches as well as establish infection. Therefore, the identification of CemR opens new possibilities for studying the pathogenicity of and .
和 是微需氧的食源性人类胃肠道病原体,主要引起腹泻疾病。这些 类的相关物种在感染和传播过程中面临着不同的大气环境,从几乎无氧到有氧条件不等。因此,它们的生活方式需要病原体调整其代谢和呼吸作用以适应定植部位不断变化的氧气浓度。我们的转录组学和蛋白质组学研究表明, 和 缺乏一种特定的调节蛋白 Cj1608 或同源物 Abu0127,分别无法重新编程三羧酸循环或呼吸途径,以有效地产生 ATP,因此无法调整生长以适应不断变化的氧气供应。我们提出,这些 能量和代谢调节剂(CemR)是长期以来寻找的控制与氧气可用性相关的代谢转变的转录因子,这对于这些细菌的生存和适应其栖息的小生境至关重要。除了在 中具有重要的普遍作用外,CemR 作为多效调节剂,还控制着微需氧条件下和氧化应激响应下许多基因的转录,这些基因通常是特定于物种的。
和 是密切相关的病原体,感染人类胃肠道。为了成功感染人类,它们需要改变新陈代谢,以适应营养和呼吸条件的变化。已经鉴定出一种名为 CemR 的调节剂,它有助于它们适应新陈代谢以适应变化的条件,特别是胃肠道中的氧气可用性,以便它们能够产生足够的能量来生存和传播。没有 CemR,这些细菌以及相关物种 ,产生的能量更少,生长更缓慢,或者在 的情况下根本无法生长。此外,CemR 是一种全局调节剂,控制每个物种中许多基因的合成,这可能使它们能够适应其生态小生境并建立感染。因此,CemR 的鉴定为研究 和 的致病性开辟了新的可能性。
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