Mitochondrial function in Babesia bovis

A variety of anti-mitochondrial drugs that had previously been found to inhibit the growth of the malarial parasite Plasmodium falciparum were tested on Babesia bovis in vitro. Several of these drugs were found to be non-toxic towards B. bovis. However, those drugs that were found to inhibit babesia...

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Published inInternational journal for parasitology Vol. 22; no. 2; pp. 165 - 171
Main Authors Gozar, M.M.G, O'Sullivan, W.J, Bagnara, A.S
Format Journal Article
LanguageEnglish
Published Oxford Elsevier Science 01.04.1992
Subjects
adenosinetriphosphatase
Animals
atp-adp translocase
Babesia bovis
Babesia bovis - drug effects
Babesia bovis - ultrastructure
Biochemistry. Physiology. Immunology. Molecular biology
Biological and medical sciences
biosynthesis
electron transfer
electron transport chain
enzyme inhibitors
enzymes
Fundamental and applied biological sciences. Psychology
inhibition
Invertebrates
metabolic inhibitors
mitochondria
Mitochondria - drug effects
Mitochondria - physiology
protein synthesis
proton pump
Protozoa
pyrimidines
ubiquinones
Protozoa
Respiratory chain
Mitochondria
Energy metabolism
Radiolabelling
Parasite
Biosynthesis
Inhibitor
Babesia bovis
Sporozoa
Chromatography
Pyrimidine
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Summary:A variety of anti-mitochondrial drugs that had previously been found to inhibit the growth of the malarial parasite Plasmodium falciparum were tested on Babesia bovis in vitro. Several of these drugs were found to be non-toxic towards B. bovis. However, those drugs that were found to inhibit babesial growth included compounds (shown in parentheses) that have the following putative mitochondrial targets in the parasite: ATP synthetase complex (rhodamine 123, oligomycin, Janus Green); ATP-ADP translocase (bongkrekic acid); electron transport (rotenone, n-heptyl-4-hydroxyquinoline-N-oxide (HQNO), antimycin A); ubiquinone (CoQ) function (BW58C, menoctone); protein synthesis (tetracycline); and the proton pump (CCCP). We have also investigated the effects of some of these drugs on pyrimidine biosynthesis de novo by following the incorporation of [14C]bicarbonate into pyrimidine nucleotides and into the pyrimidine moieties of nucleic acids. The ubiquinone analogues BW58C and menoctone inhibited this pathway in the nm-micromolar range of concentrations. Inhibitors of electron transport (antimycin A and oligomycin) and an uncoupler (CCCP) were also effective inhibitors of pyrimidine biosynthesis de novo. We conclude that B. bovis has a functional mitochondrion that contributes significantly to pyrimidine biosynthesis de novo and to the overall energy metabolism of the parasite.
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ISSN:0020-7519
1879-0135
DOI:10.1016/0020-7519(92)90097-5