Literature DB >> 3563317

A comparison of the response of Dipetalonema viteae and Brugia pahangi adult worms to antifilarial agents in vitro.

J P Court, M Martin-Short, G M Lees.   

Abstract

The drug response of Dipetalonema viteae and B. pahangi under various culture conditions have been evaluated. B. pahangi female worms proved to be more susceptible to CGP 6140 (4-nitro-4'-(N-methyl)piperazinyl thiocarbonylido-diphenylamine), CGP 20376 (N-(2-tert-butyl-5-methoxy-benzothiazol-6-yl)dithiocarbonic acid 5-(1-carboxyethyl)-ether) and amoscanate when glucose availability was restricted. This increased potency may be related to effects on glycogen metabolism by CGP 20376 and amoscanate. Using the parameters of parasite motility, survival, glucose consumption and microfilarial output, Eagles Minimum Essential Medium supplemented with 10% inactivated foetal calf serum plus either a 95% air:5% CO2 or a 95% N2:5% CO2 gas phase was shown to be highly suitable for short term maintenance (5 days). Examination of 12 drugs selected on their in vivo activity against B. pahangi and D. viteae demonstrated little difference between the drug susceptibilities of male and female worms. However, there were intrinsic differences between worm species. The relationship between these disparate susceptibilities and the reported in vivo efficacies of these drugs and the importance of selecting appropriate conditions for in vitro drug assays are discussed. Ivermectin at 10(-5) M caused a rapid flaccid paralysis and a complete suppression of microfilarial output by D. viteae. Despite continued paralysis of the worms they continued to utilise as much glucose as untreated worms over a 4 day period.

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Year:  1986        PMID: 3563317

Source DB:  PubMed          Journal:  Trop Med Parasitol        ISSN: 0177-2392


  4 in total

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4.  Recognition and killing of Brugia malayi microfilariae by human immune cells is dependent on the parasite sample and is not altered by ivermectin treatment.

Authors:  Barbara J Reaves; Connor Wallis; Ciaran J McCoy; W Walter Lorenz; Balazs Rada; Adrian J Wolstenholme
Journal:  Int J Parasitol Drugs Drug Resist       Date:  2018-09-22       Impact factor: 4.077

  4 in total

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