Investigation of the potential role of toxin-antitoxin systems in virulence and antimicrobial resistance in some gram-negative bacteria / Shahira Abdelsalam Elbanna ; Nayera Ahmed Moneib , Ramy Karam Aziz , Reham Samir Mohamed

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Shahira Abdelsalam Elbanna

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TextLanguage: English Publication details: Cairo : Shahira Abdelsalam Elbanna , 2021Description: 77 P. : charts , facsimiles ; 25cmOther title:

التحقق من تأثير أنظمة السموم ومضاداتها على ضراوة البكتيريا سالبة الجرام ودورها فى مقاومة المضادات الحيوية [Added title page title]

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Dissertation note: Thesis (Ph.D.) - Cairo University - Faculty of Pharmacy - Department of Microbiology and Immunology Summary: Toxin-antitoxin (TA) systems are widespread among bacteria, archaea and fungi. They play different roles, such as postsegregational killing, abortive infection, and persister cell formation, and have recently been proposed as novel drug targets. TA systems are classified into six types (I-VI), based on the nature of antitoxin and its mode of action. This workaimed to screen the pathogen Acinetobacter baumannii, known for its alarming antimicrobial resistance, for TA systems, and to identify a CptBA-like Type IV TA, one of the least characterized systems. Comparative genomics demonstrated the distribution of E. coliCptBA-like systems among Gram-negative bacteria, while phylogenetic analysis of CptA and CptBdelineated two major groups, in each of which Acinetobacter spp. clustered together. Multiple sequence alignment indicated the conservation of cptA and cptB in 195 strains of A. baumannii in the same syntenic order. Using A. baumannii recombinant cptA and cptB, cloned under different promoters, confirmed thetoxin-antitoxin nature of their encoded proteins, as cptB expression was able to reverse growth inhibition by CptA in a dose-time-dependent manner.Furthermore, transcriptional analysis of cptBA in its natural bacterial host (A. baumannii) demonstrated that the cptBA locus is actively co-transcribed under normal conditions; yet, their transcriptional levels were reduced under oxidative and antibiotic stress, including ciprofloxacin and meropenem

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Item type	Current library	Home library	Call number	Copy number	Status	Date due	Barcode
Thesis	قاعة الرسائل الجامعية - الدور الاول	المكتبة المركزبة الجديدة - جامعة القاهرة	Cai01.08.06.Ph.D.2021.Sh.I (Browse shelf(Opens below))		Not for loan		01010110083020000
CD - Rom	مخـــزن الرســائل الجـــامعية - البدروم	المكتبة المركزبة الجديدة - جامعة القاهرة	Cai01.08.06.Ph.D.2021.Sh.I (Browse shelf(Opens below))	83020.CD	Not for loan		01020110083020000

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Thesis (Ph.D.) - Cairo University - Faculty of Pharmacy - Department of Microbiology and Immunology

Toxin-antitoxin (TA) systems are widespread among bacteria, archaea and fungi. They play different roles, such as postsegregational killing, abortive infection, and persister cell formation, and have recently been proposed as novel drug targets. TA systems are classified into six types (I-VI), based on the nature of antitoxin and its mode of action. This workaimed to screen the pathogen Acinetobacter baumannii, known for its alarming antimicrobial resistance, for TA systems, and to identify a CptBA-like Type IV TA, one of the least characterized systems. Comparative genomics demonstrated the distribution of E. coliCptBA-like systems among Gram-negative bacteria, while phylogenetic analysis of CptA and CptBdelineated two major groups, in each of which Acinetobacter spp. clustered together. Multiple sequence alignment indicated the conservation of cptA and cptB in 195 strains of A. baumannii in the same syntenic order. Using A. baumannii recombinant cptA and cptB, cloned under different promoters, confirmed thetoxin-antitoxin nature of their encoded proteins, as cptB expression was able to reverse growth inhibition by CptA in a dose-time-dependent manner.Furthermore, transcriptional analysis of cptBA in its natural bacterial host (A. baumannii) demonstrated that the cptBA locus is actively co-transcribed under normal conditions; yet, their transcriptional levels were reduced under oxidative and antibiotic stress, including ciprofloxacin and meropenem

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