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Pharmacokinetics of aditoprim in goats using a radioassay

✍ Scribed by M. Perwaiz Iqbal; N. Mahboobali; Sarfaraz K. Niazi; M. Anwar Mahmood


Publisher
John Wiley and Sons
Year
1990
Tongue
English
Weight
373 KB
Volume
11
Category
Article
ISSN
0142-2782

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✦ Synopsis


Abstract

A simple, highly sensitive radioassay was developed for the activity of a newly discovered inhibitor of dihydrofolate reductase (DHFR), aditoprim. The procedure is based on the inhibition of binding of [^3^H]‐methotrexate ([^3^H]MTX) with bacterial dihydrofolate reductase by the antifolate, aditoprim. The analytic sensitivity using this binding inhibition method was less than 5 ng in plasma. The procedure developed requires no extraction of the drug from the plasma. The variation of simultaneous duplicate determinations was 6Β·3 per cent, whereas the variability of plasma samples assayed on different days was less than 11 per cent. The assay developed was applied to study the pharmacokinetics of aditoprim in the goat. In comparison with trimethoprim (TMP), the new inhibitor of DHFR, aditoprim, had a longer half‐life and a larger volume of distribution, suggesting enhanced and prolonged antibacterial activity of aditoprim over TMP.


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