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Tuberculosis drug discovery in the post-post-genomic era

Journal

EMBO MOLECULAR MEDICINE
Volume 6, Issue 2, Pages 158-168

Publisher

WILEY
DOI: 10.1002/emmm.201201772

Keywords

drug candidates; drug discovery; genomics; screening; tuberculosis

Funding

  1. Fondation Jacqueline Beytout
  2. German Federal Ministry of Research and Education (BMBF) [01KI1017]
  3. European Community [260872]

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The expectation that genomics would result in new therapeutic interventions for infectious diseases remains unfulfilled. In the post-genomic era, the decade immediately following the availability of the genome sequence of Mycobacterium tuberculosis, tuberculosis (TB) drug discovery relied heavily on the target-based approach but this proved unsuccessful leading to a return to whole cell screening. Genomics underpinned screening by providing knowledge and many enabling technologies, most importantly whole genome resequencing to find resistance mutations and targets, and this resulted in a selection of leads and new TB drug candidates that are reviewed here. Unexpectedly, many new targets were found to be promiscuous' as they were inhibited by a variety of different compounds. In the post-post-genomics era, more advanced technologies have been implemented and these include high-content screening, screening for inhibitors of latency, the use of conditional knock-down mutants for validated targets and siRNA screens. In addition, immunomodulation and pharmacological manipulation of host functions are being explored in an attempt to widen our therapeutic options.

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