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. 2014 Aug;58(8):4452-63.
doi: 10.1128/AAC.02309-13. Epub 2014 May 27.

In vitro and in vivo evaluation of 28DAP010, a novel diamidine for treatment of second-stage African sleeping sickness

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In vitro and in vivo evaluation of 28DAP010, a novel diamidine for treatment of second-stage African sleeping sickness

Tanja Wenzler et al. Antimicrob Agents Chemother. 2014 Aug.

Abstract

African sleeping sickness is a neglected tropical disease transmitted by tsetse flies. New and better drugs are still needed especially for its second stage, which is fatal if untreated. 28DAP010, a dipyridylbenzene analogue of DB829, is the second simple diamidine found to cure mice with central nervous system infections by a parenteral route of administration. 28DAP010 showed efficacy similar to that of DB829 in dose-response studies in mouse models of first- and second-stage African sleeping sickness. The in vitro time to kill, determined by microcalorimetry, and the parasite clearance time in mice were shorter for 28DAP010 than for DB829. No cross-resistance was observed between 28DAP010 and pentamidine on the tested Trypanosoma brucei gambiense isolates from melarsoprol-refractory patients. 28DAP010 is the second promising preclinical candidate among the diamidines for the treatment of second-stage African sleeping sickness.

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Figures

FIG 1
FIG 1
Chemical structures of 28DAP010, its prodrug DB1244, and its analogues.
FIG 2
FIG 2
In vitro activities of pentamidine versus 28DAP010 against different T. b. gambiense strains. Symbols represent the average IC50 of at least three independent determinations. The first number in each set of parentheses represents the IC50 for pentamidine and the second number that for 28DAP010. No significant correlation was observed between pentamidine and 28DAP010 activities (r2 = 0.019).
FIG 3
FIG 3
Microcalorimetry heat flow profiles of T. b. rhodesiense strain STIB900 (A) and T. b. gambiense strains STIB930 (B) and ITMAP141267 (C) in the presence of various concentrations of 28DAP010. Drug-free samples included parasites (5 × 104/ml inoculum) without drug treatment, and trypanosome-free experiment did not include any parasites or drug. Each curve represents the mean of three samples.
FIG 4
FIG 4
Plasma (filled circles) and brain (open squares) concentration-time profiles of 28DAP010 following intravenous (A) and intraperitoneal (B) administration to uninfected mice. The doses were 7.5 μmol/kg (or 2.4 mg/kg) for i.v. administration and 65 μmol/kg (or 21 mg/kg) for i.p. administration. Symbols and error bars represent means and standard errors of triplicate determinations, respectively.

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