Co-Inactivation of GlnR and CodY Regulators Impacts Pneumococcal Cell Wall Physiology

Co-Inactivation of GlnR and CodY Regulators Impacts Pneumococcal Cell Wall Physiology

CodY, a nutritional regulator highly conserved in low G+C Gram-positive bacteria, is essential in Streptococcus pneumoniae (the pneumococcus). A published codY mutant possessed suppressing mutations inactivating the fatC and amiC genes, respectively belonging to iron (Fat/Fec) and oligopeptide (Ami)...

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Veröffentlicht in:PloS one 2015-04, Vol.10 (4), p.e0123702-e0123702
Hauptverfasser: Johnston, Calum, Bootsma, Hester J, Aldridge, Christine, Manuse, Sylvie, Gisch, Nicolas, Schwudke, Dominik, Hermans, Peter W M, Grangeasse, Christophe, Polard, Patrice, Vollmer, Waldemar, Claverys, Jean-Pierre
Format: Artikel
Sprache:eng
Schlagworte:
Amidohydrolases - metabolism
Analysis
Antibiotics
Bacillus subtilis
Bacteria
Bacterial Proteins - genetics
Bacterial Proteins - metabolism
Biology
Biosynthesis
Cefotaxime
Cefotaxime - pharmacology
Cell Wall - drug effects
Cell Wall - metabolism
Cell walls
Chromosomes
Deactivation
Deoxyribonucleic acid
DNA
Efficiency
Electron microscopy
Enzymes
Genes
Genetic transformation
Glutamine
Gram-positive bacteria
Hydrolysis
Inactivation
Infectious diseases
Iron
Laboratories
Light levels
Lysozyme
Metabolism
Microscopy
Mutants
Mutation
Operons
Pathogens
Pediatrics
Peptidoglycans
Permease
Physiological aspects
Physiology
Pneumonia
Regulators
Staphylococcus aureus
Streptococcus infections
Streptococcus pneumoniae
Streptococcus pneumoniae - cytology
Streptococcus pneumoniae - drug effects
Streptococcus pneumoniae - genetics
Streptococcus pneumoniae - metabolism
Suppressors
Survival
Transformation, Genetic
Ultrastructure
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Zusammenfassung:CodY, a nutritional regulator highly conserved in low G+C Gram-positive bacteria, is essential in Streptococcus pneumoniae (the pneumococcus). A published codY mutant possessed suppressing mutations inactivating the fatC and amiC genes, respectively belonging to iron (Fat/Fec) and oligopeptide (Ami) ABC permease operons, which are directly repressed by CodY. Here we analyzed two additional published codY mutants to further explore the essentiality of CodY. We show that one, in which the regulator of glutamine/glutamate metabolism glnR had been inactivated by design, had only a suppressor in fecE (a gene in the fat/fec operon), while the other possessed both fecE and amiC mutations. Independent isolation of three different fat/fec suppressors thus establishes that reduction of iron import is crucial for survival without CodY. We refer to these as primary suppressors, while inactivation of ami, which is not essential for survival of codY mutants and acquired after initial fat/fec inactivation, can be regarded as a secondary suppressor. The availability of codY- ami+ cells allowed us to establish that CodY activates competence for genetic transformation indirectly, presumably by repressing ami which is known to antagonize competence. The glnR codY fecE mutant was then found to be only partially viable on solid medium and hypersensitive to peptidoglycan (PG) targeting agents such as the antibiotic cefotaxime and the muramidase lysozyme. While analysis of PG and teichoic acid composition uncovered no alteration in the glnR codY fecE mutant compared to wildtype, electron microscopy revealed altered ultrastructure of the cell wall in the mutant, establishing that co-inactivation of GlnR and CodY regulators impacts pneumococcal cell wall physiology. In light of rising levels of resistance to PG-targeting antibiotics of natural pneumococcal isolates, GlnR and CodY constitute potential alternative therapeutic targets to combat this debilitating pathogen, as co-inactivation of these regulators renders pneumococci sensitive to iron and PG-targeting agents.
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0123702