Lerner U H, Fredholm B B, Ransjö M
Biochem J. 1986 Dec 1;240(2):529-39. doi: 10.1042/bj2400529.
The effect of the adenylate cyclase activator forskolin on bone resorption and cyclic AMP accumulation was studied in an organ-culture system by using calvarial bones from 6-7-day-old mice. Forskolin caused a rapid and fully reversible increase of cyclic AMP, which was maximal after 20-30 min. The phosphodiesterase inhibitor rolipram (30 mumol/l), enhanced the cyclic AMP response to forskolin (50 mumol/l) from a net cyclic AMP response of 1234 +/- 154 pmol/bone to 2854 +/- 193 pmol/bone (mean +/- S.E.M., n = 4). The cyclic AMP level in bones treated with forskolin (30 mumol/l) was significantly increased after 24 h of culture. Forskolin, at and above 0.3 mumol/l, in the absence and the presence of rolipram (30 mumol/l), caused a dose-dependent cyclic AMP accumulation with an calculated EC50 (concentration producing half-maximal stimulation) value at 8.3 mumol/l. In 24 h cultures forskolin inhibited spontaneous and PTH (parathyroid hormone)-stimulated 45Ca release with calculated IC50 (concentration producing half-maximal inhibition) values at 1.6 and 0.6 mumol/l respectively. Forskolin significantly inhibited the release of 3H from [3H]proline-labelled bones stimulated by PTH (10 nmol/l). The inhibitory effect by forskolin on PTH-stimulated 45Ca release was significant already after 3 h of culture. In 24 h cultures forskolin (3 mumol/l) significantly inhibited 45Ca release also from bones stimulated by prostaglandin E2 (1 mumol/l) and 1 alpha-hydroxycholecalciferol (0.1 mumol/l). The inhibitory effect of forskolin on spontaneous and PTH-stimulated 45Ca release was transient. A dose-dependent stimulation of basal 45Ca release was seen in 120 h cultures, at and above 3 nmol of forskolin/l, with a calculated EC50 value at 16 nmol/l. The stimulatory effect of forskolin (1 mumol/l) could be inhibited by calcitonin (0.1 unit/ml), but was insensitive to indomethacin (1 mumol/l). Forskolin increased the release of 3H from [3H]proline-labelled bones cultured for 120 h and decreased the amount of hydroxyproline in bones after culture. Forskolin inhibited PTH-stimulated release of Ca2+, Pi, beta-glucuronidase and beta-N-acetylglucosaminidase in 24 h cultures. In 120 h cultures forskolin stimulated the basal release of minerals and lysosomal enzymes.(ABSTRACT TRUNCATED AT 400 WORDS)
利用6 - 7日龄小鼠的颅骨,在器官培养系统中研究了腺苷酸环化酶激活剂福斯高林对骨吸收和环磷酸腺苷(cAMP)积累的影响。福斯高林可使cAMP迅速且完全可逆地增加,20 - 30分钟后达到最大值。磷酸二酯酶抑制剂咯利普兰(30 μmol/l)可增强对福斯高林(50 μmol/l)的cAMP反应,使净cAMP反应从1234±154 pmol/骨增加到2854±193 pmol/骨(平均值±标准误,n = 4)。培养24小时后,用福斯高林(30 μmol/l)处理的骨中cAMP水平显著升高。在不存在和存在咯利普兰(30 μmol/l)的情况下,0.3 μmol/l及以上的福斯高林会导致cAMP剂量依赖性积累,计算得出的半数有效浓度(EC50)值为8.3 μmol/l。在24小时培养中,福斯高林抑制自发性和甲状旁腺激素(PTH)刺激的45Ca释放,计算得出的半数抑制浓度(IC50)值分别为1.6和0.6 μmol/l。福斯高林显著抑制PTH(10 nmol/l)刺激的[3H]脯氨酸标记骨中3H的释放。福斯高林对PTH刺激的45Ca释放的抑制作用在培养3小时后就很明显。在24小时培养中,福斯高林(3 μmol/l)也显著抑制前列腺素E2(1 μmol/l)和1α - 羟胆钙化醇(0.1 μmol/l)刺激的骨中45Ca释放。福斯高林对自发性和PTH刺激的45Ca释放的抑制作用是短暂的。在120小时培养中,当福斯高林浓度达到3 nmol/l及以上时,可观察到对基础45Ca释放的剂量依赖性刺激,计算得出的EC50值为16 nmol/l。福斯高林(1 μmol/l)的刺激作用可被降钙素(0.1单位/ml)抑制,但对吲哚美辛(1 μmol/l)不敏感。福斯高林增加了培养120小时的[3H]脯氨酸标记骨中3H的释放,并降低了培养后骨中羟脯氨酸的含量。在24小时培养中,福斯高林抑制PTH刺激的Ca2 +、无机磷、β - 葡萄糖醛酸酶和β - N - 乙酰氨基葡萄糖苷酶的释放。在120小时培养中,福斯高林刺激矿物质和溶酶体酶的基础释放。(摘要截断于400字)
