Development of novel valerolactam-benzimidazole hybrids anthelmintic derivatives: Diffusion and biotransformation studies in helminth parasites

•Further studies of novel benzimidazole bioactive hybrids are presented.•Diffusion in H. contortus (susceptible/from sheep farms) and M. vogae is presented.•Sulphoxidation drug metabolism was measured in both target parasites.•Oxidation was more relevant in H. contortus parasites from sheep farms.•N...

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Bibliographic Details
Published in:Experimental parasitology 2015-06, Vol.153, p.75-80
Main Authors: Munguía, Beatriz, Michelena, Mauricio, Melian, Elisa, Saldaña, Jenny, Ures, Ximena, Manta, Eduardo, Domínguez, Laura
Format: Article
Language:English
Subjects:
Animals
Anthelmintics - chemical synthesis
Anthelmintics - chemistry
Anthelmintics - pharmacology
Benzimidazoles - chemistry
Benzimidazoles - pharmacology
Biotransformation
Cestodes
Drug resistance
Female
Haemonchus contortus
Helminthiasis, Animal - drug therapy
Helminthiasis, Animal - parasitology
Helminths - drug effects
Helminths - growth & development
Lactams - chemistry
Lactams - pharmacology
Male
Mesocestoides vogae
Mice
Nematodes
Rats
Sheep
Sheep Diseases - drug therapy
Sheep Diseases - parasitology
Valerolactam-benzimidazole hybrids
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Summary:•Further studies of novel benzimidazole bioactive hybrids are presented.•Diffusion in H. contortus (susceptible/from sheep farms) and M. vogae is presented.•Sulphoxidation drug metabolism was measured in both target parasites.•Oxidation was more relevant in H. contortus parasites from sheep farms.•New hybrid compound 10 was not oxidized and showed a high diffusion rate. In the search for new anthelmintics able to overcome the resistance problem against all available drugs in livestock, the synthesis of novel valerolactam-benzimidazole hybrid compounds was reported. This allowed us to obtain these in vitro and in vivo bioactive compounds using Nippostrongylus brasiliensis rat model by integrating physiology-based assays and ex vivo diffusion studies. In order to further study those novel hybrid molecules, Haemonchus contortus (a sheep gastrointestinal nematode of interest) and Mesocestoides vogae tetrathyridia (a useful system to study the efficacy of anthelmintic drugs against cestoda) were used as parasite models to compare the ex vivo patterns of diffusion and biotransformation of benzimidazoles and their valerolactam-benzimidazole hybrid derivatives. On average, a nine-fold higher intraparasitic concentration of compounds was found in M. vogae compared with H.contortus, with similarities regarding the order of entry of compounds, highlighting febendazole (FEB) and its hybrid compound 10, while valerolactam compound 2 practically did not penetrate the parasites. Interestingly, sulphoxidation drug metabolism was observed and measured, revealing percentages of oxidation of 8.2% and 14.5% for albendazole (ABZ) and febendazole respectively in M. vogae, while this effect was more relevant in H. contortus parasite. More importantly, significant differences were observed between anthelmintic-susceptible adult parasites (Hc S) and those from sheep farms (Hc U). In fact, the percentages of oxidation of FEB and the hybrid compound 8 were higher in Hc U (25.5%, 54.1%, respectively) than in Hc S (8.8%, 38.2%). Interestingly, sulphoxidation of hybrid compound 10 was neither observed in M. vogae nor in H. contortus parasites, suggesting that increased drug metabolism (oxidation reactions) could not be used by these parasites as a defense mechanism against this novel drug.
ISSN:0014-4894
1090-2449
DOI:10.1016/j.exppara.2015.03.013