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Activity of quinfamide against natural infections of Entamoeba criceti in hamsters: a new potent agent for intestinal amoebiasis

Published online by Cambridge University Press:  06 April 2009

R. G. Slighter ,
A. Yarinsky ,
H. P. Drobeck  and
D. M. Bailey
R. G. Slighter
Affiliation:
Departments of ParasitologySterling-Winthrop Research Institute, Rensselaer, NY 12144
A. Yarinsky
Affiliation:
Departments of ParasitologySterling-Winthrop Research Institute, Rensselaer, NY 12144
H. P. Drobeck
Affiliation:
ToxicologySterling-Winthrop Research Institute, Rensselaer, NY 12144
D. M. Bailey
Affiliation:
Medicinal ChemistrySterling-Winthrop Research Institute, Rensselaer, NY 12144
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Summary

A novel tetrahydroquinolinyl ester, quinfamide, administered orally in multiple doses for 3 days had an ED50, of 0·25 mg/kg/day (total dose 0·75 mg/kg) for eradicating Entamoeba criceti in hamsters in several tests. It was significantly more active by direct comparison than 3 commercially available amoebicides and at least as active as 2 other esters of the parent compound, 1-(dichloroacetyl)-1,2,3,4-tetrahydro-6-quinonnol. After administration of a single dose, ED50, calculations for quinfamide averaged 0·9 mg/kg. Quinfamide was considerably more active than the other tetrahydroquinolinols, diloxanide furoate and teclozan, and it was approximately 1·5 times more active than etofamide; a statistical significance between the latter 2 drugs could be demonstrated in one of 4 tests. Administered prophylactically, quinfamide was shown to protect hamsters from re-infection with E. criceti. It also inhibited propagation of E. histolytica in vitro at a concentration of 20 /tg/ml. No adverse effects were noted in rodents after a single dose as high as 10 g/kg. Daily administration to monkeys of doses up to 500 mg/kg for as long as 37 days produced no pharmacological aberrations during or after medication; haematological studies and urine analyses were normal and no gross or microscopical tissue changes attributable to quinfamide were observed. No toxicity was revealed following acute (2 g/kg) and chronic (500 mg/kg/day × 31 days) administration of the drug to dogs and rats, respectively.

Type
Research Article
Information
Parasitology , Volume 81 , Issue 1 , August 1980 , pp. 157 - 168
Copyright
Copyright © Cambridge University Press 1980

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