Kallos J, Shaw K P
Proc Natl Acad Sci U S A. 1971 May;68(5):916-9. doi: 10.1073/pnas.68.5.916.
An affinity labeling reagent for the estrogenic-binding site of bovine liver L-glutamate dehydrogenase (EC 1.4.1.3) was prepared by conversion of diethylstilbestrol to its alkylating analogue, bromoacetyldiethylstilbestrol. Under standard assay conditions, the analogue acted as a reversible allosteric ligand with regulatory activity much like that of diethylstilbestrol. However, incubation of the enzyme with the alkylating agent in the presence of DPNH resulted in a permanent decrease in glutamate (X form) and an increase in alanine (Y form) activities, and in covalent attachment of diethylstilbestrol in the ratio of 1 mol per subunit (of particle weight 52,000). The brominated analogue behaved as an affinity label that mimicked the allosteric effects of diethylstilbestrol. Diethylstilbestrol protection of the enzyme against alkylation by bromoacetylated sterol suggested competition for the same binding site, while ADP protection indicated a shift of protein equilibrium into the X form. The diethylstilbestrol-enzyme compound was desensitized (relative to the native enzyme) to allosteric reagents such as ADP and GTP. The results were consistent with conformational freezing of the modified protein molecule into the Y form.
通过将己烯雌酚转化为其烷基化类似物溴乙酰己烯雌酚,制备了一种用于牛肝L-谷氨酸脱氢酶(EC 1.4.1.3)雌激素结合位点的亲和标记试剂。在标准测定条件下,该类似物作为一种可逆的别构配体,其调节活性与己烯雌酚非常相似。然而,在DPNH存在下,将酶与烷基化剂一起孵育会导致谷氨酸(X型)活性永久性降低,丙氨酸(Y型)活性增加,并且己烯雌酚以每亚基(颗粒重量52,000)1摩尔的比例共价结合。溴化类似物表现为一种亲和标记,模拟了己烯雌酚的别构效应。己烯雌酚对酶免受溴乙酰化固醇烷基化的保护作用表明它们竞争相同的结合位点,而ADP保护则表明蛋白质平衡向X型转变。己烯雌酚-酶复合物对诸如ADP和GTP等别构试剂脱敏(相对于天然酶)。结果与修饰后的蛋白质分子构象冻结为Y型一致。