Journal of Antimicrobial Chemotherapy, Vol 42, 55-60, Copyright © 1998 by The British Society for Antimicrobial Chemotherapy
N Basilico, E Pagani, D Monti, P Olliaro and D Taramelli
The malaria parasite metabolizes haemoglobin and detoxifies the resulting
haem by polymerizing it to form haemozoin (malaria pigment). A polymer
identical to haemozoin, beta-haematin, can be obtained in vitro from
haematin at acidic pH. Quinoline-containing anti-malarials (e.g.
chloroquine) inhibit the formation of either polymer. Haem polymerization
is an essential and unique pharmacological target. To identify molecules
with haem polymerization inhibitory activity (HPIA) and quantify their
potency, we developed a simple, inexpensive, quantitative in-vitro
spectrophotometric microassay of haem polymerization. The assay uses
96-well U-bottomed polystyrene microplates and requires 24 h and a
microplate reader. The relative amounts of polymerized and unpolymerized
haematin are determined, based on solubility in DMSO, by measuring
absorbance at 405 nm in the presence of test compounds as compared with
untreated controls. The final product (a solid precipitate of polymerized
haematin) was validated using infrared spectroscopy and the assay proved
reproducible; in this assay, activity could be partly predicted based on
the compound's chemical structure. Both water-soluble and water- insoluble
compounds can be quantified by this method. Although the throughput of this
assay is lower than that of radiometric methods, the assay is easier to set
up and cheaper, and avoids the problems related to radioactive waste
disposal.
ORIGINAL ARTICLES
A microtitre-based method for measuring the haem polymerization inhibitory activity (HPIA) of antimalarial drugs
Istituto di Microbiologia Medica, Universita di Milano.
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