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Cellular uptake of a catechol iron chelator and chloroquine into Plasmodium falciparum infected erythrocytes.

Abstract
Our study demonstrates the capacity of FR160, a catechol iron chelator, to reach and accumulate into infected Plasmodium falciparum erythrocytes and parasites (cellular accumulation ratio between 12 and 43). Steady-state FR160 accumulation is obtained after 2 hr of exposure. After 2 hr exposure, it reaches intracellular levels that are 4- to 10-fold higher in infected red blood cells than those attained in normal erythrocytes. There is quite a good correlation between the accumulation of chloroquine and FR160 in the different strains (r=0.939) and in the IC(50) values (r=0.719). In contrast, the accumulation of FR160 and its activity is poorly correlated (r=0.500), suggesting that activity of FR160 may be independent of its penetration into infected erythrocytes. The mechanism of accumulation is yet unknown but based on inhibitor studies, the uptake of FR160 seems to be not associated with the calcium pump or channel, the potassium channel or the Na(+)/H(+) exchanger. Combinations of FR160 with verapamil, diltiazem, clotrimazole, amiloride, diazoxide, 4-aminopyridine, and picrotoxin should be avoided (antagonistic effects). The potent in vitro activity of FR160 on chloroquine-resistant strains or isolates, its lower toxicity against Vero cells, its mechanisms of action, its capacity to reach rapidly and accumulate into infected erythrocytes suggest that FR160 holds much promise as a new structural lead and effective antimalarial agent or at least a promising adjuvant in treatment of malaria.
AuthorsAkli Hammadi, Florence Ramiandrasoa, Veronique Sinou, Christophe Rogier, Thierry Fusai, Jacques Le Bras, Daniel Parzy, Gerhard Kunesch, Bruno Pradines
JournalBiochemical pharmacology (Biochem Pharmacol) Vol. 65 Issue 8 Pg. 1351-60 (Apr 15 2003) ISSN: 0006-2952 [Print] England
PMID12694876 (Publication Type: Journal Article, Research Support, Non-U.S. Gov't)
Chemical References
  • FR 160
  • Siderophores
  • Chloroquine
  • Iron
  • Spermidine
Topics
  • Animals
  • Biological Transport
  • Chloroquine (blood, pharmacokinetics)
  • Erythrocytes (metabolism, parasitology)
  • Humans
  • Iron (metabolism)
  • Kinetics
  • Plasmodium falciparum (metabolism, pathogenicity)
  • Siderophores (blood, pharmacokinetics)
  • Spermidine (analogs & derivatives, blood, pharmacokinetics)

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