Sigel E, Barnard E A
J Biol Chem. 1984 Jun 10;259(11):7219-23.
A gamma-aminobutyrate/benzodiazepine receptor complex has been purified from bovine cerebral cortex by an improved procedure using a zwitterionic detergent. A high affinity binding site for the chloride ion channel-blocking ligand [35S]t-butyl bicyclophosphorothionate ( TBPS ) was co-purified with the high affinity binding sites for gamma-aminobutyrate and benzodiazepines. The latter two have previously been shown to reside on the same physical structure ( Sigel , E., Stephenson , F.A., Mamalaki , C., and Barnard , E. A. (1983) J. Biol. Chem. 258, 6965-6971). The dissociation constants, as measured in assay medium containing zwitterionic detergent were 90 +/- 20 nM for TBPS and 11 +/- 4 nM for [3H]flunitrazepam, whereas the binding of [3H]muscimol, a gamma-aminobutyrate agonist, showed a more complex binding behavior with more than one site. If the same preparation was assayed in a medium containing instead Triton X-100 as the detergent, the binding of TBPS was strongly inhibited, [3H]flunitrazepam binding was unaffected, and [3H]muscimol bound to a single class of sites with a dissociation constant of 33 +/- 3 nM. Regulatory interactions were retained in the complex isolated by the improved method: [3H]flunitrazepam binding was stimulated by gamma-aminobutyrate or by pentobarbital, and in a dose-dependent manner. The same two subunit types of Mr = 53,000 and 57,000 are present in the purified receptor complex as previously reported.
通过使用两性离子去污剂的改进方法,已从牛大脑皮层中纯化出γ-氨基丁酸/苯二氮䓬受体复合物。氯离子通道阻断配体[35S]叔丁基双环磷硫代酸盐(TBPS)的高亲和力结合位点与γ-氨基丁酸和苯二氮䓬的高亲和力结合位点共同纯化。后两者先前已被证明存在于同一物理结构上(西格尔,E.,斯蒂芬森,F.A.,马马拉基,C.,和巴纳德,E.A.(1983年)《生物化学杂志》258,6965 - 6971)。在含有两性离子去污剂的测定介质中测得的解离常数,TBPS为90±20 nM,[3H]氟硝西泮为11±4 nM,而γ-氨基丁酸激动剂[3H]蝇蕈醇的结合表现出更复杂的结合行为,有不止一个位点。如果在含有Triton X - 100作为去污剂的介质中对同一制剂进行测定,TBPS的结合受到强烈抑制,[3H]氟硝西泮的结合不受影响,[3H]蝇蕈醇与一类位点结合,解离常数为33±3 nM。通过改进方法分离的复合物中保留了调节相互作用:γ-氨基丁酸或戊巴比妥以剂量依赖的方式刺激[3H]氟硝西泮的结合。如先前报道,纯化的受体复合物中存在相同的两种分子量分别为53,000和57,000的亚基类型。
