4.5 Article

Oxantel is an N-type (methyridine and nicotine) agonist not an L-type (levamisole and pyrantel) agonist:: classification of cholinergic anthelmintics in Ascaris

Journal

INTERNATIONAL JOURNAL FOR PARASITOLOGY
Volume 34, Issue 9, Pages 1083-1090

Publisher

ELSEVIER SCI LTD
DOI: 10.1016/j.ijpara.2004.04.014

Keywords

oxantel; thenium; bephenium; levamisole; pyrantel; nicotine; ACh receptor; receptor subtypes

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Funding

  1. NIAID NIH HHS [R01 AI4794] Funding Source: Medline

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Three pharmacological subtypes of cholinergic receptors have been distinguished in Ascaris suum using a muscle contraction assay and classical pharmacological techniques. The receptor subtypes are: a B-subtype (sensitive to bephenium); an L-subtype (sensitive to levamisole and pyrantel); and an N-subtype (sensitive to nicotine and methyridine). Oxantel is a cholinergic anthelmintic that was first introduced for the treatment of whipworm, Trichuris, infections in children. Here, we compare the subtype selectivity of oxantel with thenium and other cholinergic anthelmintics. We used the A. suum assay to derive pA(2) values for the agonists: oxantel, thenium, bephenium, levamisole, pyrantel, nicotine and methyridine with the antagonists: paraherquamide, 2-desoxyparaherquamide and methyllycaconitine. pA(2) values, rather than pK(B) values, were determined for all agonists when it was found that Schild slopes for some agonists were significantly less than 1.0. The pA(2) of oxantel was 6.58 +/- 0.25 for paraherquamide; 5.39 +/- 0.28 for 2-desoxyparaherquamide; 7.01 +/- 0.19 for methyllycaconitine. Comparison of pA2 values using cluster analysis showed that oxantel was grouped with nicotine and methyridine, the N-subtype agonists. Thenium had pA(2)S of 7.84 +/- 0.41 for paraherquamide; 5.52 +/- 0.50 for 2-desoxyparaherquamide; 6.33 +/- 0.19 for methyllycaconitine. Cluster analysis placed thenium between the L-subtype agonists and the B-subtype agonist. The therapeutic significance of classification of cholinergic anthelmintics is discussed. Combination of oxantel and pyrantel would have therapeutic advantages, covering N- and L-subtypes, and so increasing spectrum of action and reducing the potential for development of resistance. Our results predict that oxantel may remain effective in some nematode isolates that have become levamisole- and pyrantel-resistant. Published by Elsevier Ltd on behalf of Australian Society for Parasitology Inc.

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