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High Throughput Phenotypic Analysis of Mycobacterium tuberculosis and Mycobacterium bovis Strains' Metabolism Using Biolog Phenotype Microarrays

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  • Bhagwati Khatri
  • Mark Fielder
  • Gareth Jones
  • William Newell
  • Manal Abu-Oun
  • Paul R Wheeler

Abstract

Tuberculosis is a major human and animal disease of major importance worldwide. Genetically, the closely related strains within the Mycobacterium tuberculosis complex which cause disease are well-characterized but there is an urgent need better to understand their phenotypes. To search rapidly for metabolic differences, a working method using Biolog Phenotype MicroArray analysis was developed. Of 380 substrates surveyed, 71 permitted tetrazolium dye reduction, the readout over 7 days in the method. By looking for ≥5-fold differences in dye reduction, 12 substrates differentiated M. tuberculosis H37Rv and Mycobacterium bovis AF2122/97. H37Rv and a Beijing strain of M. tuberculosis could also be distinguished in this way, as could field strains of M. bovis; even pairs of strains within one spoligotype could be distinguished by 2 to 3 substrates. Cluster analysis gave three clear groups: H37Rv, Beijing, and all the M. bovis strains. The substrates used agreed well with prior knowledge, though an unexpected finding that AF2122/97 gave greater dye reduction than H37Rv with hexoses was investigated further, in culture flasks, revealing that hexoses and Tween 80 were synergistic for growth and used simultaneously rather than in a diauxic fashion. Potential new substrates for growth media were revealed, too, most promisingly N-acetyl glucosamine. Osmotic and pH arrays divided the mycobacteria into two groups with different salt tolerance, though in contrast to the substrate arrays the groups did not entirely correlate with taxonomic differences. More interestingly, these arrays suggested differences between the amines used by the M. tuberculosis complex and enteric bacteria in acid tolerance, with some hydrophobic amino acids being highly effective. In contrast, γ-aminobutyrate, used in the enteric bacteria, had no effect in the mycobacteria. This study proved principle that Phenotype MicroArrays can be used with slow-growing pathogenic mycobacteria and already has generated interesting data worthy of further investigation.

Suggested Citation

  • Bhagwati Khatri & Mark Fielder & Gareth Jones & William Newell & Manal Abu-Oun & Paul R Wheeler, 2013. "High Throughput Phenotypic Analysis of Mycobacterium tuberculosis and Mycobacterium bovis Strains' Metabolism Using Biolog Phenotype Microarrays," PLOS ONE, Public Library of Science, vol. 8(1), pages 1-15, January.
  • Handle: RePEc:plo:pone00:0052673
    DOI: 10.1371/journal.pone.0052673
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    References listed on IDEAS

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    1. Michael B. Reed & Pilar Domenech & Claudia Manca & Hua Su & Amy K. Barczak & Barry N. Kreiswirth & Gilla Kaplan & Clifton E. Barry, 2004. "A glycolipid of hypervirulent tuberculosis strains that inhibits the innate immune response," Nature, Nature, vol. 431(7004), pages 84-87, September.
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