Literature DB >> 29311237

Evaluation of CpxRA as a Therapeutic Target for Uropathogenic Escherichia coli Infections.

Lana Dbeibo1, Julia J van Rensburg2, Sara N Smith3, Kate R Fortney2, Dharanesh Gangaiah2, Hongyu Gao4, Juan Marzoa3,5, Yunlong Liu4, Harry L T Mobley3, Stanley M Spinola6,2,7.   

Abstract

CpxRA is an envelope stress response system found in all members of the family Enterobacteriaceae; CpxA has kinase activity for CpxR and phosphatase activity for phospho-CpxR, a transcription factor. CpxR also accepts phosphate groups from acetyl phosphate, a glucose metabolite. Activation of CpxR increases the transcription of genes encoding membrane repair and downregulates virulence determinants. We hypothesized that activation of CpxR could serve as an antimicrobial/antivirulence strategy and discovered compounds that activate CpxR in Escherichia coli by inhibiting CpxA phosphatase activity. As a prelude to testing such compounds in vivo, here we constructed cpxA (in the presence of glucose, CpxR is activated because of a lack of CpxA phosphatase) and cpxR (system absent) deletion mutants of uropathogenic E. coli (UPEC) CFT073. By RNA sequencing, few transcriptional differences were noted between the cpxR mutant and its parent, but in the cpxA mutant, several UPEC virulence determinants were downregulated, including the fim and pap operons, and it exhibited reduced mannose-sensitive hemagglutination of guinea pig red blood cells in vitro In competition experiments with mice, both mutants were less fit than the parent in the urine, bladder, and kidney; these fitness defects were complemented in trans Unexpectedly, in single-strain challenges, only the cpxA mutant was attenuated for virulence in the kidney but not in the bladder or urine. For the cpxA mutant, this may be due to the preferential use of amino acids over glucose as a carbon source in the bladder and urine by UPEC. These studies suggest that CpxA phosphatase inhibitors may have some utility for treating complex urinary tract infections.
Copyright © 2018 American Society for Microbiology.

Entities:  

Keywords:  Escherichia coli; UPEC; antivirulence; cpxA; cpxR; cpxRA; uropathogenic; virulence determinants

Mesh:

Substances:

Year:  2018        PMID: 29311237      PMCID: PMC5820967          DOI: 10.1128/IAI.00798-17

Source DB:  PubMed          Journal:  Infect Immun        ISSN: 0019-9567            Impact factor:   3.441


  62 in total

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Journal:  Infect Immun       Date:  1999-12       Impact factor: 3.441

Review 2.  Everything old is new again: an update on current research on the Cpx envelope stress response.

Authors:  Tracy L Raivio
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3.  Expression of flagella is coincident with uropathogenic Escherichia coli ascension to the upper urinary tract.

Authors:  M Chelsea Lane; Christopher J Alteri; Sara N Smith; Harry L T Mobley
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4.  A Haemophilus ducreyi CpxR deletion mutant is virulent in human volunteers.

Authors:  Maria Labandeira-Rey; Dana Dodd; Kate R Fortney; Beth Zwickl; Barry P Katz; Diane M Janowicz; Stanley M Spinola; Eric J Hansen
Journal:  J Infect Dis       Date:  2011-06-15       Impact factor: 5.226

5.  In vivo dynamics of type 1 fimbria regulation in uropathogenic Escherichia coli during experimental urinary tract infection.

Authors:  N W Gunther; V Lockatell; D E Johnson; H L Mobley
Journal:  Infect Immun       Date:  2001-05       Impact factor: 3.441

6.  Both MisR (CpxR) and MisS (CpxA) Are Required for Neisseria gonorrhoeae Infection in a Murine Model of Lower Genital Tract Infection.

Authors:  Dharanesh Gangaiah; Erica L Raterman; Hong Wu; Kate R Fortney; Hongyu Gao; Yunlong Liu; Ann E Jerse; Stanley M Spinola
Journal:  Infect Immun       Date:  2017-08-18       Impact factor: 3.441

7.  Genetic analysis of activation of the Vibrio cholerae Cpx pathway.

Authors:  Leyla Slamti; Matthew K Waldor
Journal:  J Bacteriol       Date:  2009-06-19       Impact factor: 3.490

8.  Preferential use of central metabolism in vivo reveals a nutritional basis for polymicrobial infection.

Authors:  Christopher J Alteri; Stephanie D Himpsl; Harry L T Mobley
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9.  Mucosal immunization with iron receptor antigens protects against urinary tract infection.

Authors:  Christopher J Alteri; Erin C Hagan; Kelsey E Sivick; Sara N Smith; Harry L T Mobley
Journal:  PLoS Pathog       Date:  2009-09-18       Impact factor: 6.823

10.  Metabolic Requirements of Escherichia coli in Intracellular Bacterial Communities during Urinary Tract Infection Pathogenesis.

Authors:  Matt S Conover; Maria Hadjifrangiskou; Joseph J Palermo; Michael E Hibbing; Karen W Dodson; Scott J Hultgren
Journal:  mBio       Date:  2016-04-12       Impact factor: 7.867

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3.  First-generation structure-activity relationship studies of 2,3,4,9-tetrahydro-1H-carbazol-1-amines as CpxA phosphatase inhibitors.

Authors:  Yangxiong Li; Jessi J Gardner; Katherine R Fortney; Inga V Leus; Vincent Bonifay; Helen I Zgurskaya; Alexandre A Pletnev; Sheng Zhang; Zhong-Yin Zhang; Gordon W Gribble; Stanley M Spinola; Adam S Duerfeldt
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4.  The Yersinia pseudotuberculosis Cpx envelope stress system contributes to transcriptional activation of rovM.

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Journal:  Virulence       Date:  2019-12       Impact factor: 5.882

5.  The Cpx Stress Response Regulates Turnover of Respiratory Chain Proteins at the Inner Membrane of Escherichia coli.

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Review 6.  "Omics" Technologies - What Have They Told Us About Uropathogenic Escherichia coli Fitness and Virulence During Urinary Tract Infection?

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7.  CpxA Phosphatase Inhibitor Activates CpxRA and Is a Potential Treatment for Uropathogenic Escherichia coli in a Murine Model of Infection.

Authors:  Kate R Fortney; Sara N Smith; Julia J van Rensburg; Julie A Brothwell; Jessi J Gardner; Barry P Katz; Nagib Ahsan; Adam S Duerfeldt; Harry L T Mobley; Stanley M Spinola
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8.  Phosphatase activity of the control of virulence sensor kinase CovS is critical for the pathogenesis of group A streptococcus.

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9.  Comparative Transcriptome Analysis of Pseudomonas putida KT2440 Revealed Its Response Mechanisms to Elevated Levels of Zinc Stress.

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  9 in total

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