In vitro antigiardial activity of IRE-6A and IRE-7B, two ethyl-phenylcarbamate derivatives

Resistance is a practical problem associated to the use of benzimidazoles in the antigiardial therapy. Since benzimidazole-resistant strains of fungi have shown increased sensitivity to phenylcarbamates, in this study we synthesized and in vitro tested novel substituted phenylcarbamates against the protozoa Giardia intestinalis. IRE-6A and IRE-7B, two 4-R-ethylphenylcarbamates demonstrated an important antigiardial activity although that was modest when compared to albendazole in axenic cultures of Giardia intestinalis. Results of this study suggest a potential role of phenylcarbamates as alternative to benzimidazoles in the therapy of giardiasis.

Antiparasitic agents; Giardiasis; Phenylcarbamates albendazole; antiprotozoal agent; benzimidazole; carbamic acid derivative; ethylphenylcarbamate derivative; ire 6a; ire 7b; macrolide; nitrofuran; nitroimidazole; oxibendazole; praziquantel; triclabendazole; unclassified drug; antibiotic resistance; antibiotic sensitivity; antimicrobial activity; article; controlled study; drug determination; drug potency; drug structure; drug synthesis; fungal strain; Giardia lamblia; giardiasis; in vitro study; nonhuman; structure activity relation; Albendazole; Animals; Antiprotozoal Agents; Carbamates; Giardia lamblia

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