Joseph S K, Williams R J, Corkey B E, Matschinsky F M, Williamson J R
J Biol Chem. 1984 Nov 10;259(21):12952-5.
An early event associated with the stimulation of various secretory cells is the breakdown of phosphatidylinositol 4,5-bisphosphate and the mobilization of cellular calcium. Hydrolysis of this inositol lipid by a phosphodiesterase produces inositol trisphosphate (InsP3), a small water-soluble molecule which may serve a messenger function to release Ca2+ from internal stores. In order to assess the role of inositol lipid breakdown in the stimulation of insulin secretion we have examined the effect of InsP3 on Ca2+ fluxes in three different insulin-secreting tumor cells permeabilized by the addition of saponin. A rapid, transient release of Ca2+ from a non-mitochondrial pool occurred upon addition of InsP3 to all three cell types. Half-maximal Ca2+ release from the RIN-1046-38 and RIN-m5F cells was obtained in the concentration range 0.1-0.2 microM. However, the cells obtained from a transplantable tumor of the Syrian hamster were far more sensitive to InsP3 with half-maximal release being observed at 0.025 microM. A partially purified preparation of vesicles was isolated from this tumor which retained its responsiveness to InsP3. Half-maximal Ca2+ release from the vesicles was obtained at 0.2 microM InsP3. Our data are consistent with a role for InsP3 in mediating the increase in cytosolic free Ca2+ which occurs in response to a number of stimuli that promote the secretion of insulin.
与各种分泌细胞受到刺激相关的一个早期事件是磷脂酰肌醇4,5 - 二磷酸的分解以及细胞内钙的动员。磷酸二酯酶对这种肌醇脂质的水解产生肌醇三磷酸(InsP3),这是一种小的水溶性分子,可能作为信使发挥作用,从细胞内储存中释放Ca2+。为了评估肌醇脂质分解在刺激胰岛素分泌中的作用,我们研究了InsP3对三种不同的经皂素通透处理的胰岛素分泌肿瘤细胞中Ca2+通量的影响。向所有三种细胞类型中添加InsP3后,均出现了从非线粒体池中快速、短暂地释放Ca2+的现象。在RIN - 1046 - 38和RIN - m5F细胞中,在0.1 - 0.2微摩尔浓度范围内可获得半数最大Ca2+释放。然而,从叙利亚仓鼠的可移植肿瘤中获得的细胞对InsP3更为敏感,在0.025微摩尔时观察到半数最大释放。从该肿瘤中分离出一种部分纯化的囊泡制剂,其对InsP3仍保持反应性。在0.2微摩尔InsP3时可从囊泡中获得半数最大Ca2+释放。我们的数据与InsP3在介导细胞溶质游离Ca2+增加中所起的作用一致,这种增加是对多种促进胰岛素分泌的刺激的反应。
