Hirata M, Watanabe Y, Ishimatsu T, Ikebe T, Kimura Y, Yamaguchi K, Ozaki S, Koga T
Department of Biochemistry, Faculty of Dentistry, Kyushu University, Fukuoka, Japan.
J Biol Chem. 1989 Dec 5;264(34):20303-8.
A series of inositol 1,4,5-trisphosphate (IP3) analogs and positional isomers was examined to explore the structure-activity relationships among IP3 5-phosphatase, IP3 3-kinase, and the release of Ca2+. All analogs with additional groups on the 2nd position of IP3 inhibited the hydrolysis of [5-32P]IP3 catalyzed by erythrocyte ghosts, with a lower Ki value than seen with IP3. IP3 dehydroxylated at the 2nd position also had a lower Ki, while 2,4,5-IP3 or cyclic(1:2), 4,5-IP3 had higher Ki values. Among these compounds 2-deoxy-IP3 was as potent as IP3 in inhibiting the phosphorylation by [3H] IP3-3-kinase in rat brain cytosol. The other compounds, except for 2,4,5-IP3 inhibited the phosphorylation, however, 2-30 times higher concentrations were required. By lowering free Ca2+, the concentrations required for half-maximal inhibition were low, while those of IP3, 2-deoxy-IP3, and positional isomers remained unchanged. These compounds acted as full agonists in releasing Ca2+ from permeabilized macrophages, although 1.6-50-fold higher concentrations than IP3 were required. These compounds also inhibited the binding of [3H]IP3 to rat cerebellum and bovine adrenal cortex microsomes, but the potencies were 2.9-33 times less than that of IP3. Thus, the 2nd position of IP3 can be modified with only a slight loss of biological activity.
研究了一系列肌醇1,4,5 - 三磷酸(IP3)类似物和位置异构体,以探讨IP3 5 - 磷酸酶、IP3 3 - 激酶与Ca2+释放之间的构效关系。IP3第2位带有额外基团的所有类似物均抑制红细胞膜催化的[5 - 32P]IP3水解,其Ki值低于IP3。第2位脱羟基的IP3也具有较低的Ki值,而2,4,5 - IP3或环(1:2),4,5 - IP3具有较高的Ki值。在这些化合物中,2 - 脱氧 - IP3在抑制大鼠脑胞质溶胶中[3H] IP3 - 3 - 激酶的磷酸化方面与IP3一样有效。其他化合物,除2,4,5 - IP3外,均抑制磷酸化,然而,所需浓度高2 - 30倍。通过降低游离Ca2+,半最大抑制所需浓度较低,而IP3、2 - 脱氧 - IP3和位置异构体的浓度保持不变。这些化合物在从透化巨噬细胞释放Ca2+方面起完全激动剂作用,尽管所需浓度比IP3高1.6 - 50倍。这些化合物还抑制[3H]IP3与大鼠小脑和牛肾上腺皮质微粒体的结合,但其效力比IP3低2.9 - 33倍。因此,IP3的第2位可以进行修饰,而生物活性仅有轻微损失。
