Literature DB >> 23002228

Upregulation of the phthiocerol dimycocerosate biosynthetic pathway by rifampin-resistant, rpoB mutant Mycobacterium tuberculosis.

Gregory P Bisson1, Carolina Mehaffy, Corey Broeckling, Jessica Prenni, Dalin Rifat, Desmond S Lun, Marcos Burgos, Drew Weissman, Petros C Karakousis, Karen Dobos.   

Abstract

Multidrug-resistant tuberculosis has emerged as a major threat to tuberculosis control. Phylogenetically related rifampin-resistant actinomycetes with mutations mapping to clinically dominant Mycobacterium tuberculosis mutations in the rpoB gene show upregulation of gene networks encoding secondary metabolites. We compared the expressed proteomes and metabolomes of two fully drug-susceptible clinical strains of M. tuberculosis (wild type) to those of their respective rifampin-resistant, rpoB mutant progeny strains with confirmed rifampin monoresistance following antitubercular therapy. Each of these strains was also used to infect gamma interferon- and lipopolysaccharide-activated murine J774A.1 macrophages to analyze transcriptional responses in a physiologically relevant model. Both rpoB mutants showed significant upregulation of the polyketide synthase genes ppsA-ppsE and drrA, which constitute an operon encoding multifunctional enzymes involved in the biosynthesis of phthiocerol dimycocerosate and other lipids in M. tuberculosis, but also of various secondary metabolites in related organisms, including antibiotics, such as erythromycin and rifamycins. ppsA (Rv2931), ppsB (Rv2932), and ppsC (Rv2933) were also found to be upregulated more than 10-fold in the Beijing rpoB mutant strain relative to its wild-type parent strain during infection of activated murine macrophages. In addition, metabolomics identified precursors of phthiocerol dimycocerosate, but not the intact molecule itself, in greater abundance in both rpoB mutant isolates. These data suggest that rpoB mutation in M. tuberculosis may trigger compensatory transcriptional changes in secondary metabolism genes analogous to those observed in related actinobacteria. These findings may assist in developing novel methods to diagnose and treat drug-resistant M. tuberculosis infections.

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Year:  2012        PMID: 23002228      PMCID: PMC3497527          DOI: 10.1128/JB.01013-12

Source DB:  PubMed          Journal:  J Bacteriol        ISSN: 0021-9193            Impact factor:   3.490


  74 in total

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4.  Rapid and spontaneous loss of phthiocerol dimycocerosate (PDIM) from Mycobacterium tuberculosis grown in vitro: implications for virulence studies.

Authors:  Pilar Domenech; Michael B Reed
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5.  Gene set enrichment analysis: a knowledge-based approach for interpreting genome-wide expression profiles.

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6.  Mapping and sequencing of mutations in the Escherichia coli rpoB gene that lead to rifampicin resistance.

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7.  Activation of antibiotic biosynthesis by specified mutations in the rpoB gene (encoding the RNA polymerase beta subunit) of Streptomyces lividans.

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Authors:  Zahoor Ahmad; Lee G Klinkenberg; Michael L Pinn; Mostafa M Fraig; Charles A Peloquin; William R Bishai; Eric L Nuermberger; Jacques H Grosset; Petros C Karakousis
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9.  Specific mutations in the Mycobacterium tuberculosis rpoB gene are associated with increased dnaE2 expression.

Authors:  Indra L Bergval; Paul R Klatser; Anja R J Schuitema; Linda Oskam; Richard M Anthony
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10.  Dormancy phenotype displayed by extracellular Mycobacterium tuberculosis within artificial granulomas in mice.

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Review 2.  Metabolomics: Applications and Promise in Mycobacterial Disease.

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3.  Biochemical Characterization of Isoniazid-resistant Mycobacterium tuberculosis: Can the Analysis of Clonal Strains Reveal Novel Targetable Pathways?

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Journal:  Mol Cell Proteomics       Date:  2018-05-29       Impact factor: 5.911

4.  In vitro and in vivo fitness costs associated with Mycobacterium tuberculosis RpoB mutation H526D.

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5.  Methods for Proteomic Analyses of Mycobacteria.

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Review 6.  Immunometabolism during Mycobacterium tuberculosis Infection.

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Journal:  Trends Microbiol       Date:  2020-05-11       Impact factor: 17.079

7.  Revisiting Protocols for the NMR Analysis of Bacterial Metabolomes.

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8.  Analysis of serum metabolic profile by ultra-performance liquid chromatography-mass spectrometry for biomarkers discovery: application in a pilot study to discriminate patients with tuberculosis.

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9.  Diphenylether-Modified 1,2-Diamines with Improved Drug Properties for Development against Mycobacterium tuberculosis.

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Journal:  ACS Infect Dis       Date:  2016-05-13       Impact factor: 5.084

10.  Rifampin Resistance Mutations Are Associated with Broad Chemical Remodeling of Mycobacterium tuberculosis.

Authors:  Nivedita Lahiri; Rupal R Shah; Emilie Layre; David Young; Chris Ford; Megan B Murray; Sarah M Fortune; D Branch Moody
Journal:  J Biol Chem       Date:  2016-05-10       Impact factor: 5.157

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