Genetic and chemical evaluation of Trypanosoma brucei oleate desaturase as a candidate drug target.

PLoS One

Facultad de Ciencias Bioquímicas y Farmacéuticas, Instituto de Biología Molecular y Celular de Rosario, CONICET, Universidad Nacional de Rosario, Rosario, Santa Fe, Argentina.

Published: December 2010

AI Article Synopsis

  • Trypanosomes can create polyunsaturated fatty acids, crucial for their growth and membrane function, and the oleate desaturase (OD) enzyme plays a key role in this process.
  • Experiments showed that inhibiting OD with specific compounds significantly reduced growth rates in both procyclic and bloodstream forms of T. brucei, indicating its importance for the parasites' survival.
  • Knocking down OD expression led to decreased linoleate levels and slower growth, confirming that linoleate is vital for normal membrane functionality in trypanosomes, making OD a potential target for treatments since it is absent in mammalian cells.

Article Abstract

Background: Trypanosomes can synthesize polyunsaturated fatty acids. Previously, we have shown that they possess stearoyl-CoA desaturase (SCD) and oleate desaturase (OD) to convert stearate (C18) into oleate (C18:1) and linoleate (C18:2), respectively. Here we examine if OD is essential to these parasites.

Methodology: Cultured procyclic (insect-stage) form (PCF) and bloodstream-form (BSF) Trypanosoma brucei cells were treated with 12- and 13-thiastearic acid (12-TS and 13-TS), inhibitors of OD, and the expression of the enzyme was knocked down by RNA interference. The phenotype of these cells was studied.

Principal Findings: Growth of PCF T. brucei was totally inhibited by 100 µM of 12-TS and 13-TS, with EC(50) values of 40±2 and 30±2 µM, respectively. The BSF was more sensitive, with EC(50) values of 7±3 and 2±1 µM, respectively. This growth phenotype was due to the inhibitory effect of thiastearates on OD and, to a lesser extent, on SCD. The enzyme inhibition caused a drop in total unsaturated fatty-acid level of the cells, with a slight increase in oleate but a drastic decrease in linoleate level, most probably affecting membrane fluidity. After knocking down OD expression in PCF, the linoleate content was notably reduced, whereas that of oleate drastically increased, maintaining the total unsaturated fatty-acid level unchanged. Interestingly, the growth phenotype of the RNAi-induced cells was similar to that found for thiastearate-treated trypanosomes, with the former cells growing twofold slower than the latter ones, indicating that the linoleate content itself and not only fluidity could be essential for normal membrane functionality. A similar deleterious effect was found after RNAi in BSF, even with a mere 8% reduction of OD activity, indicating that its full activity is essential.

Conclusions/significance: As OD is essential for trypanosomes and is not present in mammalian cells, it is a promising target for chemotherapy of African trypanosomiasis.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2997783PMC
http://journals.plos.org/plosone/article?id=10.1371/journal.pone.0014239PLOS

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