| Indication |
For the treatment or prevention of Pneumocystis carinii
pneumonia in patients who are intolerant to
trimethoprim-sulfamethoxazole (TMP-SMX). Also indicated for the acute
oral treatment of mild to moderate PCP in patients who are intolerant to
TMP-SMX. |
| Pharmacodynamics |
Atovaquone is a highly lipophilic drug that closely resembles
the structure ubiquinone. Its inhibitory effect being comparable to
ubiquinone, in sensitive parasites atovaquone can act by selectively
affecting mitochondrial electron transport and parallel processes such
as ATP and pyrimidine biosynthesis. For illustration, cytochrome bc1
complex (complex III) seems to serve as a highly discriminating
molecular target for atovaquone in Plasmodia
atovaquone has the advantage of not causing myelosuppression, which is
an important issue in patients who have undergone bone marrow
transplantation. |
| Mechanism of action |
Atovaquone is a hydroxy- 1, 4- naphthoquinone, an analog of
ubiquinone, with antipneumocystis activity. The mechanism of action
against Pneumocystis carinii has not been fully elucidated. In
Plasmodium species, the site of action appears to be the cytochrome bc1
complex (Complex III). Several metabolic enzymes are linked to the
mitochondrial electron transport chain via ubiquinone. Inhibition of
electron transport by atovaquone will result in indirect inhibition of
these enzymes. The ultimate metabolic effects of such blockade may
include inhibition of nucleic acid and ATP synthesis. Atovaquone also
has been shown to have good in vitro activity against Toxoplasma gondii. |
| Absorption |
The bioavailability of atovaquone is low and variable and is
highly dependent on formulation and diet. Bioavailability of the
suspension increases two-fold when administered with meals. When
administered with food, bioavailability is approximately 47%. Without
food, the bioavailability is 23%. |
| Volume of distribution |
|
| Protein binding |
Atovaquone is extensively bound to plasma proteins (99.9%) over the concentration range of 1 to 90 µg/mL. |
| Metabolism |
Some evidence suggests limited metabolism (although no metabolites have been identified). |
| Route of elimination |
The half-life of atovaquone is long due to presumed enterohepatic
cycling and eventual fecal elimination. There was little or no excretion
of atovaquone in the urine (less than 0.6%). |
| Half life |
2.2 to 3.2 days |
| Clearance |
- 10.4 +/- 5.5 ml/min [HIV-infected patients receiving IV administration]
|
| Toxicity |
The median lethal dose is higher than the maximum oral dose tested
in mice and rats (1825 mg/kg per day). Overdoses up to 31,500 mg of
atovaquone have been reported. In one such patient who also took an
unspecified dose of dapsone, methemoglobinemia occurred. Rash has also
been reported after overdose. |
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