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李斯特菌对 c-di-AMP 代谢失调的适应作用是其在渗透压适应中的作用基础,并确定了一种磷霉素摄取系统。

Adaptation of Listeria monocytogenes to perturbation of c-di-AMP metabolism underpins its role in osmoadaptation and identifies a fosfomycin uptake system.

机构信息

FG Synthetic Microbiology, Institute for Biotechnology, BTU Cottbus-Senftenberg, 01968, Senftenberg, Germany.

Department of General Microbiology, Institute for Microbiology and Genetics, University of Goettingen, 37077, Göttingen, Germany.

出版信息

Environ Microbiol. 2022 Sep;24(9):4466-4488. doi: 10.1111/1462-2920.16084. Epub 2022 Jun 10.

Abstract

The human pathogen Listeria monocytogenes synthesizes and degrades c-di-AMP using the diadenylate cyclase CdaA and the phosphodiesterases PdeA and PgpH respectively. c-di-AMP is essential because it prevents the uncontrolled uptake of osmolytes. Here, we studied the phenotypes of cdaA, pdeA, pgpH and pdeA pgpH mutants with defects in c-di-AMP metabolism and characterized suppressor mutants restoring their growth defects. The characterization of the pdeA pgpH mutant revealed that the bacteria show growth defects in defined medium, a phenotype that is invariably suppressed by mutations in cdaA. The previously reported growth defect of the cdaA mutant in rich medium is suppressed by mutations that osmotically stabilize the c-di-AMP-free strain. We also found that the cdaA mutant has an increased sensitivity against isoleucine. The isoleucine-dependent growth inhibition of the cdaA mutant is suppressed by codY mutations that likely reduce the DNA-binding activity of encoded CodY variants. Moreover, the characterization of the cdaA suppressor mutants revealed that the Opp oligopeptide transport system is involved in the uptake of the antibiotic fosfomycin. In conclusion, the suppressor analysis corroborates a key function of c-di-AMP in controlling osmolyte homeostasis in L. monocytogenes.

摘要

人类病原体李斯特菌分别使用二腺苷酸环化酶 CdaA、磷酸二酯酶 PdeA 和 PgpH 合成和降解 c-di-AMP。c-di-AMP 是必不可少的,因为它可以防止渗透物的不受控制摄取。在这里,我们研究了 c-di-AMP 代谢缺陷的 cdaA、pdeA、pgpH 和 pdeA pgpH 突变体的表型,并对恢复其生长缺陷的抑制突变体进行了特征描述。pdeA pgpH 突变体的特征表明,细菌在限定培养基中表现出生长缺陷,这种表型始终被 cdaA 突变抑制。先前报道的 cdaA 突变体在丰富培养基中的生长缺陷被渗透物稳定 c-di-AMP 无细胞系的突变所抑制。我们还发现 cdaA 突变体对异亮氨酸的敏感性增加。cdaA 突变体的异亮氨酸依赖性生长抑制被 codY 突变抑制,codY 突变可能降低编码 CodY 变体的 DNA 结合活性。此外,cdaA 抑制突变体的特征描述表明,Opp 寡肽转运系统参与了抗生素磷霉素的摄取。总之,抑制分析证实了 c-di-AMP 在控制李斯特菌中渗透物稳态方面的关键作用。

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