Toxin-Antitoxin Systems in Pathogenic Bacteria

Bacterial toxin-antitoxin (TA) systems, which are ubiquitously present in bacterial genomes, are not essential for normal cell proliferation. The TA systems regulate fundamental cellular processes, facilitate survival under stress conditions, have essential roles in virulence and represent potential...

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Bibliographic Details
Other Authors:	Alonso, Juan Carlos (Editor)
Format:	Electronic Book Chapter
Language:	English
Published:	Basel, Switzerland MDPI - Multidisciplinary Digital Publishing Institute 2021
Subjects:	Medicine tuberculosis toxin-antitoxin systems bacterial cell death NAD+ stress-response toxin-antitoxin system mazF type II toxin mRNA interferase X-ray crystallography cognate interactions cross-interactions molecular insulation antitoxin TA systems addiction anti-addiction type I toxin-antitoxin system small protein toxin structure Fst/Ldr family toxin-antitoxin M. tuberculosis bacteria pathogenesis protein-protein interactions cross-talk protein interface tolerance persistence cross-resistance PemI/PemK Klebsiella pneumoniae toxin activation antibacterial agents bacterial persistence Stenotrophomonas maltophilia opportunistic pathogen clinical origin environmental origin biofilm antibiotic resistance cell wall inhibition nucleotide hydrolysis uridine diphosphate-N-acetylglucosamine n/a
Online Access:	DOAB: download the publication DOAB: description of the publication
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520			\|a Bacterial toxin-antitoxin (TA) systems, which are ubiquitously present in bacterial genomes, are not essential for normal cell proliferation. The TA systems regulate fundamental cellular processes, facilitate survival under stress conditions, have essential roles in virulence and represent potential therapeutic targets. These genetic TA loci are also shown to be involved in the maintenance of successful multidrug-resistant mobile genetic elements. The TA systems are classified as types I to VI, according to the nature of the antitoxin and to the mode of toxin inhibition. Type II TA systems encode a labile antitoxin and its stable toxin; degradation of the antitoxin renders a free toxin, which is bacteriostatic by nature. A free toxin generates a reversible state with low metabolic activity (quiescence) by affecting important functions of bacterial cells such as transcription, translation, DNA replication, replication and cell-wall synthesis, biofilm formation, phage predation, the regulation of nucleotide pool, etc., whereas antitoxins are toxin inhibitors. Under stress conditions, the TA systems might form networks. To understand the basis of the unique response of TA systems to stress, the prime causes of the emergence of drug-resistant strains, and their contribution to therapy failure and the development of chronic and recurrent infections, must be known in order to grasp how TA systems contribute to the mechanisms of phenotypic heterogeneity and pathogenesis that will enable the rational development of new treatments for infections caused by pathogens.
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650		7	\|a Medicine \|2 bicssc
653			\|a tuberculosis
653			\|a toxin-antitoxin systems
653			\|a bacterial cell death
653			\|a NAD+
653			\|a stress-response
653			\|a toxin-antitoxin system
653			\|a mazF
653			\|a type II
653			\|a toxin
653			\|a mRNA interferase
653			\|a X-ray crystallography
653			\|a cognate interactions
653			\|a cross-interactions
653			\|a molecular insulation
653			\|a antitoxin
653			\|a TA systems
653			\|a addiction
653			\|a anti-addiction
653			\|a type I toxin-antitoxin system
653			\|a small protein toxin structure
653			\|a Fst/Ldr family
653			\|a toxin-antitoxin
653			\|a M. tuberculosis
653			\|a bacteria
653			\|a pathogenesis
653			\|a protein-protein interactions
653			\|a cross-talk
653			\|a protein interface
653			\|a tolerance
653			\|a persistence
653			\|a cross-resistance
653			\|a toxin-antitoxin system
653			\|a PemI/PemK
653			\|a Klebsiella pneumoniae
653			\|a toxin-antitoxin systems
653			\|a toxin activation
653			\|a antibacterial agents
653			\|a bacterial persistence
653			\|a Stenotrophomonas maltophilia
653			\|a opportunistic pathogen
653			\|a clinical origin
653			\|a environmental origin
653			\|a biofilm
653			\|a antibiotic resistance
653			\|a cell wall inhibition
653			\|a nucleotide hydrolysis
653			\|a uridine diphosphate-N-acetylglucosamine
653			\|a n/a
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Toxin-Antitoxin Systems in Pathogenic Bacteria

MARC

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