Shieh H L, Hansen H, Zhu J, Riedel H
Section on Molecular Biology, Joslin Diabetes Center, Boston, MA, USA.
Cancer Detect Prev. 1996;20(6):576-89.
Conventional mammalian protein kinase C (PKC) isoforms alpha, beta 1, and gamma were expressed in Saccharomyces cerevisiae and resulted in a differential increase in the yeast doubling time in response to distinct classes of PKC activators. Mutants were created in the regulatory domain of PKC alpha to map the interaction with the different activators. The macrocyclic lactone bryostatin 5 preferentially regulated PKC alpha activity through the second cysteine-rich sequence (CYS2) of Cl, while regulation by the diterpene ester mezerein displayed strong preference for the first cysteine-rich sequence (CYS1) of Cl. The phorbol esters phorbol-12-myristate-13-acetate (PMA) and 12-deoxyphorbol 13-phenylacetate 20-acetate (dPPA) regulated PKC enzymatic activity equally potently via CYS1 or CYS2 albeit at reduced levels compared with native PKC alpha. For the diterpene ester ingenol-3, 20-dibenzoate and the indol alkaloids (-)-7-octyl-indolactam V and (-)-indolactam V, no responses were observed for mutants lacking either CYS1 or CYS2 whereas native PKC alpha activity was regulated. These in vivo results were complemented by in vitro binding and catalytic assays which showed correlation between PKC enzymatic activity and the cell growth characteristics. The observed phenotype can be exploited to screen natural compounds in vivo for their PKC regulatory potential and to map the underlying interactions.
传统的哺乳动物蛋白激酶C(PKC)亚型α、β1和γ在酿酒酵母中表达,并且在响应不同类别的PKC激活剂时,导致酵母倍增时间出现差异增加。在PKCα的调节结构域中创建突变体,以绘制与不同激活剂的相互作用图谱。大环内酯类苔藓抑素5优先通过C1的第二个富含半胱氨酸序列(CYS2)调节PKCα活性,而二萜酯mezerein的调节则对C1的第一个富含半胱氨酸序列(CYS1)表现出强烈偏好。佛波酯佛波醇-12-肉豆蔻酸酯-13-乙酸酯(PMA)和12-脱氧佛波醇13-苯乙酸酯20-乙酸酯(dPPA)通过CYS1或CYS2同等有效地调节PKC酶活性,尽管与天然PKCα相比水平有所降低。对于二萜酯ingenol-3,20-二苯甲酸酯以及吲哚生物碱(-)-7-辛基-吲哚内酰胺V和(-)-吲哚内酰胺V,缺乏CYS1或CYS2的突变体未观察到反应,而天然PKCα活性受到调节。这些体内结果通过体外结合和催化试验得到补充,这些试验表明PKC酶活性与细胞生长特性之间存在相关性。观察到的表型可用于在体内筛选天然化合物的PKC调节潜力,并绘制潜在的相互作用图谱。
