4.4 Article

(Post-) Genomic approaches to tackle drug resistance in Leishmania

Journal

PARASITOLOGY
Volume 140, Issue 12, Pages 1492-1505

Publisher

CAMBRIDGE UNIV PRESS
DOI: 10.1017/S0031182013000140

Keywords

Leishmania; drug resistance; antimonials; miltefosine; genomics; metabolomics

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Funding

  1. GeMInI consortium
  2. Research Foundation Flanders (FWO) [G.0B81.12]
  3. EC-FP7 project Kaladrug-R [222895]
  4. Inbev-Baillet Latour Fund
  5. Belgian Cooperation

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Leishmaniasis, like other neglected diseases is characterized by a small arsenal of drugs for its control. To safeguard the efficacy of current drugs and guide the development of new ones it is thus of utmost importance to acquire a deep understanding of the phenomenon of drug resistance and its link with treatment outcome. We discuss here how (post-) genomic approaches may contribute to this purpose. We highlight the need for a clear definition of the phenotypes under consideration: innate and acquired resistance versus treatment failure. We provide a recent update of our knowledge on the Leishmania genome structure and dynamics, and compare the contribution of targeted and untargeted methods for the understanding of drug resistance and show their limits. We also present the main assays allowing the experimental validation of the genes putatively involved in drug resistance. The importance of analysing information downstream of the genome is stressed and further illustrated by recent metabolomics findings. Finally, the attention is called onto the challenges for implementing the acquired knowledge to the benefit of the patients and the population at risk.

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