bis(1-3-dibutylbarbiturate)trimethine-oxonol and tetraphenylphosphonium

bis(1-3-dibutylbarbiturate)trimethine-oxonol has been researched along with tetraphenylphosphonium* in 1 studies

Other Studies

1 other study(ies) available for bis(1-3-dibutylbarbiturate)trimethine-oxonol and tetraphenylphosphonium

ArticleYear
The membrane potential of the intraerythrocytic malaria parasite Plasmodium falciparum.
    The Journal of biological chemistry, 2004, Mar-19, Volume: 279, Issue:12

    The membrane potential (Deltapsi) of the mature asexual form of the human malaria parasite, Plasmodium falciparum, isolated from its host erythrocyte using a saponin permeabilization technique, was investigated using both the radiolabeled Deltapsi indicator tetraphenylphosphonium ([(3)H]TPP(+)) and the fluorescent Deltapsi indicator DiBAC(4)(3) (bis-oxonol). For isolated parasites suspended in a high Na(+), low K(+) solution, Deltapsi was estimated from the measured distribution of [(3)H]TPP(+) to be -95 +/- 2 mV. Deltapsi was reduced by the specific V-type H(+) pump inhibitor bafilomycin A(1), by the H(+) ionophore CCCP, and by glucose deprivation. Acidification of the parasite cytosol (induced by the addition of lactate) resulted in a transient hyperpolarization, whereas a cytosolic alkalinization (induced by the addition of NH(4)(+)) resulted in a transient depolarization. A decrease in the extracellular pH resulted in a membrane depolarization, whereas an increase in the extracellular pH resulted in a membrane hyperpolarization. The parasite plasma membrane depolarized in response to an increase in the extracellular K(+) concentration and hyperpolarized in response to a decrease in the extracellular K(+) concentration and to the addition of the K(+) channel blockers Ba(2+) or Cs(+) to the suspending medium. The data are consistent with Deltapsi of the intraerythrocytic P. falciparum trophozoite being due to the electrogenic extrusion of H(+) via the V-type H(+) pump at the parasite surface. The current associated with the efflux of H(+) is countered, in part, by the influx of K(+) via Ba(2+)- and Cs(+)-sensitive K(+) channels in the parasite plasma membrane.

    Topics: Animals; Barbiturates; Carbonyl Cyanide m-Chlorophenyl Hydrazone; Erythrocytes; Fluorescent Dyes; Glucose; Ionophores; Isoxazoles; Macrolides; Membrane Potentials; Onium Compounds; Organophosphorus Compounds; Plasmodium falciparum; Potassium Channels

2004