首页> 美国卫生研究院文献>Environmental Health Perspectives >Structure-activity correlations for interactions of bicyclophosphorus esters and some polychlorocycloalkane and pyrethroid insecticides with the brain-specific t-butylbicyclophosphorothionate receptor.
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Structure-activity correlations for interactions of bicyclophosphorus esters and some polychlorocycloalkane and pyrethroid insecticides with the brain-specific t-butylbicyclophosphorothionate receptor.

机译:双环磷酸酯与某些聚氯环烷烃和拟除虫菊酯类杀虫剂与脑特异性叔丁基双环磷硫代酸酯受体相互作用的结构活性相关性。

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摘要

[35S]t-Butylbicyclophosphorothionate or [35S]TBPS is an improved radioligand for the picrotoxinin binding site in rat brain synaptic membranes. The toxic isomers of the hexachlorocyclohexanes, polychlorobornanes, and chlorinated cyclodienes displace [35S]TBPS with a stereospecificity and potency generally correlated with their mammalian toxicity. In a few cases this correlation is improved by correction for metabolic activation or detoxification on using a coupled brain receptor/liver microsomal oxidase system. The alpha-cyano-3-phenoxybenzyl pyrethroids, although less potent, inhibit [35S]TBPS binding in a stereospecific manner correlated with their toxicity. Scatchard analyses indicate that these three classes of polychlorocycloalkane insecticides act at the TBPS binding site within the gamma-aminobutyric acid (GABA) receptor-ionophore complex whereas the alpha-cyano pyrethroids interact with a closely associated site. These insecticides and TBPS analogs may serve as useful probes further to elucidate the topography of the TBPS binding site and its relationship to the chloride channel.
机译:[35S] t-丁基二环磷酸正硫酸酯或[35S] TBPS是大鼠脑突触膜中微毒素结合位点的改良放射性配体。六氯环己烷,聚氯冰片烷和氯化环二烯的毒性异构体取代[35S] TBPS的立体特异性和效力通常与其哺乳动物毒性有关。在某些情况下,通过使用耦合的脑受体/肝微粒体氧化酶系统校正代谢激活或排毒可以改善这种相关性。 α-氰基-3-苯氧基苄基拟除虫菊酯虽然效力不强,但以与它们的毒性相关的立体特异性方式抑制[35S] TBPS结合。斯卡查德分析表明,这三类聚氯环烷杀虫剂在γ-氨基丁酸(GABA)受体-离子载体复合物内的TBPS结合位点起作用,而α-氰基拟除虫菊酯与紧密相关的位点相互作用。这些杀虫剂和TBPS类似物可作为有用的探针,进一步阐明TBPS结合位点的形貌及其与氯离子通道的关系。

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