AI Article Synopsis

  • The search for effective drugs against Mycobacterium tuberculosis faces challenges due to costly and time-consuming testing methods for both replicating and nonreplicating bacteria.
  • Researchers developed a new testing method called the charcoal agar resazurin assay (CARA), which allows for quicker and more efficient differentiation of bactericidal and bacteriostatic activities in antimycobacterial compounds.
  • Testing revealed that two known TB drugs, PA-824 (pretomanid) and TMC207 (bedaquiline), primarily exhibit bacteriostatic properties rather than bactericidal ones.

Article Abstract

The search for drugs that can kill replicating and nonreplicating Mycobacterium tuberculosis faces practical bottlenecks. Measurement of CFU and discrimination of bacteriostatic from bactericidal activity are costly in compounds, supplies, labor, and time. Testing compounds against M. tuberculosis under conditions that prevent the replication of M. tuberculosis often involves a second phase of the test in which conditions are altered to permit the replication of bacteria that survived the first phase. False-positive determinations of activity against nonreplicating M. tuberculosis may arise from carryover of compounds from the nonreplicating stage of the assay that act in the replicating stage. We mitigate these problems by carrying out a 96-well microplate liquid MIC assay and then transferring an aliquot of each well to a second set of plates in which each well contains agar supplemented with activated charcoal. After 7 to 10 days-about 2 weeks sooner than required to count CFU-fluorometry reveals whether M. tuberculosis bacilli in each well have replicated extensively enough to reduce a resazurin dye added for the final hour. This charcoal agar resazurin assay (CARA) distinguishes between bacterial biomasses in any two wells that differ by 2 to 3 log10 CFU. The CARA thus serves as a pretest and semiquantitative surrogate for longer, more laborious, and expensive CFU-based assays, helps distinguish bactericidal from bacteriostatic activity, and identifies compounds that are active under replicating conditions, nonreplicating conditions, or both. Results for 14 antimycobacterial compounds, including tuberculosis (TB) drugs, revealed that PA-824 (pretomanid) and TMC207 (bedaquiline) are largely bacteriostatic.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4576094PMC
http://dx.doi.org/10.1128/AAC.00803-15DOI Listing

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