1α-羟基-3-表维生素D3的分离与鉴定,一种甲状旁腺激素分泌的强效抑制剂。
Isolation and identification of 1alpha-hydroxy-3-epi-vitamin D3, a potent suppressor of parathyroid hormone secretion.
作者信息
Brown Alex J, Ritter Cynthia S, Weiskopf A S, Vouros P, Sasso Gino J, Uskokovic Milan R, Wang Guochun, Reddy G Satyanarayana
机构信息
Washington University School of Medicine, 660S Euclid Avenue, Box 8126, St. Louis, Missouri 63110, USA.
出版信息
J Cell Biochem. 2005 Oct 15;96(3):569-78. doi: 10.1002/jcb.20553.
Since our original demonstration of the metabolism of 1alpha,25(OH)2D3 into 1alpha,25(OH)2-3-epi-D3 in human keratinocytes, there have been several reports indicating that epimerization of the 3 hydroxyl group of vitamin D compounds is a common metabolic process. Recent studies reported the metabolism of 25OHD3 and 24(R),25(OH)2D3 into their respective C-3 epimers, indicating that the presence of 1alpha hydroxyl group is not necessary for the 3-epimerization of vitamin D compounds. To determine whether the presence of a 25 hydroxyl group is required for 3-epimerization of vitamin D compounds, we investigated the metabolism of 1alphaOHD3, a non-25 hydroxylated vitamin D compound, in rat osteosarcoma cells (ROS 17/2.8). We noted metabolism of 1alphaOHD3 into a less polar metabolite which was unequivocally identified as 1alphaOH-3-epi-D3 using the techniques of HPLC, GC/MS, and 1H-NMR analysis. We also identified 1alphaOH-3-epi-D3 as a circulating metabolite in rats treated with pharmacological concentrations of 1alphaOHD3. Thus, these results indicated that the presence of a 25 hydroxyl group is not required for 3-epimerization of vitamin D compounds. Furthermore, the results from the same studies also provided evidence to indicate that 1alphaOH-3-epi-D3, like 1alphaOHD3, is hydroxylated at C-25. We then evaluated the biological activities of 1alphaOH-3-epi-D3. Treatment of normal rats every other day for 7 days with 2.5 nmol/kg of 1alphaOH-3-epi-D3 did not raise serum calcium, while the same dose of 1alphaOHD3 increased serum calcium by 3.39 +/- 0.52 mg/dl. Interestingly, in the same rats which received 1alphaOH-3-epi-D3 we also noted a reduction in circulating PTH levels by 65 +/- 7%. This ability of 1alphaOH-3-epi-D3 to suppress PTH levels in normal rats without altering serum calcium was further tested in rats with reduced renal function. The results indicated that the ED50 of 1alphaOH-3-epi-D3 for suppression of PTH was only slightly higher than that of 1alpha,25(OH)2D3, but that the threshold dose of the development of hypercalcemia (total serum Ca > 10.5 mg/dl) was nearly 80 times higher. These findings indicate that 1alphaOH-3-epi-D3 is a highly selective vitamin D analog with tremendous potential for treatment of secondary hyperparathyroidism in chronic renal failure patients.
自从我们最初证明在人角质形成细胞中1α,25(OH)₂D₃可代谢为1α,25(OH)₂-3-表-D₃以来,已有多篇报道表明维生素D化合物3位羟基的差向异构化是一个常见的代谢过程。最近的研究报道了25OHD₃和24(R),25(OH)₂D₃分别代谢为它们各自的C-3差向异构体,这表明1α羟基的存在对于维生素D化合物的3-差向异构化并非必需。为了确定25羟基的存在对于维生素D化合物的3-差向异构化是否必要,我们研究了非25羟基化的维生素D化合物1αOHD₃在大鼠骨肉瘤细胞(ROS 17/2.8)中的代谢。我们注意到1αOHD₃代谢为一种极性较小的代谢产物,通过高效液相色谱(HPLC)、气相色谱/质谱联用(GC/MS)和¹H-核磁共振(¹H-NMR)分析技术明确鉴定其为1αOH-3-表-D₃。我们还鉴定出1αOH-3-表-D₃是用药理浓度的1αOHD₃处理的大鼠体内的一种循环代谢产物。因此,这些结果表明25羟基的存在对于维生素D化合物的3-差向异构化并非必需。此外,同一研究的结果还提供证据表明,与1αOHD₃一样,1αOH-3-表-D₃在C-25位发生羟基化。然后我们评估了1αOH-3-表-D₃的生物学活性。每隔一天用2.5 nmol/kg的1αOH-3-表-D₃处理正常大鼠7天,血清钙未升高,而相同剂量的1αOHD₃使血清钙升高了3.39±0.52 mg/dl。有趣的是,在接受1αOH-3-表-D₃的同一批大鼠中,我们还发现循环甲状旁腺激素(PTH)水平降低了65±7%。在肾功能减退的大鼠中进一步测试了1αOH-3-表-D₃在不改变血清钙的情况下抑制正常大鼠PTH水平的能力。结果表明,1αOH-3-表-D₃抑制PTH的半数有效剂量(ED50)仅略高于1α,25(OH)₂D₃,但高钙血症(血清总钙>10.5 mg/dl)发生的阈值剂量几乎高80倍。这些发现表明1αOH-3-表-D₃是一种高度选择性的维生素D类似物,在治疗慢性肾衰竭患者的继发性甲状旁腺功能亢进方面具有巨大潜力。
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