Please use this identifier to cite or link to this item: http://gukir.inflibnet.ac.in:8080/jspui/handle/123456789/5809
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dc.contributor.authorAnderson, RJ
dc.contributor.authorBendell, DJ
dc.contributor.authorHooper, M
dc.contributor.authorCairns, D
dc.contributor.authorMackay, SP
dc.contributor.authorHiremath, SP
dc.contributor.authorJivanagi, AS
dc.contributor.authorBadami, S
dc.contributor.authorBiradar, JS
dc.contributor.authorTownson, S
dc.date.accessioned2020-06-12T15:08:55Z-
dc.date.available2020-06-12T15:08:55Z-
dc.date.issued2001
dc.identifier.citationJOURNAL OF PHARMACY AND PHARMACOLOGY , Vol. 53 , 1 , p. 89 - 94en_US
dc.identifier.uri10.1211/0022357011775055
dc.identifier.urihttp://gukir.inflibnet.ac.in:8080/jspui/handle/123456789/5809-
dc.description.abstractTransition state phosphoramidate inhibitors of beta -tubulin were designed as potential antifilarial agents. The reaction of 2-aminobenzimidazole with diisopropyl phosphite and carbon tetrachloride at a low temperature gave the unexpected 1-diisopropoxyphosphoryl-2-aminobenzimidazole which on heating gave the novel benzimidazole derivative, 2-(diisopropoxyphosphoryl)aminobenzimidazole. Both products were fully characterized and the synthetic procedure to both compounds was optimized. The procedure was used to prepare the related 5-benzoyl-2-(diisopropoxyphosphoryl)aminobenzimidazole and 5-benzoyl-2-(diethoxyphosphoryl)aminobenzimidazole (1d). In a preliminary trial against Brugia pahangi compound Id was found to have no antifilarial activity. This lack of activity may be attributed to its extreme insolubility and thus low bioavailability. The synthesis of analogous, more soluble, phosphorothioate-substituted benzimidazoles using the same methods may yield compounds with greater antifilarial activity.en_US
dc.publisherROYAL PHARMACEUTICAL SOC GREAT BRITAIN
dc.titlePotential transition state phosphoramidate inhibitors of beta-tubulin as antifilarial agentsen_US
dc.typeArticle
Appears in Collections:1. Journal Articles

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