Pavlovitch J H, Cournot-Witmer G, Bourdeau A, Balsan S, Fischer J A, Heynen G
J Clin Invest. 1981 Sep;68(3):803-810. doi: 10.1172/jci110317.
The possible suppressive effects of 24,25-dihydroxycholecalciferol on secondary hyperparathyroidism and increased bone resorption were investigated in adult rats raised on a diet normal in calcium, phosphorus, and vitamin D, and subjected to acute bilateral nephrectomy. The animals had received subcutaneous radiocalcium 4 wk before the experiment. 5 h after nephrectomy an increase in serum total calcium, (45)Ca-specific activity, citrate, phosphorus, and magnesium concentrations were observed. Serum immunoreactive parathyroid hormone increased, while serum calcitonin decreased. The osteoclast count in the tibial metaphyses was augmented. The biochemical and histological changes observed were partly parathyroid hormone and calcitonin independent, as they also occurred in parathyroidectomized hypocalcemic rats. Pretreatment with 650 pmol of 24,25-dihydroxycholecalciferol 16 h before nephrectomy prevented bone calcium mobilization and diminished the rise in serum total calcium and citrate both in parathyroid-intact and in parathyroidectomized animals. In parathyroid-intact rats, serum immunoreactive parathyroid hormone and calcitonin remained normal in spite of the fall in serum-ionized calcium, and the number of osteoclasts did not increase. In parathyroidectomized rats, 24,25-dihydroxycholecalciferol did not prevent the postnephrectomy rise in the osteoclast count. This latter observation suggests that this metabolite exerts its effect on bone either by acting on cells other than osteoclasts, i.e., the osteocytes, or by inhibiting cell activity. At equimolar dosage 1,25-dihydroxycholecalciferol had a potent stimulatory effect on bone resorption. This effect of 1,25-dihydroxycholecalciferol was partly blocked by the simultaneous administration of 24,25-dihydroxycholecalciferol. The potential clinical significance of these observations remains to be determined.
在以钙、磷和维生素D含量正常的饮食饲养并接受急性双侧肾切除的成年大鼠中,研究了24,25 - 二羟胆钙化醇对继发性甲状旁腺功能亢进和骨吸收增加的可能抑制作用。实验前4周,这些动物接受了皮下注射放射性钙。肾切除术后5小时,观察到血清总钙、(45)Ca比活性、柠檬酸盐、磷和镁浓度升高。血清免疫反应性甲状旁腺激素增加,而血清降钙素降低。胫骨干骺端的破骨细胞计数增加。观察到的生化和组织学变化部分与甲状旁腺激素和降钙素无关,因为它们也发生在甲状旁腺切除的低钙血症大鼠中。肾切除术前16小时用650 pmol的24,25 - 二羟胆钙化醇预处理可防止骨钙动员,并减少甲状旁腺完整和甲状旁腺切除动物血清总钙和柠檬酸盐的升高。在甲状旁腺完整的大鼠中,尽管血清离子钙下降,但血清免疫反应性甲状旁腺激素和降钙素仍保持正常,破骨细胞数量也未增加。在甲状旁腺切除的大鼠中,24,25 - 二羟胆钙化醇不能防止肾切除术后破骨细胞计数的升高。后一观察结果表明,这种代谢产物对骨的作用要么是通过作用于破骨细胞以外的细胞,即骨细胞,要么是通过抑制细胞活性。在等摩尔剂量下,1,25 - 二羟胆钙化醇对骨吸收有强烈的刺激作用。1,25 - 二羟胆钙化醇的这种作用部分被同时给予的24,25 - 二羟胆钙化醇所阻断。这些观察结果的潜在临床意义尚待确定。